Endocrinopathies in Survivors of Childhood Neoplasia

Abstract

Advancements in cancer treatments have increased the number of survivors of childhood cancers. Endocrinopathies are common complications following cancer therapy and may occur decades later. The objective of the current review is to address the main endocrine abnormalities detected in childhood cancer survivors including disorders of the hypothalamic-pituitary axis, thyroid, puberty, gonads, bone, body composition, and glucose metabolism.

Introduction

Approximately 1 in 285 children will be diagnosed with cancer before the age 20 years, and 1 in 530 young adults between the ages of 20 and 39 years is a childhood cancer survivor (CCS) (1). Endocrine complications are among the most common sequelae observed in CCS, and they frequently occur as cancer therapy-related late – effects appearing years, even decades, after the exposure to chemotherapy and/or radiotherapy. The prevalence of an endocrine disorder in 1423 at risk adult CCS was reported to be 62% (95% CI 59.5–64.6) (2). The 60-year cumulative risk of having an endocrinopathy in an individual diagnosed with cancer between the ages of 5 and 9 years was 43% in a large cohort of Northern European CCS (3). The occurrence of endocrine disorders documented in an Italian Transition Unit for adult CCS was 48.46 and 62.78% in females and males, respectively (Figure 1) (4). Treatment exposures placing individuals at risk of endocrinopathies have traditionally included alkylating agent based chemotherapy and radiotherapy. More recently, selective mitogen-activated kinase inhibitors and immune system modulators have been shown to also be associated with endocrine dysfunction. The long-term consequences of the use of these novel therapies, some of which are prescribed in maintenance regimens, remain to be fully elucidated (5–7). Healthcare providers should be equipped to diagnose and manage acute and long-term endocrine complications that may arise in maturing CCS. This review will address the risk of endocrine disorders associated with the treatment of pediatric cancer and brain tumors. The data summarized in this review are based on a systematic search of the medical literature using MEDLINE/Pubmed (from 1970 to May 2014) using keywords relevant to this topic. Additional searches were conducted within the reference lists of relevant articles.

Figure 1

Disorders of the Hypothalamus and Pituitary

Tumor development and/or surgical resections close to the hypothalamus and/or pituitary may induce direct anatomical damage to these structures and result in multiple hypothalamic/pituitary dysfunctions (Table 1). Disorders of the hypothalamus/pituitary are also common following their exposure to direct or scatter radiotherapy. More recently, Ipilimumab, an immune system modulator, was shown to potentially cause auto-immune hypophysitis with ensuing anterior panhypopituitarism (7). Pituitary dysfunction was the most frequent endocrine complication in a Northern European cohort comparing 31,723 CCS and 211,261 controls. In this study, the standard hospitalization rate ratio of hypopituitarism was 88.0 (95% CI 72.1–107.5) in CCS when compared to matched controls from the local general population (3).

Growth hormone deficiency and poor linear growth

Growth failure and short stature are among the most common sequelae of childhood cancer therapy (8). Several etiologies may contribute to growth failure in CCS including growth hormone deficiency (GHD), exposures to spinal and total-body irradiation (TBI), pubertal disorders, chemotherapy treatments including glucocorticoids, hypothyroidism, suboptimal nutrition, and renal disease (9–12).

In CCS, GHD is frequently attributed to cranial radiotherapy doses of 12–64 Gy to the hypothalamus/pituitary (4). Radiation has a dose and time dependent effect on GH secretion. Merchant et al. demonstrated that GHD was likely to develop within 36 months of exposure to hypothalamic/pituitary radiotherapy in individuals receiving doses ≥20 Gy (13) (Figure 2). In comparison to radiotherapy, the impact of chemotherapy alone on GHD secretion is more controversial and less common (14–17). Imatinib, a tyrosine kinase inhibitor (TKI), has been associated with growth deceleration and with failure of provocative GH stimulation testing (18, 19). Imatinib is presumed to inhibit bone growth by impeding the kinase mediated release of GH (5).

Figure 2

Growth hormone deficiency should be investigated in skeletally immature CCS when linear growth velocity decelerates over a 6-month period. The effect of GHD on growth may be masked by precocious puberty and by hyperinsulinemia in the context of rapid weight gain (“growth without growth hormone”) with seemingly normal linear growth driven by sex steroids and insulin respectively in affected individuals (20, 21). CCS exposed to spinal radiotherapy are at risk of having skeletal disproportions; this should ideally be investigated by measuring the sitting height (12). Biochemical evaluation for GHD requires dynamic testing, which despite limitations related to poor reproducibility in the general population, remains acceptable for the assessment of GH secretion in CCS (22). In the general population, the diagnosis of GHD typically requires failing dynamic tests using two different secretagogues; however, in CCS exposed to cranial radiotherapy and individuals with a history of a brain tumor close to the hypothalamus/pituitary, failing one test was considered sufficient in the consensus guidelines published by the Growth Hormone Research Society (23). Secretagogues used in dynamic testing include insulin, arginine, levodopa, clonidine, and glucagon. GH releasing hormone (GHRH) should not be used for the assessment of GH secretion in this population given the primarily hypothalamic location of radiation-induced damage (24). Plasma levels of IGF-1 and IGFBP3, although commonly practiced, are not reliable screening tools in CCS exposed to cranial radiotherapy and are associated with high rates of false-negatives (25).

Treatment with recombinant GH (rGH) replacement therapy is typically not initiated until 12 months after successfully completing cancer or brain tumor treatments. The mitogenic potential of GH stimulating tumor growth is a safety concern in CCS (26). Studies suggest that rGH in patients with brain tumors are not associated with primary disease recurrence (27–29). However, there may be an increase in the development of second neoplasm in CCS treated with GH (30, 31). Ergun-Longmire et al. reported a relative risk of 2.15 (95% CI, 1.3–3.5; p < 0.002) of developing a second neoplasm in CCS treated with rGH when compared to controls and the most commonly identified neoplasms were meningiomas (30). Nevertheless, using the same multi-center cohort of CCS and reporting specifically on the risk of subsequent central nervous system neoplasms after a longer period of follow-up, Patterson et al. recently reported an adjusted rate ratio of meningioma and gliomas in GH treated survivors of CNS tumors when compared to CNS tumor survivors who were not treated with GH of 1.0 (95% CI 0.6–1.8, p = 0.94), thus indicating negligible differences between the two groups in regards to this particular risk (32).

The benefits of rGH extend beyond linear growth and are highlighted in adult GHD studies. Some of the advantages include improvements in bone mineral density (BMD), cardiovascular function, reduction in metabolic syndrome, and sustained improvements in quality of life (33). The benefits and risk of rGH have to be carefully weighed in children and adult survivors. Ongoing studies are needed to investigate and characterize the risk of developing second neoplasms as well as the proposed advancements in the physiological and psycho-social well-being of rGH in CCS.

Disorders of luteinizing hormone and follicle-stimulating hormone

Central precocious puberty

Central precocious puberty (CPP) is defined by the early activation of the hypothalamic–pituitary–gonadal axis leading to the onset of puberty prior to the ages of 8 and 9-years in girls and boys, respectively (34, 35). The consequences of CPP include the premature closure of growth plates resulting in decreased adult height prospects. Precocious puberty, especially menarche, can generate significant psycho-social adjustment challenges in young children, particularly in those with special needs. While radiotherapy to the hypothalamus/pituitary is the main risk factor associated with CPP in CCS; pubertal development can also be triggered prematurely by tumors located near the hypothalamus or optic pathways independently from radiation exposure. Additional risk factors include hydrocephalus, female sex, exposure to radiotherapy before the age of 5 years, and increased BMI (36, 37).

The mean linear velocity in children with CPP can be 8–10 cm/year (+2 to +4 SDS for chronological age) at diagnosis (38); however, in CCS the linear growth velocity may be normal or poor secondary to concurrent GHD or spinal damage from radiotherapy (39). Clinicians should not rely on the measurement of testicular volume for the diagnosis of puberty in males exposed to gonadotoxic chemotherapy regimens (as those with alkylating agents) and/or testicular irradiation. In these individuals, treatment-related germ cell injury can impair testicular growth without necessarily affecting their ability to produce testosterone and this can be particularly misleading in the context of CPP. Clinicians should be aware of these caveats and have a low threshold to initiate laboratory testing if there is suspicion of early pubertal growth based on other clinical markers such as penile enlargement, scrotal skin thinning, or pubarche.

Biochemical evidence of CPP includes pubertal basal levels of luteinizing hormone (LH) and sex steroids (estradiol or testosterone). Random basal values may be inconclusive secondary to the pulsatile nature of gonadotropins and stimulated values may be necessary to establish the diagnosis. GnRH agonists are used in stimulation testing and a pubertal LH value and a LH to follicle-stimulating hormone (FSH) ratio >1 is consistent with CPP (34, 40). Radiographic evaluation encompasses an assessment of a child’s skeletal maturation (41, 40). In females a pelvic ultrasound demonstrating pubertal sized uterus and ovaries may also be helpful in confirming the diagnosis (42).

