Ruptured Emphysematous Prostatic Abscess Caused by K1-ST23 Hypervirulent Klebsiella pneumoniae Presenting as Brain Abscesses: A Case Report and Literature Review

Abstract

Emphysematous prostatic abscess (EPA) is an extremely rare but potentially fatal urinary tract infection (UTI). Here, we describe a case (a 69-year-old male with prediabetes) of ruptured EPA caused by a hypervirulent Klebsiella pneumoniae (hvKp) K1-ST23 strain, presenting as motor aphasia. Our patient presented with ruptured EPA concurrent with various severe systemic pyogenic complications (e.g., urethro-prostatic fistula, ascending UTIs, epididymal and scrotal abscesses, and liver, lung, and brain abscesses). Whole-body computed tomography (CT) and next-generation sequencing (NGS) were useful for the detection of ruptured EPA and its systemic complications, and for identification of K1-ST23 hvKp strains, respectively. Subsequently, the infections were successfully treated with aggressive antimicrobial therapy and multiple surgical procedures. This case highlights the significance of awareness of this rare entity, the clinical importance of CT for the early diagnosis of EPA and the detection of its systemic complications in view of hvKp being an important causative organism of severe community-acquired UTI, and the usefulness of NGS to identify hvKp strains.

Introduction

Prostatic abscess is an uncommon sequela of urinary tract infection (UTI). In the post-antimicrobial era, the incidence is low at approximately 0.5% (1). Among them, emphysematous prostatic abscess (EPA), characterized by gas accumulation and abscess formation within the prostate gland, is an extremely rare but life-threatening condition if left untreated (2). However, an accurate diagnosis remains challenging because of the non-specific symptoms and signs.

Case Description

A 69-year-old Japanese man was admitted to our hospital with a 7-day history of slurred speech. He had no past history of prostatic manipulation. On admission, the patient had a low-grade fever of 37.8°C, tachycardia of 109 beats/min, blood pressure of 122/90 mmHg, and oxygen saturation of 97% on ambient air. Motor aphasia was recognized on neurologic examination. Digital rectal examination revealed a soft and non-tender enlarged prostate. Laboratory testing revealed neutrophilic leukocytosis, elevated levels of C-reactive protein (20.86 mg/dL; reference: <0.15 mg/dL), fasting blood glucose (135 mg/dL; reference: <110 mg/dL), and HbA1c (6.3%; reference: <6.0%). Mild hepatorenal dysfunction was also observed. Urinalysis was positive for bacteriuria and pyuria. Cerebrospinal fluid analysis was unremarkable. Brain computed tomography (CT) and magnetic resonance imaging (MRI) revealed a lesion in the left lenticular nucleus, suggestive of a brain abscess (Figures 1A,B). We subsequently searched for the cause of the brain abscess on a whole-body CT. Pelvic CT revealed an enlarged multilobular prostate gland characterized by capsulized fluid cavities and multiple gas bubbles, suggesting EPA caused by anaerobic bacteria (Figures 2A,B). We also recognized severe pyogenic complications of EPA, which were different from Fournier's gangrene. We classified a wide spectrum of complications into four predominant categories according to the route of spread of infection. We found direct extension as the 1st route, which involved spread into the left seminal vesicle and extraperitoneal space of the ischioanal fossa (Figures 2A,B), and an ascending infection of the ipsilateral urinary tract as the 2nd route, which caused left hydronephrosis, acute focal bacterial nephritis, and thrombophlebitis of the adjacent left iliac vein (Figures 2C,D). We also found a retrograde infection of the ipsilateral spermatic duct as the 3rd route, which led to an epididymal abscess (Figure 2A), and hematogenous spread to the liver (Figure 2E) and lungs (Figure 2F) as the 4th route. Pelvic MRI further characterized the pelvic infection and revealed active prostatic inflammation involving the urinary bladder and left seminal vesicles, which ruptured into the extraperitoneal perivesicular space, and subsequent fistula formation of the bulbar urethra with the prostate (Figure 3). Based on these findings, we concluded that brain abscess was highly likely due to hematogenous seeding of the primary prostate infection. We started to treat the pelvic infection with the insertion of a transurethral Foley catheter and commencement of empiric antimicrobial therapy (meropenem, 4 g/day IV).

