Introduction

Front. Psychiatry

Frontiers in Psychiatry

Front. Psychiatry

1664-0640

Frontiers Media S.A.

10.3389/fpsyt.2013.00150

Psychiatry

Review Article

Similar and Different Gray Matter Deficits in Schizophrenia Patients and Their Unaffected Biological Relatives

Xiao

Yuan

¹ ^† Zhang

Wenjing

¹ ^† Lui

¹ * Yao

¹ Gong

Qiyong

¹ *

¹Department of Radiology, Huaxi MR Research Center (HMRRC), West China Hospital, Sichuan University, Chengdu, China

Edited by: Stefan Borgwardt, University of Basel, Switzerland

Reviewed by: Wi Hoon Jung, Seoul National University, South Korea; Kerstin Bendfeldt, University Basel, Switzerland

*Correspondence: Su Lui and Qiyong Gong, Department of Radiology, Huaxi MR Research Center (HMRRC), West China Hospital, Sichuan University, No. 37, Guoxue Xiang, Chengdu 610041, China e-mail: lusuwcums@tom.com; qiyonggong@hmrrc.org.cn

^†Yuan Xiao and Wenjing Zhang have contributed equally to this work.

This article was submitted to Neuropsychiatric Imaging and Stimulation, a section of the journal Frontiers in Psychiatry.

02 10 2013

21 11 2013

2013

150

16 09 2013 07 11 2013

2013

This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

Neuroimaging studies have revealed significant reductions in the gray matter (GM) of several brain regions in patients with schizophrenia, a neuropsychiatric disorder with high hereditability. However, it is unclear whether unaffected relatives have GM abnormalities in common with their affected relatives, which may relate to susceptibility to developing schizophrenia. To address this issue, we conducted two separate meta-analyses of voxel-based morphometry to investigate GM abnormalities in schizophrenia patients and their unaffected relatives. One meta-analysis compared a patient group with healthy controls, whereas the other meta-analysis compared the unaffected relatives with healthy controls. Eight studies comprising 495 patients with schizophrenia, 584 unaffected relatives of patients, and 596 healthy controls were systematically included in the present study. Compared to healthy controls, the patient group showed decreased GM in the right cuneus, the right superior frontal gyrus, the right insula and the left claustrum, and increased GM in the bilateral putamen, the right parahippocampal gyrus, the left precentral gyrus, the left inferior temporal gyri, and the right cerebellar tonsil. The comparison between unaffected relatives and healthy controls showed a GM reduction in the left claustrum, the bilateral parahippocampal gyri, the left fusiform gyrus, the right inferior temporal gyrus, and the bilateral medial prefrontal cortices, whereas increased GM was observed in the right hippocampus, the right fusiform gyrus, the right precentral gyrus, and the right precuneus. Thus, our meta-analyses show that the GM changes in schizophrenia patients and their unaffected relatives are largely different, although there is subtle overlap in some regions.

schizophrenia unaffected relatives MRI voxel-based morphometry gray matter meta-analysis

Introduction

Anatomical brain abnormalities have been well established in schizophrenia (1, 2). However, the molecular mechanism that underlies anatomical brain abnormalities in schizophrenia remains unclear, and an important question is whether these abnormalities are related to the illness itself or are linked to genetic risk, as an endophenotype (3). Characterizing endophenotypes is a compelling venture because endophenotypes may represent less complex disease antecedents that are easier to study than the illness syndrome itself. As many brain structures are highly heritable (4) and are influenced by genetic variants that are beginning to emerge in large-scale studies (5), brain structures may be a good endophenotype (3). Previous studies of unaffected relatives of schizophrenia patients demonstrated gray matter (GM) abnormalities that were similar but less pronounced than those in the patients, suggesting that the abnormalities are related to genetic susceptibility to the disorder (6, 7).