Treatment with a GnRH agonist suppresses the secretion of gonadotropins and may be useful in improving final height prospects by delaying skeletal maturation and allowing a longer time for linear growth (43). This treatment may also act synergistically with rGH and improve the final adult height of GH-deficient CCS who also have CPP (43). Determining the best time to discontinue GnRH agonist therapy even in children with idiopathic CPP can be challenging and requires taking into account multiple factors including chronological age, bone age, target height, psycho-social maturation, and parental preferences. This determination is rendered even more challenging by the possible development over time of permanent LH/FSH deficiency in these patients (44). The use of aromatase inhibitors in order to prolong the delay in closure of growth plates in concert with rGH has been utilized by some clinicians to augment the height outcomes of CCS (45). Data remain inconclusive as to whether or not aromatase inhibitors improve adult height and many pediatric endocrinologists consider their use to be experimental.

LH/FSH deficiency

The deficiency in LH/FSH, also referred to as hypogonadotropic hypogonadism, can result in delayed or arrested pubertal development during childhood. The post-pubertal male and female with LH/FSH deficiency may present with androgen insufficiency symptoms and secondary amenorrhea, respectively. LH/FSH deficiency can occur after tumor and/or surgery related damage or after doses of radiotherapy to the hypothalamic–pituitary area >30 Gy (36, 46, 47). Female CCS diagnosed after the age of 10 years and who received doses >50 Gy are at high risk for delayed menarche (36). Deficiency in LH/FSH may also occur in the context of ipilimumab-induced auto-immune hypophysitis, as detailed in Section “Corticotropin Deficiency” (7). Replacement is warranted for the development and maintenance of secondary sex characteristic, optimal bone mass accrual, and body composition. Sex steroids also play a pivotal role in the metabolism of lipids and carbohydrates (48).

Corticotropin deficiency

Corticotropin (ACTH) deficiency, also known as central adrenal insufficiency, can occur in CCS following tumor and/or surgery related damage or after the exposure of the hypothalamus/pituitary to radiotherapy doses ≥30 Gy (49). Hudson et al. identified disorders of the hypothalamic–pituitary–adrenal axis in 13.8% of CCS exposed to cranial radiotherapy (2). In a study of children with embryonal brain tumors treated with radiotherapy, the 4-year cumulative incidence of ACTH deficiency was 38 ± 6% and there was no significant difference in those patients who received irradiation of >42 and <42 Gy (50). The incidence of ACTH deficiency in patients receiving TBI as part of preconditioning of BMT has been reported at 6% (51) ACTH deficiency was documented in 60% (n = 50) of patients receiving BMT for malignant and non-malignant reasons. It was more likely to occur in patients who had been transplanted <1 year prior to testing and all the subjects who were diagnosed were asymptomatic (15). The clustering of ACTH deficiency cases within a year of transplant in this study suggests that a large proportion of patients experience transient forms of this condition as a result of their exposure to high-dose glucocorticoids. More recently, ACTH deficiency has been associated with the use of imatinib, a TKI with 48% of individuals diagnosed 3–71 months following the exposure (52). Ipilimumab, an immune system modulator can cause auto-immune hypophysitis with ensuing panhypopituitarism, especially at doses >3 mg/kg with a reported prevalence of 4.9–17% (7, 53, 54). The onset of hypophysitis may not occur until 6 weeks after therapy and affected individuals may require 2–5 years of glucocorticoid therapy (55). Future investigations are needed to determine when and for how long CCS treated with these agents should be tested. If patients are deemed insufficient, the chronicity of the insufficiency should also be studied.

Symptoms of ACTH deficiency include fatigue, weakness, nausea, vomiting, anorexia, and abdominal cramping. When exposed to a severe illness, patients with ACTH deficiency may develop life threatening complications including hypoglycemia related seizures and hypotensive shock. Untreated ACTH deficiency may be associated with decreased free water clearance and hyponatremia; replacement with hydrocortisone in such instances, especially in post-surgical patients, may unmask co-existent central diabetes insipidus. A screening cortisol level, collected at 8 a.m. that is ≥10 mcg/dl is reassuring and against the presence of ACTH deficiency; a value ≤5 mcg/dl at 8 a.m. should in contrast raise high suspicions regarding this diagnosis. Definitive testing includes insulin tolerance, low dose cosyntropin or metyrapone stimulation tests. A peak cortisol value <18 μg/dl following low dose (1 microgram) cosyntropin is the most commonly used diagnostic criterion (56). The treatment of ACTH deficiency relies on replacement therapy with hydrocortisone and patient and family education regarding stress dosing during times of illness.

TSH deficiency

Thyroid stimulating hormone deficiency, also known as central hypothyroidism, is rarely reported in CCS. It can occur as a result of tumor and/or surgery related damage or after hypothalamic/pituitary exposure to radiotherapy doses ≥30 Gy (44, 50, 57, 58). One CCS study detected TSH deficiency in 6% (n = 71) of childhood brain tumor survivors (59). Deficiency in TSH may also occur in the context of ipilimumab-induced auto-immune hypophysitis, as detailed in Section “Corticotropin Deficiency” (7). Hypothyroidism is associated with poor linear growth, delayed bone age, and disturbances in pubertal timing during childhood. It can also cause fatigue, fluid retention, constipation, cold intolerance, proximal muscle weakness, and depression. A serum free T4 (FT4) below normal in conjunction with a low or normal serum TSH is characteristic of TSH deficiency. Levothyroxine is used to treat this form of hypothyroidism with doses are adjusted to maintain FT4 values within mid to high normal ranges (60). In contrast to primary hypothyroidism (PH), serum TSH values are not helpful in the monitoring of this condition, as they are expected to remain low even after inadequate replacement with levothyroxine.

Hyperprolactinemia

Prolactin production by the pituitary gland is controlled by the hypothalamus, with a predominantly inhibitory tone due to dopaminergic input. Disruptions of hypothalamic–pituitary connections due to tumor growth, surgery, or doses of radiotherapy >30–50 Gy can result in hyperprolactinemia because of the loss of hypothalamic inhibition on prolactin secretion (44, 61, 62). Patients with hyperprolactinemia can present with galactorrhea. Furthermore, elevated prolactin levels may suppress LH and FSH production and cause hypogonadism. Nevertheless, hyperprolactinemia in CCS tends to remain asymptomatic, especially in a patient population where individuals are concurrently at risk of gonadotropin deficiency and primary gonadal failure because of their cancer treatment exposures (62).

Central diabetes insipidus

Central diabetes insipidus is the clinical manifestation of the deficit in secretion and release of the anti-diuretic hormone (ADH). Hypothalamic neurons are responsible of the production of ADH; the latter is carried by axonal transport to the posterior pituitary from which it is released into the circulation. The deficiency in ADH impairs the affected individual’s ability to concentrate urine with ensuing polyuria, polydipsia, and dehydration when access to free water is compromised. Central diabetes insipidus can be a mode of revelation of childhood brain malignancies such as dysgerminomas or hypophyseal non-Hodgkin’s lymphomas (63, 64). In these instances, it can initially be isolated and as the tumoral infiltration worsens additional pituitary functions become deficient (64). More commonly, however, diabetes insipidus occurs in the context of pan-hypopituitarism due to the presence of a tumor in close proximity to the sellar region or as a consequence of surgical procedures aimed at removing it. Central diabetes insipidus does not occur as a late effect of cranial radiotherapy and is hence rarely discussed in the literature dedicated to CCS (65). Central diabetes insipidus does not seem to be associated with the use of ipilimumab (7). The management of central diabetes insipidus consists of replacement therapy using desmopressin with close monitoring of fluid intake and urine output in order to avoid overtreatment and ensuing hyponatremia and seizures. Significant shifts in replacement needs are noted in the post-operative patient, mandating close monitoring in the inpatient setting until stabilization is achieved (66, 67). This was well characterized following neurosurgical interventions on sellar/supra sellar tumors such as craniophayngioma with the classical description of a triple phase response consisting of a first phase of transient diabetes insipidus lasting for up to 2 days, followed by an anti-diuretic phase of 1–2 weeks before the onset of permanent diabetes insipidus (67). Patients with altered thirst sensation are more easily managed with the determination of a fixed daily fluid requirement in addition to a fixed dose of desmopressin in order to avoid significant fluctuations in their hydration status (66).

Disorders of the Thyroid

The radiosensitive nature of the thyroid gland predisposes it to dysfunctions including hypothyroidism, hyperthyroidism, nodules, and cancer (Table 2). Hudson et al. identified thyroid disorders in up to 66.4% of CCS exposed to neck radiotherapy (2). Thyroid dysfunction has been attributed to multiple cancer therapies including radiotherapy with direct or scatter exposure of the neck, TKI, 131 I-Metaidobenzylguanidine ([131I] MIBG), retinoid X receptor agonist autoantibodies, angiogenesis inhibitor thalidomide, and interferon-α (68–70).