Figure 1

Figure 2

Figure 3

On day 5, all the urine culture and two sets of blood cultures collected on admission yielded Klebsiella pneumoniae, which was susceptible to conventional antimicrobials, yet naturally resistant to ampicillin. Although the K. pneumoniae isolate was negative for the string test, we performed next-generation sequencing (NGS) for capsular genotyping, virulence factors, and multilocus sequencing typing (MLST). The isolate was found to belong to a sequence type (ST) 23 serotype K1 strain harboring virulence-associated genes, including kfuA (an iron uptake system), magA (specific to K1 capsule serotype), rmpA (regulator of mucoid phenotype), ybtS (yersiniabactin gene), iroN (gene for the outer membrane receptor, FepA, of Fe³⁺-bound salmochelin), and mrkD (type 3 fimbrial adhesin gene). Based on the antimicrobial susceptibility test results, antimicrobial de-escalation was performed (ciprofloxacin, 1,200 mg/day IV). On day 14, a left scrotal abscess developed progressively, presumably originating from the adjacent epididymal abscess, and required surgical drainage. On day 21, follow-up CT showed a decrease in the size of the EPA, and multiple intrapelvic abscesses, liver abscess, and pulmonary septic emboli.

However, on day 24, we performed an additional brain abscess drainage on a CT-guided stereotactic procedure because follow-up brain MRI confirmed a gradual progression of the existing brain abscess and multiple new ones (Figures 1C,D). Subsequently, the treatment was replaced with a 3-week course of intravenous ceftriaxone (3 g/day) and ciprofloxacin (1,200 mg/day). On follow-up CT/MRI, the brain abscesses gradually reduced in size. The patient continued rehabilitation for disuse syndrome and motor aphasia, and these improved with training. Fasting blood glucose levels after control of infection were in the range of 110–125 mg/dL, suggesting prediabetes. The patient was discharged on day 88. He remained clinically stable at 1-year follow-up. The timeline of the case presentation and clinical course is presented in Supplementary Figure 1.

Discussion

Herein, we describe a rare case of EPA caused by a hypervirulent K. pneumoniae (hvKp) K1-ST23 strain. Within a few days, the patient developed abscess rupture concurrent with various serious systemic pyogenic complications successfully treated with aggressive antimicrobial therapy and multiple surgical interventions. Our case illustrates several valuable clinical pearls.

First, our patient with EPA exhibited abscess rupture, leading to a variety of serious systemic pyogenic complications. We conducted an updated systematic review of case reports to investigate the characteristics and epidemiology of EPA (Table 1). The literature search was performed with English language restriction using electronic databases of PubMed from January 1, 1983, until July 28, 2021. The following search terms were used: “emphysematous prostatic abscess” (Mesh) or “emphysematous prostatic abscess” (tiab) or “emphysematous prostatitis” (Mesh) or “emphysematous prostatitis” (tiab). Consequently, 22 cases were included (2–21). EPA is most often diagnosed in Asia (68%), with an average age of 60 years (range, 35–75 years). The underlying disease was diabetes mellitus (96%), followed by liver cirrhosis (27%), recent urological surgery (23%), and alcoholism (18%). Unlike prostatic abscess, in which Escherichia coli is the main causative organism; the most common causative organism of EPA is K. pneumoniae (50%), followed by Escherichia coli (18%) and Candida albicans (14%). EPA is often misdiagnosed as the usual type of UTI, leading to time delay (range, 4–12 days) in the accurate diagnosis and proper treatment. EPA can have a variable presentation, ranging from asymptomatic to lethal. Frequent complications of EPA include localized spread of infection to adjacent areas, ascending infections, or disseminated hematogenous spread. Although rare, the most feared sequelae include a urethro-prostatic fistula or abscess rupture into the urethra, perineum, bladder, or rectum (13, 22). Metastatic infections are common (55%), with a high mortality rate of 23%. CT is the most useful diagnostic imaging tool. The mainstay of treatment includes adequate antimicrobial therapy and drainage; in 86% of cases, surgical drainage was performed using a transperineal (45%), transurethral (41%), or transrectal (9%) approach. Suprapubic cystostomy is often performed for urinary diversion (45.4%).

The present case presented with systemic complications via all the aforementioned routes of infection. Despite fatal complications (e.g., urethro-prostatic fistula, epididymal and scrotal abscesses, and metastatic hepatic/pulmonary/brain abscesses), CT/MRI screening was useful for early detection, and the infection was successfully controlled by aggressive antimicrobial therapy and multiple surgical drainage procedures.

Second, our case underscores the significance of early diagnosis of invasive K. pneumoniae infections in healthy subjects. The hvKp is a major causative agent in invasive community-acquired infections characterized by pyogenic liver abscess (PLA) with a high mortality, and has been reported in the Asian Pacific Rim, starting in Taiwan since the 1980s, and is now spreading worldwide (23). The hvKp strain has a much more vicious phenotype than the classical K. pneumoniae (cKp) strain due to its high toxicity and metastatic potential, resulting in grave secondary infections such as endophthalmitis, meningitis, and septic pulmonary emboli. Thus, early diagnosis and prompt treatment are required; however, the following three clinical issues for hvKp infection were exemplified by our case.