The majority of previous morphometric studies, however, studied schizophrenia patients and their unaffected relatives separately. Decreased GM volume in the left superior temporal gyrus and the left medial temporal lobe were the most common findings in the comparative studies of patients with schizophrenia and healthy controls with no personal or family history of psychosis (2). However, the results observed in such comparisons may reflect a complex combination of multiple causes, such as genetics, substance abuse, environmental factors, obstetric complications and birth injuries (8, 9), and other factors secondary to the illness. Indeed, whether these changes are the result of the use of antipsychotic medication or the severity of the illness itself is a matter of debate. However, studying unaffected relatives avoids the confounding factors of chronicity and antipsychotic medication. Furthermore, this population is independent of psychosis, thus avoiding the possible neurotoxic effects of psychosis, which may be present even in high-risk populations. Finally, a focus on unaffected relatives makes it possible to study genetic factors and environmental factors with respect to their roles in schizophrenia etiology (1). The most commonly reported abnormal brain region in unaffected relatives is the hippocampus, which was confirmed in a meta-analysis of non-psychotic first-degree relatives of schizophrenia patients (10). However, it should be noted that the hippocampus is also one of the most commonly investigated brain regions in studies of unaffected relatives of schizophrenia patients using region-of-interest (ROI) analysis. Only a few studies have employed whole-brain data-driven unbiased methods, such as voxel-based morphometry (VBM), which performs voxel-wise comparisons of gray and white matter probabilities between groups of subjects. The most common findings in whole-brain comparison studies comparing unaffected relatives with healthy controls involve the left putamen/globus pallidus (basal ganglia), the amygdala, and the parahippocampal gyrus (11), which are similar to the results of studies involving patients. However, one important problem with independent studies of patients and unaffected relatives is that the patients and unaffected relatives are not biologically related; thus, one cannot conclude from these studies whether the patients share anatomical deficits with their unaffected relatives. Only a few studies have explored whole-brain anatomical deficits in both patients and their unaffected biological relatives (6, 7, 12–17), but the findings are inconsistent. Hu et al. (17) found that untreated patients with first-episode schizophrenia and their unaffected siblings shared decreases of GM in the left middle temporal gyrus. A study of discordant monozygotic twins found that non-psychotic twins showed no significant differences in regional GM relative to the healthy control twins, although twins with schizophrenia had smaller GM in the insula, superior/medial frontal, pre/postcentral, cingulate, and superior temporal gyri compared to healthy control twins (13). Negative results of GM in first-degree relatives were also found in another study (12), though patients with schizophrenia reported reduced GM primarily in the anterior cingulate gyrus and the insula. In an optimized VBM study, Honea et al. (14) investigated a large group of patients and their unaffected siblings and found that siblings tended to share GM decreases in the medial frontal, superior temporal, and insular cortices with their affected siblings, but these decreases were not significant after multiple comparison correction.

Thus, the aims of the present meta-analysis were to determine whether schizophrenia patients and their unaffected biological relatives have GM abnormalities and if so, to map the common and the different alterations of GM between both groups.

Materials and Methods Selection procedures

Studies were selected using a systematic search strategy. Two independent researchers conducted a two-step literature review process. First, we performed a database search to find putative VBM studies. The keywords included (1) schizophrenia, (2) families or relatives or sibling or parents or offspring or twins, (3) structural MRI, (4) VBM or voxel-based analysis. These items were entered in various combinations when searching. Only articles published in print or online before July 2013 in English were selected using two databases (Pubmed and Medline). Second, the reference lists of the selected articles and similar studies were manually checked for additional studies that fit these criteria but that were not identified by our computerized searching process. We included all studies that met the following criteria: (a) an original paper in a peer-reviewed journal; (b) investigating GM volume or GM density/concentration by VBM at the whole-brain level among schizophrenia patients, their relatives or siblings and healthy controls; and (c) use of Montreal Neurological Institute (MNI) or Talairach coordinates in the VBM analyses. Studies that had overlapping samples were excluded. Studies lacking biological relatives of patients with schizophrenia were also excluded. The relatives investigated in each study were supposed to come from the studied patients’ own families, not from other families with a history of schizophrenia. We contacted the corresponding authors for details required for the present meta-analysis. In our present meta-analysis, Meta-analysis Of Observational Studies in Epidemiology (MOOSE) guidelines are followed (18).

Voxel-based meta-analysis

Prior to conducting the voxel-based meta-analysis, we extracted peak coordinates resulting from VBM analyses across the whole-brain and then excluded those coordinates using partial coverage, ROIs, or small volume correction (SVCs). This approach ensured that the studies we collected were comparable and that their purpose was to localize GM alterations across the entire cortex. Within each included study, the same statistical threshold used throughout the whole-brain was carefully checked to avoid biases toward liberally thresholded brain regions, as it is not uncommon in neuroimaging studies that the statistical thresholds for some ROI are more liberal than for the rest of the brain (19).

The Effect-Size Signed Differential Mapping (ES-SDM) (http://www.sdmproject.com/software), which is a new version of SDM, was chosen as our primary meta-analytical software (20). ES-SDM has several advantages over other voxel-based methods. First, the criterion that ES-SDM uses for selecting reported peak coordinates is so strict that it ensures that only regions with statistical significance at the whole-brain level will be considered in the meta-analysis, which prevents biases resulting from methods using liberal thresholds and ROI methods in neuroimaging studies (19). Second, previous methods such as activation likelihood estimation (ALE) (21) and multilevel kernel density analysis (MKDA) (22) only need reported peak coordinates. As for the ES-SDM, the use of effect-size enables combination of reported peak coordinates with statistical parametric maps allowing more detailed and accurate meta-analysis (20). Third, to avoid any voxel appearing significant in opposite directions, ES-SDM permits the representation of both GM increases and decreases in the same map. Last, complementary analyses such as jack-knife, subgroup, and meta-regression analyses are readily used to assess the robustness and heterogeneity of the results (20).