Primary hypothyroidism

Primary hypothyroidism is the most common thyroid abnormality in CCS. In a study by Armstrong et al., the relative risk of PH in CCS was 17.1 when compared to sibling controls (70). The study also documented that up to 50% Hodgkin lymphoma patients receiving >45 Gy developed hypothyroidism within 5-years (70). Female sex and older age at diagnosis were also associated with an increased incidence of hypothyroidism. The risk of PH has primarily been attributed to direct or scatter radiation of the neck including cranio-spinal radiotherapy as well as TBI for cytoreduction before HSCT (50, 58, 59, 71). Subclinical or compensated PH is more commonly diagnosed than overt PH in the context of low dose radiotherapy and HSCT, with some patients experiencing spontaneous recovery (58). Chemotherapy alone has not been traditionally associated with PH. However, TKIs such as sorafenib, sunitinib, and imatinib have been noted to cause thyroid dysfunction (72–74). Hypothyroidism during treatment with sunitinib occurred in 7–85% of patients (72, 73). The pathophysiology of TKI causing PH remains elusive; it may be secondary to destruction of the thyroid gland, impairments of thyroid hormone transport or metabolism, or reduced TSH clearance (72). PH was documented in 13 out 16 CCS of neuroblastoma treated with [131I] MIBG in a long-term follow-up study over a period of 15.5 years (11.2–20.2) (69).

Extended surveillance for thyroid dysfunction is crucial as hypothyroidism in CCS exposed to radiotherapy and radio-labeled agents may occur decades later. The clinical presentation of PH is similar to central hypothyroidism in CCS; however, biochemically they differ. The labs in PH include an elevated plasma TSH level with normal or low free T4; both values are used in monitoring replacement using levothyroxine at substitutive doses.

Hyperthyroidism

Hyperthyroidism was diagnosed in up to 5% of survivors in a report by Armstrong et al., a rate that was 8 times greater than in sibling controls (70). Overt hyperthyroidism albeit rare has been reported in CCS after hematopoietic stem-cell transplant (HSCT) (75–77). The occurrence of hyperthyroidism may be more common shortly after HSCT with Jung et al. reporting a prevalence of 4.5% in the first 3 months following transplant (77). Lower prevalence values (0.7–2%) have been reported in studies incorporating long-term follow in the pediatric HSCT population (75, 76).

Autoimmune induced thyroid disease

Positive thyroid autoantibodies have been reported in cases of hypothyroidism and hyperthyroidism in CCS of allogeneic HSCT (78, 79). It has been presumed to be related to the transfer of auto-immunity from the stem-cell donor to the HSCT recipient. However, the presence of thyroid antibodies does not necessarily lead to progression to hypothyroidism in the context of HSCT (80). Auto-immune thyroiditis may exacerbate the thyroid toxicity of certain, but not all, TKI (72, 81). Autoimmune and non-autoimmune thyroiditis are also well established toxicities of interferon-α, a human recombinant cytokine used in the treatment of some solid tumors and hematologic malignancies (82). Newer anticancer agents such as the monoclonal antibodies have also been associated with rare cases of auto-immune hypothyroidism and transient hyperthyroidism. The incidences of ipilimumab-induced auto-immune hypothyroidism in small case reports have been 0–2, 7, and 19% in patients receiving standard doses, high doses, and combination therapy with bevacizumab, respectively (82).

Thyroid neoplasms

Second thyroid neoplasms may occur later than two decades after the diagnosis of the primary cancer in CCS (83, 84). Armstrong et al. conveyed that 20 years after diagnosis, the risk of having a thyroid nodule in CCS after exposure to neck irradiation was 20%, which is 27 times higher than the sibling population (70). The association between the development of thyroid cancer and direct or scatter radiation of the neck is well known (85). In a large cohort of 12,575 CCS, 111 cases of second primary cancers were pathologically confirmed in patients who had received radiotherapy (86). The most common second primary cancer was papillary thyroid carcinoma and the risk was highest in patients who had received ≤20 Gy, were of female and of a young age (<10 years) at the time of diagnosis of the primary cancer (86). Hodgkin lymphoma is the primary cancer most commonly associated with thyroid cancer. The cumulative incidence of thyroid cancer was 2.3% (95% CI, 1.7–3.1) in this population (83). A recent report by Veiga et al. suggested that alkylating agents in conjunction with <20 Gy of irradiation can increase the incidence of thyroid neoplasm by 2.4 (95% CI, 1.3–4.5; p = 0.002) (83). Radiolabeled agents such as 131I MIBG used in the treatment of neuroblastomas have also been associated with the development of papillary thyroid cancer (68).

The currently recommended screening modality for thyroid cancer in CCS at risk is the yearly clinical examination of the neck by an experienced provider. There is significant disagreement regarding the use of thyroid ultrasound for the purposes of screening in the absence of clinical symptoms, because of the high probability of finding abnormal results leading to higher rates of diagnostic procedures and unnecessary anxiety to patients and their families; the yield in identifying malignant nodules with ultrasonography is indeed low, even in survivors of Hodgkin lymphoma (87–90). Kovalchik et al. recently validated an absolute risk prediction model (AUC 0.80, 95% CI), screening for thyroid cancer in CCS. The model was based on sex, age <15 years at primary cancer diagnosis, history of thyroid nodule, radiotherapy to the neck, and exposure to alkylating agents (91). The diagnosis of second primary thyroid cancer in CCS relies on the presence of a positive result on a fine needle aspiration biopsy of a suspected nodule; the treatment approach and prognosis are identical to thyroid cancer cases diagnosed in the general population (87).

Disorders of the Gonads

Males

The testes have two functional compartments, a reproductive compartment and an endocrine compartment (Table 2). The reproductive compartment consists of germ cells and the Sertoli cells that support them. The endocrine compartment encompasses the Leydig cells, which are responsible for producing testosterone. The two compartments are affected differently by cancer therapies and understanding this dichotomy in testicular function is imperative in counseling male CCS in regards to their risk of gonadal dysfunction.

Leydig cell dysfunction

Hypogonadism after chemotherapy exposure alone is rare (92, 93). However, high doses of alkylating agents, such as cyclophosphamide can cause low testosterone (94, 95). There are also case reports of broad acting kinase inhibitors causing low testosterone and gynecomastia (96). Leydig cell dysfunction as a result of testicular irradiation is dependent on the age of the exposure and the dose of irradiation. Pre-pubertal males receiving doses >24 Gy are at high risk for hypogonadism, whereas pubertal males are at risk when exposed to >33 Gy (97–99). An elevated LH and a low normal morning testosterone define subclinical hypogonadism, and can be attributed to moderate doses of alkylating agent and low dose of testicular irradiation (<20 Gy); however, subclinical hypogonadism rarely requires exogenous testosterone replacement therapy (99–101). At risk, CCS should be followed closely for signs and biochemical evidence of hypogonadism that warrant replacement therapy during pubertal years and adulthood.

Germ cell dysfunction

Germ cells are more sensitive to testicular irradiation and chemotherapy than Leydig cells. Chemotherapy agents associated with germ cell dysfunction include cyclophosphamide, procarbazine, ifosfamide, busulfan, melphalan, and cisplatin (99, 102). Green et al. reported germ cell dysfunction with subsequent azospermia in 38.2% (n = 275) males exposed to chemotherapy and/or testicular irradiation (103). Small testicular volume, elevated FSH, and low inhibin B levels are associated with poor fertility prognosis in males; however, these clinical and biochemical findings lack sensitivity and specificity in male CCS. Males exposed to gonadotoxic agents may recover germ cell function and it is recommended that they have semen analyses in order to determine fertility status (103, 104).

Sperm cryopreservation is recommended in cancer patients prior to therapy with gonodotoxic agents. In pre-pubertal males, an approach combining testicular tissue extraction, spermatogonial stem-cell preservation, and later transplantation of decontaminated (non-malignant) cells has been proposed but remains experimental (99, 105, 106).