As the first clinical issue, hvKp-related primary extrahepatic genitourinary infections are increasingly being reported. Although the exact pathogenesis of hvKp remains unknown, many studies have indicated that hvKp initially colonizes the gastrointestinal tract, from where it preferentially infects other organs, mainly the liver. Therefore, UTI caused by hvKp has been considered secondary to hematogenous spread from preceding bacteremia. In fact, there are several reported cases of PLA with hematogenous spread to the kidney, perirenal tissues, and prostate, leading to local abscess formation (23). Conversely, several hvKp cases with community-acquired UTIs without PLA have also been reported (24–26). Similarly, the main source of infection in our case was the prostate gland, and concomitant liver abscess was highly likely secondary to the primary prostatic infection. Thus, our case underscores the importance of considering the possibility of hvKp infection even in patients with community-acquired UTIs.

The second clinical issue concerns the significance of serotype K1 K. pneumoniae in our case. To our knowledge, the present case is the first case of EPA caused by serotype K1 hvKp infection presenting with a brain abscess. The K1 strain has a strong propensity to cause metastatic ocular and neurologic complications. In a single-center, retrospective study of 177 patients with PLA in Taiwan, the incidence of metastatic complications was 13% (27). The frequency of metastatic complications was significantly higher in patients with K1 strains than in patients with non-K1 strains (19 vs. 5%, p = 0.007). Multivariate logistic regression analyses demonstrated that the K1 strain was the sole significant risk factor for metastatic complications (adjusted odds ratio, 4.8; 95% confidence interval, 1.5–15.7, p = 0.009), strongly suggesting that the K1 strains should be recognized as a distinct virulent organism. In addition, such metastatic complications have been reported in patients with K1 strains without hepatic involvement, suggesting that their development is unrelated to the presence of PLA (25, 26). Thus, our case highlights the importance of considering serotype K1 hvKp as a rare causative agent of community-acquired brain abscess and of screening for the primary site of infection.

The third clinical issue is to identify a hvKp strain definitely. Although numerous studies have been conducted to differentiate hvKp strains from cKp strains in terms of epidemiologic and genetic differences, there are still no clear microbiological and molecular diagnostic criteria for hvKp strains. A positive string test, indicating a hypermucoviscous colony phenotype on the agar plate, is widely believed to be a unique characteristic of hvKp strains. However, hypermucoviscosity and hypervirulence do not always coincide, as shown by the fact that there are both string test-negative hvKp strains and string test-positive cKp strains. A study evaluating 140 cases of K. pneumoniae bloodstream infections revealed that the string test alone is not adequate to differentiate hvKp strains from cKp strains (69.2% sensitivity, 89.5% specificity, 60.0% positive predictive value, and 92.7% negative predictive value), supporting this notion (28). The hvKp strains have some capsular types necessary for their virulence, with K1/K2 capsular serotypes being the most prevalent and virulent reported to date. Regarding virulence-associated genes, rmpA is remarkably related to the hvKp strain (29). Type 1 and type 3 fimbriae are deeply involved in bacterial resistance to phagocytosis, adhesion to biological/non-biological surfaces, and altered antibiotic permeability. Iron is a metal necessary for bacterial growth and plays an important role in infection spread, and siderophores (aerobactin, enterobactin, salmochelin, and yersiniabactin), secreted by K. pneumoniae, have the ability to sequester iron, contributing to their high virulence. However, while all the factors described above play important roles in the process of increased virulence, no single causal risk factor alone is the sole determinant of hypervirulence. Recently, a new genotype/phenotype approach for the comprehensive detection of a specific set of biomarkers has been proposed for the successful identification of hvKp strains (30). Further investigation is expected to accumulate in the future. In our case, NGS was useful for identifying the hvKp strain because it allows simultaneous analysis of MLST and virulence-associated genes, belongs to a K1-ST23 hvKp strain, and has the same profile of virulence-associated genes as the K1-ST23 hvKp strains previously identified in Japan, suggesting high genetic similarity (31). In our case review, only one case of EPA caused by the serotype K1 hvKp strain has been reported (Table 1). Given the high incidence of K. pneumoniae pathogens in EPA patients and the highly invasive nature of EPA, a thorough investigation of these strains is warranted.

Untreated glucose intolerance might have contributed to the virulent phenotype observed in our case, since hyperglycemia impairs neutrophil phagocytosis of K1/K2 capsular serotypes (32).