Females

The ovaries do not replicate the functional dichotomy (distinct endocrine and reproductive compartments) observed in the testes. The female ovarian follicle is responsible for estrogen production and oocyte maturation, and both functions are simultaneously affected by gonadal failure. The extent of ovarian damage and subsequent residual function do not solely depend on the intensity of the cancer treatments received by the patient. These also depend on the number of viable follicles, or “ovarian reserve,” at the time of the exposure. Patients whose viable follicles were depleted during therapy do not experience a recovery of their ovarian function after the completion of cancer treatments and are diagnosed with acute ovarian insufficiency (107). A subset of individuals, with a less severe but nevertheless significant depletion of their ovarian reserve, will experience a resumption of pubertal development or menstrual cycles in the few years following the completion of cancer therapy only to be diagnosed several years later with premature menopause, which is defined as ovarian failure prior to the age of 40 years (108). Given naturally declining numbers of follicles during a woman’s lifespan, ovarian reserve and, consequently, vulnerability to damage from gonadotoxic agents, are particularly dependent on chronological age at the time of exposure to cancer treatments (107, 108). Cancer treatments associated with ovarian toxicity include abdominopelvic irradiation (API) and chemotherapy agents such as cyclophosphamide, procarbazine, busulfan, melphalan, and thiotepa (107–110). Chemotherapy is less toxic to the ovaries of pre-pubertal females in comparison to pubertal and adult females (107, 111–113). The ovarian toxicity of API is age and dose dependent, irradiation doses >20 Gy in female, CCS >13 years old, and TBI in CCS > 10-years is correlated with ovarian insufficiency (107, 114, 115). A study of an AML cohort treated with chemotherapy alone (anthracyclines and cytarabine) demonstrated that menarche occurred at the mean age of 13.1 years and fertility rates were similar to their siblings (92). Even in the absence of exposure to API and despite the occurrence of menarche at a normal age, CCS were nevertheless shown to have a decreased reproductive capacity in comparison to healthy controls in another report (113). The risk of premature menopause was 8 and 0.8% (RR = 13.21, 95% CI = 3.26–53.51; p < 0.001) in CCS and siblings, respectively (108). The cumulative incidence of premature menopause was highest among CCS exposed to both alkylating agents and API (108). Evidence of ovarian insufficiency includes elevated gonadotropins, low anti-mullerian hormone (AMH) levels, and reduced mean ovarian volume (113). AMH is an acceptable marker of ovarian follicular reserve in female CCS, and low levels are indicative of declining ovarian function (116–119). Despite declining ovarian reserve in CCS, some survivors have successful pregnancies, with live birth rates of 63–73% (119–121).

Young CCS with ovarian failure may experience poor linear growth and poor bone mineralization. Older hypo-gonadal females can develop menopausal symptoms and are at risk for osteoporosis and cardiovascular disease (122, 123). Sex hormone replacement therapy is warranted in female CCS with ovarian failure. The use of cryopreserved ovarian tissue from pre-pubertal females carries the risk of re-seeding malignant cells and is considered experimental; by contrast, mature oocyte cryopreservation is no longer considered experimental and may represent a viable option for young pubertal females prior to gonadotoxic therapies (124). The availability of this technique, along with better ways of assessing ovarian reserve in females at risk of premature menopause may improve fertility prospects in the CCS population.

Bone Health Related Complications

Childhood cancer survivors have an increased risk of poor bone health and decreased BMD (Table 2). Contributing factors include the primary cancer (increased osteoclast stimulation in hematological malignancies), treatment exposures, and concurrent hormone deficiencies (125). CCS treated with glucocorticoids and methotrexate or exposed to cranio-spinal radiotherapy, especially receiving >24 Gy of cranial irradiation are susceptible to decreased BMD (125, 126). The association between central nervous system exposures to radiotherapy and low BMD is likely due to radiation related endocrinopathies (deficiencies in GH and/or sex steroids in particular) (126). Lower BMD can be observed prior to cancer therapies because of the effect of the primary illness itself on bone (127). In a recent report on childhood ALL, the 3-year cumulative symptomatic fracture risk was 17.8% (n = 399). Fractures were more likely to occur during therapy than during follow up (127). The decline in BMD did not correlate with fracture risk in this study as well as in a report on survivors of osteosarcoma (127, 128). Recent studies have provided further reassurance regarding the continued recovery of BMD after the completion of therapy, a progress that continues, even in older individuals followed through adulthood (126, 129).

Optimizing bone health in CCS includes hormone replacement therapy for those with GHD, hypogonadism, and vitamin D deficiency. It is also recommended that survivors receive adequate nutritional calcium, participate in weight bearing activities, and avoid smoking (125, 128).

Overweight, Obesity, and Disorders of Glucose Homeostasis

Obesity is a recognized public health challenge with far reaching consequences on overall states of health in the general population (130, 131) (Table 2). The prevalence of obesity and metabolic syndrome in the overall CCS population seems to be comparable to that observed in the general population (2, 130, 132). Hudson et al. demonstrated the prevalence of obesity, hypertension, dyslipidemia, and diabetes was 36.5, 22.6, 50.9, and 5.9%, respectively, in a cohort of CCS followed for 26.3 years after diagnosis (2). Nevertheless, survivors of ALL and brain tumors have significantly higher risks of obesity and overweight (133). Additional risk factors include female sex, doses of cranial radiotherapy >20 Gy, age at exposure <4-years old, and GHD (134, 135). CCS with a history of brain tumor development, radiotherapy, or surgery within the hypothalamus or near the sellar region are at risk of developing a particularly severe form of obesity characterized by hyperphagia and rapid weight gain, and which is sometimes referred to as “central” or “hypothalamic” obesity (136, 137). In these patients with significant hypothalamic injury, increased parasympathetic tone and ensuing hyperinsulinemia (the latter promoting fat storage) have been suggested as possible causes for this phenomenon (136, 137). Treatment approaches for this particular type of obesity have included octreotide and dextroamphetamine (137, 138). In a randomized, double-blind placebo-controlled study of 18 individuals with hypothalamic obesity, octreotide allowed the stabilization of BMI with lower rates of weight gain and lower insulin secretion over a treatment period of 6 months (137). The use of dextroamphetamine in five children with hypothalamic obesity allowed the stabilization of BMI over a period of 24 months (138). The small numbers of patients enrolled in these studies with limited long-term follow-up data to support sustainable efficacy as well as the cost and possible side effects of the medications used in these reports have hindered the wider adoption of such treatment strategies. CCS were also shown to have a higher risk of diabetes mellitus, especially following exposure to TBI, abdominal radiotherapy, and alkylating agents (139, 140). Further research is needed in order to understand the mechanism by which such treatments leave lasting impacts on metabolism and glucose homeostasis as a preamble in optimizing the management of these disorders.

Summary

Endocrine complications are common in CCS. Healthcare providers need to be aware of the lifelong endocrinopathies associated with treatment exposures. Further research is needed in order to improve risk prediction and develop patient centered screening strategies as the early diagnosis of endocrine disorders and timely treatment of these complications can improve overall states of health and the quality of life of individuals belonging to this vulnerable population.

References

• 1

  WardEDesantisCRobbinsAKohlerBJemalA. Childhood and adolescent cancer statistics, 2014. CA Cancer J Clin (2014) 64:83–103.10.3322/caac.21219

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 2

  HudsonMMNessKKGurneyJGMulrooneyDAChemaitillyWKrullKRet alClinical ascertainment of health outcomes among adults treated for childhood cancer. JAMA (2013) 309:2371–81.10.1001/jama.2013.6296

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 3

  de Fine LichtSWintherJFGudmundsdottirTHolmqvistASBonnesenTGAsdahlPHet alHospital contacts for endocrine disorders in Adult Life after Childhood Cancer in Scandinavia (ALiCCS): a population-based cohort study. Lancet (2014) 383:1981–9.10.1016/S0140-6736(13)62564-7

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 4

  BrignardelloEFelicettiFCastiglioneAChiabottoPCorriasAFagioliFet alEndocrine health conditions in adult survivors of childhood cancer: the need for specialized adult-focused follow-up clinics. Eur J Endocrinol (2013) 168:465–72.10.1530/EJE-12-1043

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 5

  LodishMB. Clinical review: kinase inhibitors: adverse effects related to the endocrine system. J Clin Endocrinol Metab (2013) 98:1333–42.10.1210/jc.2012-4085

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 6

  KongYCFlynnJC. Opportunistic autoimmune disorders potentiated by immune-checkpoint inhibitors anti-CTLA-4 and anti-PD-1. Front Immunol (2014) 5:206.10.3389/fimmu.2014.00206

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 7

  CorselloSMBarnabeiAMarchettiPDe VecchisLSalvatoriRTorinoF. Endocrine side effects induced by immune checkpoint inhibitors. J Clin Endocrinol Metab (2013) 98:1361–75.10.1210/jc.2012-4075

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 8

  ChowEJFriedmanDLYasuiYWhittonJAStovallMRobisonLLet alDecreased adult height in survivors of childhood acute lymphoblastic leukemia: a report from the childhood cancer survivor study. J Pediatr (2007) 150(370–5):5e1.10.1016/j.jpeds.2006.11.036

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 9

  ChowEJLiuWSrivastavaKLeisenringWMHayashiRJSklarCAet alDifferential effects of radiotherapy on growth and endocrine function among acute leukemia survivors: a childhood cancer survivor study report. Pediatr Blood Cancer (2013) 60:110–5.10.1002/pbc.24198

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 10

  KnijnenburgSLMulderRLSchouten-Van MeeterenAYBökenkampABlufpandHvan Dulmen-den BroederEet alEarly and late renal adverse effects after potentially nephrotoxic treatment for childhood cancer. Cochrane Database Syst Rev (2013) 10:CD008944.10.1002/14651858.CD008944.pub2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 11

  XuWJanssAPackerRJPhillipsPGoldweinJMoshangTJr. Endocrine outcome in children with medulloblastoma treated with 18 Gy of craniospinal radiation therapy. Neuro Oncol (2004) 6:113–8.10.1215/S1152851703000462

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 12

  ClaytonPEShaletSM. The evolution of spinal growth after irradiation. Clin Oncol (1991) 3:220–2.10.1016/S0936-6555(05)80744-7

  • CrossRef
  • Google Scholar

• 13

  MerchantTERoseSRBosleyCWuSXiongXLustigRH. Growth hormone secretion after conformal radiation therapy in pediatric patients with localized brain tumors. J Clin Oncol (2011) 29:4776–80.10.1200/JCO.2011.37.9453

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 14

  RoseSRSchreiberREKearneyNSLustigRHDanishRKBurghenGAet alHypothalamic dysfunction after chemotherapy. J Pediatr Endocrinol Metab (2004) 17:55–66.10.1515/JPEM.2004.17.1.55

  • CrossRef
  • Google Scholar

• 15

  GundgurthiAGargMKNairVPakhetraRDasSSharmaSet alEndocrine complications after busulphan and cyclophosphamide based hematopoietic stem cell transplant: a single tertiary care centre experience. Ind J Endocrinol Metab (2013) 17:855–63.10.4103/2230-8210.117248

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 16

  BakkerBOostdijkWBrestersDWalenkampMJVossenJMWitJM. Disturbances of growth and endocrine function after busulphan-based conditioning for haematopoietic stem cell transplantation during infancy and childhood. Bone Marrow Transplant (2004) 33:1049–56.10.1038/sj.bmt.1704481

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 17

  van den HeijkantSHoorweg-NijmanGHuismanJDrentMvan der PalHKaspersGJet alEffects of growth hormone therapy on bone mass, metabolic balance, and well-being in young adult survivors of childhood acute lymphoblastic leukemia. J Pediatr Hematol Oncol (2011) 33:e231–8.10.1097/MPH.0b013e31821bbe7a

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 18

  RastogiMVStorkLDrukerBBlasdelCNguyenTBostonBA. Imatinib mesylate causes growth deceleration in pediatric patients with chronic myelogenous leukemia. Pediatr Blood Cancer (2012) 59:840–5.10.1002/pbc.24121

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 19

  MarianiSGionaFBascianiSBramaMGnessiL. Low bone density and decreased inhibin-B/FSH ratio in a boy treated with imatinib during puberty. Lancet (2008) 372:111–2.10.1016/S0140-6736(08)61023-5

  • CrossRef
  • Google Scholar

• 20

  RosenfieldRLFurlanettoR. Physiologic testosterone or estradiol induction of puberty increases plasma somatomedin-C. J Pediatr (1985) 107:415–7.10.1016/S0022-3476(85)80522-9

  • CrossRef
  • Google Scholar

• 21

  IwayamaHKamijoTUedaN. Hyperinsulinemia may promote growth without GH in children after resection of suprasellar brain tumors. Endocrine (2011) 40:130–3.10.1007/s12020-011-9493-y

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 22

  SizonenkoPCClaytonPECohenPHintzRLTanakaTLaronZ. Diagnosis and management of growth hormone deficiency in childhood and adolescence. Part 1: diagnosis of growth hormone deficiency. Growth Horm IGF Res (2001) 11:137–65.10.1054/ghir.2001.0203

  • CrossRef
  • Google Scholar

• 23

  Growth Hormone Research Society. Consensus guidelines for the diagnosis and treatment of growth hormone (GH) deficiency in childhood and adolescence: summary statement of the GH Research Society. GH Research Society. J Clin Endocrinol Metab (2000) 85:3990–3.10.1210/jc.85.11.3990

  • CrossRef
  • Google Scholar

• 24

  SchriockEALustigRHRosenthalSMKaplanSLGrumbachMM. Effect of growth hormone (GH)-releasing hormone (GRH) on plasma GH in relation to magnitude and duration of GH deficiency in 26 children and adults with isolated GH deficiency or multiple pituitary hormone deficiencies: evidence for hypothalamic GRH deficiency. J Clin Endocrinol Metab (1984) 58:1043–9.

  • Pubmed Abstract
  • Google Scholar

• 25

  BlijdorpKvan den Heuvel-EibrinkMPietersRBootASluimerJvan der LelijAJet alThe limited screening value of insulin-like growth factor-I as a marker for alterations in body composition in very long-term adult survivors of childhood cancer. Pediatr Blood Cancer (2012) 59:711–6.10.1002/pbc.24015

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 26

  ChemaitillyWRobisonLL. Safety of growth hormone treatment in patients previously treated for cancer. Endocrinol Metab Clin North Am (2012) 41:785–92.10.1016/j.ecl.2012.07.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 27

  SklarCAMertensACMitbyPOcchiogrossoGQinJHellerGet alRisk of disease recurrence and second neoplasms in survivors of childhood cancer treated with growth hormone: a report from the childhood cancer survivor study. J Clin Endocrinol Metab (2002) 87:3136–41.10.1210/jcem.87.7.8606

  • CrossRef
  • Google Scholar

• 28

  SwerdlowAJReddingiusREHigginsCDSpoudeasHAPhippsKQiaoZet alGrowth hormone treatment of children with brain tumors and risk of tumor recurrence. J Clin Endocrinol Metab (2000) 85:4444–9.10.1210/jcem.85.12.7044

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 29

  KaravitakiNWarnerJTMarlandAShineBRyanFArnoldJet alGH replacement does not increase the risk of recurrence in patients with craniopharyngioma. Clin Endocrinol (2006) 64:556–60.10.1111/j.1365-2265.2006.02508.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 30

  Ergun-LongmireBMertensACMitbyPQinJHellerGShiWet alGrowth hormone treatment and risk of second neoplasms in the childhood cancer survivor. J Clin Endocrinol Metab (2006) 91:3494–8.10.1210/jc.2006-0656

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 31

  WoodmanseeWWZimmermannAGChildCJRongQErfurthEMBeck-PeccozPet alIncidence of second neoplasm in childhood cancer survivors treated with GH: an analysis of GeNeSIS and HypoCCS. Eur J Endocrinol (2013) 168:565–73.10.1530/EJE-12-0967

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 32

  PattersonBCChenYSklarCANegliaJYasuiYMertensAet alGrowth hormone exposure as a risk factor for the development of subsequent neoplasms of the central nervous system: a report from the Childhood Cancer Survivor Study. J Clin Endocrinol Metab (2014) 99:2030–7.10.1210/jc.2013-4159

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 33

  FollinCThilenUAhrenBErfurthEM. Improvement in cardiac systolic function and reduced prevalence of metabolic syndrome after two years of growth hormone (GH) treatment in GH-deficient adult survivors of childhood-onset acute lymphoblastic leukemia. J Clin Endocrinol Metab (2006) 91:1872–5.10.1210/jc.2005-2298

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 34

  MuirA. Precocious puberty. Pediatr Rev (2006) 27:373–81.10.1542/pir.27-10-373

  • CrossRef
  • Google Scholar

• 35

  PartschCJSippellWG. Treatment of central precocious puberty. Best Pract Res Clin Endocrinol Metab (2002) 16:165–89.10.1053/beem.2002.0188

  • CrossRef
  • Google Scholar

• 36

  ArmstrongGTWhittonJAGajjarAKunLEChowEJStovallMet alAbnormal timing of menarche in survivors of central nervous system tumors: a report from the childhood cancer survivor study. Cancer (2009) 115:2562–70.10.1002/cncr.24294

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 37

  OberfieldSESorannoDNirenbergAHellerGAllenJCDavidRet alAge at onset of puberty following high-dose central nervous system radiation therapy. Arch Pediatr Adolesc Med (1996) 150:589–92.10.1001/archpedi.1996.02170310023003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 38

  CarelJCLahlouNRogerMChaussainJL. Precocious puberty and statural growth. Hum Reprod Update (2004) 10:135–47.10.1093/humupd/dmh012

  • CrossRef
  • Google Scholar

• 39

  UruenaMStanhopeRChessellsJMLeiperAD. Impaired pubertal growth in acute lymphoblastic leukaemia. Arch Dis Child (1991) 66:1403–7.10.1136/adc.66.12.1403

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 40

  LeePA. Central precocious puberty. An overview of diagnosis, treatment, and outcome. Endocrinol Metab Clin North Am (1999) 28:901–18.10.1016/S0889-8529(05)70108-0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 41

  GreulichWWPyleSI. Radiographic Atlas of Skeletal Development of the Hand and Wrist. 2nd ed. Stanford, CA: Stanford University Press (1959).