Conclusions

Herein, we report a case of ruptured EPA secondary to K1-ST23 hvKp infection with serious systemic pyogenic complications that was successfully treated with aggressive antimicrobial therapy and multiple surgical procedures. CT is useful for the accurate diagnosis and early detection of complications. EPA is an extremely rare, yet potentially fatal sequela of UTI, which can be curable if treated properly at an early stage. Therefore, clinicians should recognize this rare clinical entity and perform systemic CT screening in patients with potentially severe UTI. In addition, our case highlights the clinical importance of keeping in mind hvKp infections as a possible cause of community-acquired UTI in immunocompromised individuals including prediabetes, and of NGS to identify hvKp strains for appropriate treatment.

Funding

Next-generation sequencing experiments were funded by the Nagoya University Graduate School of Medicine, under Grant [Japan Agency for Medical Research and Development (AMED)/16fk0108307h0402]. Other parts of this study were not funded by any institution.

Publisher's Note

All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.

References

• 1.

  AckermanALParameshwarPSAngerJT. Diagnosis and treatment of patients with prostatic abscess in the post-antibiotic era. Int J Urol. (2018) 25:103–10. 10.1111/iju.13451

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 2.

  KuoPHHuangKHLeeCWLeeWJChenSJLiuKL. Emphysematous prostatitis caused by Klebsiella pneumoniae. J Formos Med Assoc. (2007) 106:74–7. 10.1016/S0929-6646(09)60219-9

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 3.

  MarianiAJJacobsLDClappPRHariharanAStamsUKHodgesCV. Emphysematous prostatic abscess: diagnosis and treatment. J Urol. (1983) 129:385–6. 10.1016/S0022-5347(17)52112-6

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 4.

  BartkowskiDPLaneskyJR. Emphysematous prostatitis and cystitis secondary to Candida albicans. J Urol. (1988) 139:1063–5. 10.1016/S0022-5347(17)42774-1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 5.

  LuDCLeiMHChangSC. Emphysematous prostatic abscess due to Klebsiella pneumoniae. Diagn Microbiol Infect Dis. (1998) 31:559–61. 10.1016/S0732-8893(98)00032-7

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 6.

  LinDCLinYMTongYC. Emphysematous prostatic abscess after transurethral microwave thermotherapy. J Urol. (2001) 166:625. 10.1097/00005392-200108000-00059

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 7.

  BaeGBKimSWShinBCOhJTDoBHParkJHet al. Emphysematous prostatic abscess due to Klebsiella pneumoniae: report of a case and review of the literature. J Korean Med Sci. (2003) 18:758–60. 10.3346/jkms.2003.18.5.758

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 8.

  SampathkumarKMuraliTRSoorajYSMahaldarAR. Emphysematous prostatitis in renal transplant. Indian J Urol. (2007) 23:476–8. 10.4103/0970-1591.36728

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 9.

  TaiHC. Emphysematous prostatic abscess: a case report and review of literature. J Infect. (2007) 54:e51–4. 10.1016/j.jinf.2006.03.033

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 10.

  JuanYSHuangCHChangKWangCJChuangSMShenJTet al. Emphysematous prostatic abscess due to candidiasis: a case report. Kaohsiung J Med Sci. (2008) 24:99–102. 10.1016/S1607-551X(08)70104-9

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 11.

  ThornerDASfakianosJPCabreraFLangEKColonI. Emphysematous prostatitis in a diabetic patient. J Urol. (2010) 183:2025. 10.1016/j.juro.2010.01.084

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 12.

  CheungWKTsangYM. Emphysematous infections of the prostate and scrotum in an older adult in a nursing home. J Am Geriatr Soc. (2011) 59:2378–9. 10.1111/j.1532-5415.2011.03710.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 13.

  WenSCJuanYSWangCJChangKoShihMCPShenJTet al. Emphysematous prostatic abscess: case series study and review. Int J Infect Dis. (2012) 16:e344–9. 10.1016/j.ijid.2012.01.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 14.

  HsuLNChiangPHKangCH. Emphysematous prostatic abscess: rare case and systematic review. J Formos Med Assoc. (2015) 114:292–3. 10.1016/j.jfma.2013.07.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 15.

  LeeCYTsaiHCLeeSSJChenYS. Concomitant emphysematous prostatic and periurethral abscesses due to Klebsiella pneumoniae: a case report and review of the literature. Southeast Asian J Trop Med Public Health. (2014) 45:1099–106.

  • Pubmed Abstract
  • Google Scholar

• 16.