  • Google Scholar

• 42

  HaberHPWollmannHARankeMB. Pelvic ultrasonography: early differentiation between isolated premature thelarche and central precocious puberty. Eur J Pediatr (1995) 154:182–6.10.1007/BF01954267

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 43

  GleesonHKStoeterROgilvy-StuartALGattamaneniHRBrennanBMShaletSM. Improvements in final height over 25 years in growth hormone (GH)-deficient childhood survivors of brain tumors receiving GH replacement. J Clin Endocrinol Metab (2003) 88:3682–9.10.1210/jc.2003-030366

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 44

  FernandezABradaMZabulieneLKaravitakiNWassJA. Radiation-induced hypopituitarism. Endocr Relat Cancer (2009) 16:733–72.10.1677/ERC-08-0231

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 45

  StephenMDZagePEWaguespackSG. Gonadotropin-dependent precocious puberty: neoplastic causes and endocrine considerations. Int J Pediatr Endocrinol (2011) 2011:184502.10.1155/2011/184502

  • CrossRef
  • Google Scholar

• 46

  RelanderTCavallin-StahlEGarwiczSOlssonAMWillenM. Gonadal and sexual function in men treated for childhood cancer. Med Pediatr Oncol (2000) 35:52–63.10.1002/1096-911X(200007)35:1<52::AID-MPO9>3.0.CO;2-Y

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 47

  ByrneJFearsTRMillsJLZeltzerLKSklarCMeadowsATet alFertility of long-term male survivors of acute lymphoblastic leukemia diagnosed during childhood. Pediatr Blood Cancer (2004) 42:364–72.10.1002/pbc.10449

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 48

  GreenfieldDMWaltersSJColemanREHancockBWEastellRDaviesHAet alPrevalence and consequences of androgen deficiency in young male cancer survivors in a controlled cross-sectional study. J Clin Endocrinol Metab (2007) 92:3476–82.10.1210/jc.2006-2744

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 49

  RoseSRDanishRKKearneyNSSchreiberRELustigRHBurghenGAet alACTH deficiency in childhood cancer survivors. Pediatr Blood Cancer (2005) 45:808–13.10.1002/pbc.20327

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 50

  LaughtonSJMerchantTESklarCAKunLEFouladiMBroniscerAet alEndocrine outcomes for children with embryonal brain tumors after risk-adapted craniospinal and conformal primary-site irradiation and high-dose chemotherapy with stem-cell rescue on the SJMB-96 trial. J Clin Oncol (2008) 26:1112–8.10.1200/JCO.2008.13.5293

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 51

  Ogilvy-StuartALClarkDJWallaceWHGibsonBEStevensRFShaletSMet alEndocrine deficit after fractionated total body irradiation. Arch Dis Child (1992) 67:1107–10.10.1136/adc.67.9.1107

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 52

  BilgirOKebapcilarLBilgirFSaríIOnerPKaracaBet alIs there any relationship between imatinib mesylate medication and hypothalamic-pituitary-adrenal axis dysfunction?Int J Clin Pract (2010) 64:45–50.10.1111/j.1742-1241.2008.01856.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 53

  BlansfieldJABeckKETranKYangJCHughesMSKammulaUSet alCytotoxic T-lymphocyte-associated antigen-4 blockage can induce autoimmune hypophysitis in patients with metastatic melanoma and renal cancer. J Immunother (2005) 28:593–8.10.1097/01.cji.0000178913.41256.06

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 54

  MakerAVYangJCSherryRMTopalianSLKammulaUSRoyalREet alIntrapatient dose escalation of anti-CTLA-4 antibody in patients with metastatic melanoma. J Immunother (2006) 29:455–63.10.1097/01.cji.0000208259.73167.58

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 55

  WeberJSDummerRde PrilVLebbeCHodiFSInvestigatorsMDX. Patterns of onset and resolution of immune-related adverse events of special interest with ipilimumab: detailed safety analysis from a phase 3 trial in patients with advanced melanoma. Cancer (2013) 119:1675–82.10.1002/cncr.27969

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 56

  ChrousosGPKinoTCharmandariE. Evaluation of the hypothalamic-pituitary-adrenal axis function in childhood and adolescence. Neuroimmunomodulation (2009) 16:272–83.10.1159/000216185

  • CrossRef
  • Google Scholar

• 57

  RoseSRLustigRHPitukcheewanontPBroomeDCBurghenGALiHet alDiagnosis of hidden central hypothyroidism in survivors of childhood cancer. J Clin Endocrinol Metab (1999) 84:4472–9.10.1210/jc.84.12.4472

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 58

  BouladFBromleyMBlackPHellerGSarafoglouKGillioAet alThyroid dysfunction following bone marrow transplantation using hyperfractionated radiation. Bone Marrow Transplant (1995) 15:71–6.

  • Pubmed Abstract
  • Google Scholar

• 59

  SchmiegelowMFeldt-RasmussenURasmussenAKPoulsenHSMullerJ. A population-based study of thyroid function after radiotherapy and chemotherapy for a childhood brain tumor. J Clin Endocrinol Metab (2003) 88:136–40.10.1210/jc.2002-020380

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 60

  SlawikMKlawitterBMeiserESchoriesMZwermannOBormKet alThyroid hormone replacement for central hypothyroidism: a randomized controlled trial comparing two doses of thyroxine (T4) with a combination of T4 and triiodothyronine. J Clin Endocrinol Metab (2007) 92:4115–22.10.1210/jc.2007-0297

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 61

  ConstineLSWoolfPDCannDMickGMcCormickKRaubertasRFet alHypothalamic-pituitary dysfunction after radiation for brain tumors. N Engl J Med (1993) 328:87–94.10.1056/NEJM199301143280203

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 62

  DarzyKHShaletSM. Pathophysiology of radiation-induced growth hormone deficiency: efficacy and safety of GH replacement. Growth Horm IGF Res (2006) 16(Suppl A):S30–40.10.1016/j.ghir.2006.03.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 63

  RamelliGPvon der WeidNStangaZMullisPEBuergiU. Suprasellar germinomas in childhood and adolescence: diagnostic pitfalls. J Pediatr Endocrinol Metab (1998) 11:693–7.10.1515/JPEM.1998.11.6.693

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 64

  SilfenMEGarvinJHJrHaysAPStarkmanHSAranoffGSLevineLSet alPrimary central nervous system lymphoma in childhood presenting as progressive panhypopituitarism. J Pediatr Hematol Oncol (2001) 23:130–3.10.1097/00043426-200102000-00013

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 65

  SpoudeasHA. Growth and endocrine function after chemotherapy and radiotherapy in childhood. Eur J Cancer (2002) 38:1748–59.10.1016/S0959-8049(02)00169-7

  • CrossRef
  • Google Scholar

• 66

  Di IorgiNNapoliFAllegriAEOlivieriIBertelliEGalliziaAet alDiabetes insipidus-diagnosis and management. Hormone Res Paediatr (2012) 77:69–84.10.1159/000336333

  • CrossRef
  • Google Scholar

• 67

  MishraGChandrashekharSR. Management of diabetes insipidus in children. Ind J Endocrinol Metab (2011) 15:S180–7.10.4103/2230-8210.84858

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 68

  ClementSCvan Eck-SmitBLvan TrotsenburgASKremerLCTytgatGAvan SantenHM. Long-term follow-up of the thyroid gland after treatment with 131I-Metaiodobenzylguanidine in children with neuroblastoma: importance of continuous surveillance. Pediatr Blood Cancer (2013) 60:1833–8.10.1002/pbc.24681

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 69

  HaugenBR. Drugs that suppress TSH or cause central hypothyroidism. Best Pract Res Clin Endocrinol Metab (2009) 23:793–800.10.1016/j.beem.2009.08.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 70

  ArmstrongGTStovallMRobisonLL. Long-term effects of radiation exposure among adult survivors of childhood cancer: results from the childhood cancer survivor study. Radiat Res (2010) 174:840–50.10.1667/RR1903.1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 71

  ChowEJFriedmanDLStovallMYasuiYWhittonJARobisonLLet alRisk of thyroid dysfunction and subsequent thyroid cancer among survivors of acute lymphoblastic leukemia: a report from the childhood cancer survivor Study. Pediatr Blood Cancer (2009) 53:432–7.10.1002/pbc.22082

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 72

  IllouzFBraunDBrietCSchweizerURodienP. Endocrine side-effects of anti-cancer drugs: thyroid effects of tyrosine kinase inhibitors. Eur J Endocrinol (2014) 171:R91–9.10.1530/EJE-14-0198

  • CrossRef
  • Google Scholar

• 73

  DesaiJYassaLMarquseeEGeorgeSFratesMCChenMHet alHypothyroidism after sunitinib treatment for patients with gastrointestinal stromal tumors. Ann Intern Med (2006) 145:660–4.10.7326/0003-4819-145-9-200611070-00008

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 74

  IllouzFLaboureau-SoaresSDuboisSRohmerVRodienP. Tyrosine kinase inhibitors and modifications of thyroid function tests: a review. Eur J Endocrinol (2009) 160:331–6.10.1530/EJE-08-0648

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 75

  IshiguroHYasudaYTomitaYShinagawaTShimizuTMorimotoTet alLong-term follow-up of thyroid function in patients who received bone marrow transplantation during childhood and adolescence. J Clin Endocrinol Metab (2004) 89:5981–6.10.1210/jc.2004-0836

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 76

  SandersJEHoffmeisterPAWoolfreyAECarpenterPAStorerBEStorbRFet alThyroid function following hematopoietic cell transplantation in children: 30 years’ experience. Blood (2009) 113:306–8.10.1182/blood-2008-08-173005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 77

  JungYJJeonYJChoWKLeeJWChungNGJungMHet alRisk factors for short term thyroid dysfunction after hematopoietic stem cell transplantation in children. Kor J Pediatr (2013) 56:298–303.10.3345/kjp.2013.56.7.298

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 78

  SklarCBouladFSmallTKernanN. Endocrine complications of pediatric stem cell transplantation. Front Biosci (2001) 6:G17–22.

  • Pubmed Abstract
  • Google Scholar

• 79

  AuWYLieAKKungAWLiangRHawkinsBRKwongYL. Autoimmune thyroid dysfunction after hematopoietic stem cell transplantation. Bone Marrow Transplant (2005) 35:383–8.10.1038/sj.bmt.1704766

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 80

  SavaniBNKoklanarisEKLeQShenoyAGoodmanSBarrettAJ. Prolonged chronic graft-versus-host disease is a risk factor for thyroid failure in long-term survivors after matched sibling donor stem cell transplantation for hematologic malignancies. Biol Blood Marrow Transplant (2009) 15:377–81.10.1016/j.bbmt.2008.11.032

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 81

  RiniBITamaskarIShaheenPSalasRGarciaJWoodLet alHypothyroidism in patients with metastatic renal cell carcinoma treated with sunitinib. J Natl Cancer Inst (2007) 99:81–3.10.1093/jnci/djk008

  • CrossRef
  • Google Scholar

• 82

  TorinoFBarnabeiAParagliolaRBaldelliRAppetecchiaMCorselloSM. Thyroid dysfunction as an unintended side effect of anticancer drugs. Thyroid (2013) 23:1345–66.10.1089/thy.2013.0241

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 83

  VeigaLHBhattiPRonckersCMSigurdsonAJStovallMSmithSAet alChemotherapy and thyroid cancer risk: a report from the childhood cancer survivor study. Cancer Epidemiol Biomarkers Prev (2012) 21:92–101.10.1158/1055-9965.EPI-11-0576

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 84

  ReulenRCFrobisherCWinterDLKellyJLancashireERStillerCAet alLong-term risks of subsequent primary neoplasms among survivors of childhood cancer. JAMA (2011) 305:2311–9.10.1001/jama.2011.747

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 85

  TaylorAJCroftAPPalaceAMWinterDLReulenRCStillerCAet alRisk of thyroid cancer in survivors of childhood cancer: results from the British childhood cancer survivor Study. Int J Cancer (2009) 125:2400–5.10.1002/ijc.24581

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 86

  BhattiPVeigaLHRonckersCMSigurdsonAJStovallMSmithSAet alRisk of second primary thyroid cancer after radiotherapy for a childhood cancer in a large cohort study: an update from the childhood cancer survivor study. Radiat Res (2010) 174:741–52.10.1667/RR2240.1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 87

  MetzgerMLHowardSCHudsonMMGowKWLiCSKrasinMJet alNatural history of thyroid nodules in survivors of pediatric Hodgkin lymphoma. Pediatr Blood Cancer (2006) 46:314–9.10.1002/pbc.20541

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 88

  SklarCWhittonJMertensAStovallMGreenDMarinaNet alAbnormalities of the thyroid in survivors of Hodgkin’s disease: data from the childhood cancer survivor study. J Clin Endocrinol Metab (2000) 85:3227–32.10.1210/jc.85.9.3227

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 89

  LandierWBhatiaSEshelmanDAForteKJSweeneyTHesterALet alDevelopment of risk-based guidelines for pediatric cancer survivors: the children’s oncology group long-term follow-up guidelines from the children’s oncology group late effects committee and nursing discipline. J Clin Oncol (2004) 22:4979–90.10.1200/JCO.2004.11.032

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 90

  BrignardelloECorriasAIsolatoGPalestiniNCordero di MontezemoloLFagioliFet alUltrasound screening for thyroid carcinoma in childhood cancer survivors: a case series. J Clin Endocrinol Metab (2008) 93:4840–3.10.1210/jc.2008-1528

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 91

  KovalchikSARonckersCMVeigaLHSigurdsonAJInskipPDde VathaireFet alAbsolute risk prediction of second primary thyroid cancer among 5-year survivors of childhood cancer. J Clin Oncol (2013) 31:119–27.10.1200/JCO.2012.41.8996

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 92

  Molgaard-HansenLSkouASJuulAGlosliHJahnukainenKJarfeltMet alPubertal development and fertility in survivors of childhood acute myeloid leukemia treated with chemotherapy only: a NOPHO-AML study. Pediatr Blood Cancer (2013) 60:1988–95.10.1002/pbc.24715

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 93

  RidolaVFawazOAubierFBergeronCde VathaireFPichonFet alTesticular function of survivors of childhood cancer: a comparative study between ifosfamide- and cyclophosphamide-based regimens. Eur J Cancer (2009) 45:814–8.10.1016/j.ejca.2009.01.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 94

  KenneyLBLauferMRGrantFDGrierHDillerL. High risk of infertility and long term gonadal damage in males treated with high dose cyclophosphamide for sarcoma during childhood. Cancer (2001) 91:613–21.10.1002/1097-0142(20010201)91:3<613::AID-CNCR1042>3.0.CO;2-R

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 95

  RomeriusPStåhlOMoëllCRelanderTCavallin-StåhlEWiebeTet alHypogonadism risk in men treated for childhood cancer. J Clin Endocrinol Metab (2009) 94:4180–6.10.1210/jc.2009-0337

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 96

  LodishMBStratakisCA. Endocrine side effects of broad-acting kinase inhibitors. Endocr Relat Cancer (2010) 17:R233–44.10.1677/ERC-10-0082

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 97

  LeiperADGrantDBChessellsJM. Gonadal function after testicular radiation for acute lymphoblastic leukaemia. Arch Dis Child (1986) 61:53–6.10.1136/adc.61.1.53

  • CrossRef
  • Google Scholar

• 98

  IzardMA. Leydig cell function and radiation: a review of the literature. Radiother Oncol (1995) 34:1–8.10.1016/0167-8140(94)01501-S

  • CrossRef
  • Google Scholar

• 99

  KenneyLBCohenLEShnorhavorianMMetzgerMLLockartBHijiyaNet alMale reproductive health after childhood, adolescent, and young adult cancers: a report from the Children’s Oncology Group. J Clin Oncol (2012) 30:3408–16.10.1200/JCO.2011.38.6938

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 100

  BramswigJHHeimesUHeiermannESchlegelWNieschlagESchellongG. The effects of different cumulative doses of chemotherapy on testicular function. Results in 75 patients treated for Hodgkin’s disease during childhood or adolescence. Cancer (1990) 65:1298–302.10.1002/1097-0142(19900315)65:6<1298::AID-CNCR2820650607>3.0.CO;2-W

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 101

  AfifyZShawPJClavano-HardingACowellCT. Growth and endocrine function in children with acute myeloid leukaemia after bone marrow transplantation using busulfan/cyclophosphamide. Bone Marrow Transplant (2000) 25:1087–92.10.1038/sj.bmt.1702384

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 102

  MeistrichML. Effects of chemotherapy and radiotherapy on spermatogenesis in humans. Fertil Steril (2013) 100:1180–6.10.1016/j.fertnstert.2013.08.010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 103

  GreenDMZhuLZhangNSklarCAKeRWKuttehWHet alLack of specificity of plasma concentrations of inhibin B and follicle-stimulating hormone for identification of azoospermic survivors of childhood cancer: a report from the St Jude lifetime cohort study. J Clin Oncol (2013) 31:1324–8.10.1200/JCO.2012.43.7038

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 104

  DubeyPWilsonGMathurKKHagemeisterFBFullerLMHaCSet alRecovery of sperm production following radiation therapy for Hodgkin’s disease after induction chemotherapy with mitoxantrone, vincristine, vinblastine, and prednisone (NOVP). Int J Radiat Oncol Biol Phys (2000) 46:609–17.10.1016/S0360-3016(99)00338-7

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 105

  Practice Committee of American Society for Reproductive M. Fertility preservation in patients undergoing gonadotoxic therapy or gonadectomy: a committee opinion. Fertil Steril (2013) 100:1214–23.10.1016/j.fertnstert.2013.08.012

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 106

  GoossensEVan SaenDTournayeH. Spermatogonial stem cell preservation and transplantation: from research to clinic. Hum Reprod (2013) 28:897–907.10.1093/humrep/det039

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 107

  ChemaitillyWMertensACMitbyPWhittonJStovallMYasuiYet alAcute ovarian failure in the childhood cancer survivor study. J Clin Endocrinol Metab (2006) 91:1723–8.10.1210/jc.2006-0020

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 108

  SklarCAMertensACMitbyPWhittonJStovallMKasperCet alPremature menopause in survivors of childhood cancer: a report from the childhood cancer survivor study. J Natl Cancer Inst (2006) 98:890–6.10.1093/jnci/djj243

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 109

  MichelGSociéGGebhardFBernaudinFThuretIVannierJPet alLate effects of allogeneic bone marrow transplantation for children with acute myeloblastic leukemia in first complete remission: the impact of conditioning regimen without total-body irradiation – a report from the Societe Francaise de Greffe de Moelle. J Clin Oncol (1997) 15:2238–46.