  WangHSShihMC. Images in clinical medicine. Emphysematous prostatitis. N Engl J Med. (2016) 375:879. 10.1056/NEJMicm1507124

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 17.

  SuzukiKYamaguchiTYanaiM. Simultaneous occurrence of hypermucoviscous Klebsiella pneumoniae emphysematous prostatic abscess, emphysematous cystitis, and renal abscess. ID Cases. (2018) 14:e00464. 10.1016/j.idcr.2018.e00464

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 18.

  LiZWenJZhangN. Emphysematous prostatic abscess due to candidiasis: a case report and review of the literature. Medicine. (2020) 99:e19391. 10.1097/MD.0000000000019391

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 19.

  MetriMKalraSNarayananDLRamanitharanMKsS. Emphysematous prostatitis with secondary psoas abscess-a lethal outcome following prostate biopsy. Urology. (2020) 142:e45–6. 10.1016/j.urology.2020.04.085

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 20.

  MayoufSFouratiMBchirSKammounOMseddiMASlimenMH. Emphysematous prostatitis: a case report. Urol Case Rep. (2020) 34:101459. 10.1016/j.eucr.2020.101459

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 21.

  CraneABDiazMCAJiangYPergamentKM. Rare case of endogenous Klebsiella endophthalmitis associated with emphysematous prostatitis in a patient with diabetes, cirrhosis and COVID-19. BMJ Case Rep. (2021) 14:e240425. 10.1136/bcr-2020-240425

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 22.

  GargPKHadkeNS. Prostato-ano-cutaneous fistula: unusual complication of prostatic abscess. ANZ J Surg. (2008) 78:1032–3. 10.1111/j.1445-2197.2008.04727.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 23.

  RussoTAMarrCM. Hypervirulent Klebsiella pneumoniae. Clin Microbiol Rev. (2019) 32:e00001–19. 10.1128/CMR.00001-19

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 24.

  SuzukiKNakamuraAEnokiyaTIwashitaYTomatsuEMurakiYet al. Septic arthritis subsequent to urosepsis caused by hypermucoviscous Klebsiella pneumoniae. Intern Med. (2013) 52:1641–5. 10.2169/internalmedicine.52.0175

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 25.

  DubeyDRazaFSSawhneyAPandeyA. Klebsiella pneumoniae renal abscess syndrome: a rare case with metastatic involvement of lungs, eye, and Brain. Case Rep Infect Dis. (2013) 2013:685346. 10.1155/2013/685346

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 26.

  HyunJIKimYJJeonYHKimSIParkYJKangMWet al. A case of ventriculitis associated with renal abscess caused by serotype K1 Klebsiella pneumoniae. Infect Chemother. (2014) 46:120–4. 10.3947/ic.2014.46.2.120

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 27.

  FangCTLaiSYYiWCHsuehPRLiuKLChangSC. Klebsiella pneumoniae genotype K1: an emerging pathogen that causes septic ocular or central nervous system complications from pyogenic liver abscess. Clin Infect Dis. (2007) 45:284–93. 10.1086/519262

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 28.

  HaradaSAokiKYamamotoSIshiiYSekiyaNKuraiHet al. Clinical and molecular characteristics of klebsiella pneumoniae isolates causing bloodstream infections in Japan: occurrence of hypervirulent infections in health care. J Clin Microbiol. (2019) 57:e01206–19. 10.1128/JCM.01206-19

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 29.

  YuWLKoWCChengKCLeeHCKeDSLeeCCet al. Association between rmpA and magA genes and clinical syndromes caused by Klebsiella pneumoniae in Taiwan. Clin Infect Dis. (2006) 42:1351–8. 10.1086/503420

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 30.

  RussoTAOlsonRFangCTStoesserNMillerMMacDonaldUet al. Identification of biomarkers for differentiation of hypervirulent Klebsiella pneumoniae from Classical K. pneumoniae. J Clin Microbiol. (2018) 56:e00776–18. 10.1128/JCM.00776-18

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 31.

  HaradaSIshiiYSagaTAokiKTatedaK. Molecular epidemiology of Klebsiella pneumoniae K1 and K2 isolates in Japan. Diagn Microbiol Infect Dis. (2018) 91:354–9. 10.1016/j.diagmicrobio.2018.03.010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 32.

  LinJCSiuLKFungCPTsouHHWangJJChenCTet al. Impaired phagocytosis of capsular serotypes K1 or K2 Klebsiella pneumoniae in type 2 diabetes mellitus patients with poor glycemic control. J Clin Endocrinol Metab. (2006) 91:3084–7. 10.1210/jc.2005-2749

  • Pubmed Abstract
  • CrossRef
  • Google Scholar