  • Pubmed Abstract
  • Google Scholar

• 110

  RivkeesSACrawfordJD. The relationship of gonadal activity and chemotherapy-induced gonadal damage. JAMA (1988) 259:2123–5.10.1001/jama.1988.03720140043031

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 111

  SklarC. Reproductive physiology and treatment-related loss of sex hormone production. Med Pediatr Oncol (1999) 33:2–8.10.1002/(SICI)1096-911X(199907)33:1<2::AID-MPO2>3.3.CO;2-Z

  • CrossRef
  • Google Scholar

• 112

  BrydoyMFossaSDDahlOBjoroT. Gonadal dysfunction and fertility problems in cancer survivors. Acta Oncol (2007) 46:480–9.10.1080/02841860601166958

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 113

  El-ShalakanyAHAliMSAbdelmaksoudAAAbd El-GhanySHasanEA. Ovarian function in female survivors of childhood malignancies. Pediatr Hematol Oncol (2013) 30:328–35.10.3109/08880018.2013.778927

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 114

  MatsumotoMShinoharaOIshiguroHShimizuTHattoriKIchikawaMet alOvarian function after bone marrow transplantation performed before menarche. Arch Dis Child (1999) 80:452–4.10.1136/adc.80.5.452

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 115

  SandersJEBucknerCDAmosDLevyWAppelbaumFRDoneyKet alOvarian function following marrow transplantation for aplastic anemia or leukemia. J Clin Oncol (1988) 6:813–8.

  • Google Scholar

• 116

  VisserJAde JongFHLavenJSThemmenAP. Anti-Mullerian hormone: a new marker for ovarian function. Reproduction (2006) 131:1–9.10.1530/rep.1.00529

  • CrossRef
  • Google Scholar

• 117

  Lie FongSLavenJSHakvoort-CammelFGSchipperIVisserJAThemmenAPet alAssessment of ovarian reserve in adult childhood cancer survivors using anti-Mullerian hormone. Hum Reprod (2009) 24:982–90.10.1093/humrep/den487

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 118

  DewaillyDAndersenCYBalenABroekmansFDilaverNFanchinRet alThe physiology and clinical utility of anti-Mullerian hormone in women. Hum Reprod Update (2014) 20:370–85.10.1093/humupd/dmt062

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 119

  NielsenSNAndersenANSchmidtKTRechnitzerCSchmiegelowKBentzenJGet alA 10-year follow up of reproductive function in women treated for childhood cancer. Reprod Biomed Online (2013) 27:192–200.10.1016/j.rbmo.2013.04.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 120

  GreenDMWhittonJAStovallMMertensACDonaldsonSSRuymannFBet alPregnancy outcome of female survivors of childhood cancer: a report from the childhood cancer survivor study. Am J Obstet Gynecol (2002) 187:1070–80.10.1067/mob.2002.126643

  • CrossRef
  • Google Scholar

• 121

  ReulenRCZeegersMPWallaceWHFrobisherCTaylorAJLancashireERet alPregnancy outcomes among adult survivors of childhood cancer in the British childhood cancer survivor study. Cancer Epidemiol Biomarkers Prev (2009) 18:2239–47.10.1158/1055-9965.EPI-09-0287

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 122

  AisenbergJHsiehKKalaitzoglouGWhittamEHellerGSchneiderRet alBone mineral density in young adult survivors of childhood cancer. J Pediatr Hematol Oncol (1998) 20:241–5.10.1097/00043426-199805000-00010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 123

  OstbergJEStorryCDonaldAEAttarMJHalcoxJPConwayGS. A dose-response study of hormone replacement in young hypogonadal women: effects on intima media thickness and metabolism. Clin Endocrinol (2007) 66:557–64.

  • Pubmed Abstract
  • Google Scholar

• 124

  Practice Committees of American Society for Reproductive Medicine, Society for Assisted Reproductive Technology. Mature oocyte cryopreservation: a guideline. Fertil Steril (2013) 99:37–43.10.1016/j.fertnstert.2012.09.028

  • CrossRef
  • Google Scholar

• 125

  SalaABarrRD. Osteopenia and cancer in children and adolescents: the fragility of success. Cancer (2007) 109:1420–31.10.1002/cncr.22546

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 126

  GurneyJGKasteSCLiuWSrivastavaDKChemaitillyWNessKKet alBone mineral density among long-term survivors of childhood acute lymphoblastic leukemia: results from the St. Jude Lifetime Cohort Study. Pediatr Blood Cancer (2014) 61:1270–6.10.1002/pbc.25010

  • CrossRef
  • Google Scholar

• 127

  te WinkelMLPietersRHopWCRoosJCBökkerinkJPLeeuwJAet alBone mineral density at diagnosis determines fracture rate in children with acute lymphoblastic leukemia treated according to the DCOG-ALL9 protocol. Bone (2014) 59:223–8.10.1016/j.bone.2013.11.017

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 128

  Pirker-FruhaufUMFriesenbichlerJUrbanECObermayer-PietschBLeithnerA. Osteoporosis in children and young adults: a late effect after chemotherapy for bone sarcoma. Clin Orthop Relat Res (2012) 470:2874–85.10.1007/s11999-012-2448-7

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 129

  Mostoufi-MoabSBrodskyJIsaacoffEJTsampalierosAGinsbergJPZemelBet alLongitudinal assessment of bone density and structure in childhood survivors of acute lymphoblastic leukemia without cranial radiation. J Clin Endocrinol Metab (2012) 97:3584–92.10.1210/jc.2012-2393

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 130

  OgdenCLCarrollMDKitBKFlegalKM. Prevalence of childhood and adult obesity in the United States, 2011-2012. JAMA (2014) 311:806–14.10.1001/jama.2014.732

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 131

  ParkMHFalconerCVinerRMKinraS. The impact of childhood obesity on morbidity and mortality in adulthood: a systematic review. Obes Rev (2012) 13:985–1000.10.1111/j.1467-789X.2012.01015.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 132

  WarnerELFluchelMWrightJSweeneyCBoucherKMFraserAet alA population-based study of childhood cancer survivors’ body mass index. J Cancer Epidemiol (2014) 2014:531958.10.1155/2014/531958

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 133

  SklarCAMertensACWalterAMitchellDNesbitMEO’LearyMet alChanges in body mass index and prevalence of overweight in survivors of childhood acute lymphoblastic leukemia: role of cranial irradiation. Med Pediatr Oncol (2000) 35:91–5.10.1002/1096-911X(200008)35:2<91::AID-MPO1>3.0.CO;2-G

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 134

  OeffingerKCMertensACSklarCAYasuiYFearsTStovallMet alObesity in adult survivors of childhood acute lymphoblastic leukemia: a report from the childhood cancer survivor study. J Clin Oncol (2003) 21:1359–65.10.1200/JCO.2003.06.131

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 135

  GarmeyEGLiuQSklarCAMeachamLRMertensACStovallMAet alLongitudinal changes in obesity and body mass index among adult survivors of childhood acute lymphoblastic leukemia: a report from the childhood cancer survivor study. J Clin Oncol (2008) 26:4639–45.10.1200/JCO.2008.16.3527

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 136

  LustigRHPostSRSrivannaboonKRoseSRDanishRKBurghenGAet alRisk factors for the development of obesity in children surviving brain tumors. J Clin Endocrinol Metab (2003) 88:611–6.10.1210/jc.2002-021180

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 137

  LustigRHHindsPSRingwald-SmithKChristensenRKKasteSCSchreiberREet alOctreotide therapy of pediatric hypothalamic obesity: a doubleblind, placebo-controlled trial. J Clin Endocrinol Metab (2003) 88:2586–92.10.1210/jc.2002-030003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 138

  MasonPWKrawieckiNMeachamLR. The use of dextroamphetamine to treat obesity and hyperphagia in children treated for craniopharyngioma. Arch Pediatr Adolesc Med (2002) 156:887–92.10.1001/archpedi.156.9.887

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 139

  MeachamLRSklarCALiSLiuQGimpelNYasuiYet alDiabetes mellitus in long-term survivors of childhood cancer. Increased risk associated with radiation therapy: a report from the childhood cancer survivor study. Arch Int Med (2009) 169:1381–8.10.1001/archinternmed.2009.209

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 140

  de VathaireFEl-FayechCBen AyedFFHaddyNGuiboutCWinterDet alRadiation dose to the pancreas and risk of diabetes mellitus in childhood cancer survivors: a retrospective cohort study. Lancet Oncol (2012) 13:1002–10.10.1016/S1470-2045(12)70323-6

  • Pubmed Abstract
  • CrossRef
  • Google Scholar