Two meta-analyses were conducted separately to describe differences in GM between patients and healthy controls and between relatives and healthy controls. A Gaussian kernel of 20 mm half-width was employed to assign indicators of proximity to the reported coordinates as it can optimally balance sensitivity and specificity in ES-SDM (20). A systematic voxel-based leave-one-out jack-knife analysis was also conducted to test the replicability of the results in various combinations of the included studies. The findings might be highly conclusive and replicable if previous significant ES-SDM results could be replicated in all or most study combinations. The standard ES-SDM thresholds (uncorrected P < 0.005, extent threshold of clusters >10 voxels) which were proposed to optimally balance the sensitivity and specificity and to be an approximate equivalent to corrected P-value = 0.05 in ES-SDM for effect-size were used (20).

Results Included studies

The search flow diagram is shown in Figure 1. Of the 159 initial hits identified by the database search, 127 articles were excluded for not using VBM or voxel-based analysis, by reading their abstracts. Of the remaining 32 articles, 25 did not meet the predefined inclusion criteria (because of factors such as carrying out only white matter analysis, lack of information or data from relatives of patients with schizophrenia, use of overlapping samples). The other seven articles were shortlisted for using VBM to investigate GM changes in patients, unaffected relatives, and healthy controls. However, further investigation revealed that in one of the seven articles, the relatives investigated were not from the investigated patients’ families, but from other families. The remaining six articles, together with two articles identified from the reference lists, comprised the final list of eight articles to be included. Seven of eight studies included different types of first-degree relatives, namely, one of monozygotic discordant twins (13), three of siblings (12, 14, 17), two of parents (7, 15), one of both parents and siblings (6). Only one study included the first- and second-degree of relatives (16). Among the included articles, four utilized GM density while the other four utilized GM volume to measure differences between groups. A total of 495 patients with schizophrenia, 584 relatives of patients, and 596 healthy controls were included. All of the studies included both types of VBM comparison (i.e., patients vs. controls and relatives vs. controls). In addition, Lui et al. (15) distinguished patients with familial schizophrenia from patients with sporadic illness and no family history. Thus, Lui et al. provided two VBM comparisons for each group, because the two groups of patients and relatives were separately compared with healthy controls. Consequently, each meta-analysis contained nine datasets. The demographic characteristics of the patients, relatives of patients with schizophrenia, and healthy controls are presented in Tables 1 and 2.

Figure 1

Flow diagram of inclusion and exclusion criteria for the meta-analysis.

Table 1

Demographic characteristics of the studies comparing schizophrenia patients and healthy controls.

Study	Sample size		Age in years (SD)		Male in proportions (%)		GM types of VBM	MRI strength	Smoothing FWHM	Medication
	Pat	Con	Pat	Con	Pat	Con
(17)	51	59	22.29 (3.95)	23.2 (2.58)	66.7	64.4	GM volume	3 T	8 mm	N^b
(6)	31	37	38.0 (11.24)	39.36 (9.97)	51.6	45.9	GM volume	3 T	8 mm	Y
(12)	155	122	26.91 (5.6)	27.5 (8.2)	80.65	50	GM density	1.5 T	4 mm	Y
(7)	30	30	22.63 (3.76)	22.77 (3.34)	56.7	60.0	GM density	3 T	6 mm	Y
(13)	9	34	33.8 (13.1)	39.3 (9.5)	66.7	70.6	GM volume	1.5 T	8 mm	Y
(15)^a	10	10	22.0 (8.2)	23.0 (7.9)	50	50	GM density	3 T	8 mm	N
(15)^a	10	10	21.2 (7.5)	23.0 (7.9)	50	50	GM density	3 T	8 mm	N
(14)	169	212	36.39 (9.46)	33.31 (9.86)	78.2	48.6	GM volume	1.5 T	10 mm	Y
(16)	26	49	36.85 (13.7)	35.27 (11.1)	50	46.9	GM density	1.5 T	12 mm	Y

(1) ^aTwo independent VBM comparisons between patients and healthy controls were conducted by Lui et al.

(2) ^bN, patients without medication; Y, patients medicated with antipsychotics.

(3) Pat, patients; Con, controls; SD, standard deviation; VBM, voxel-based morphometry; GM, gray matter; FWHM, full-width at half-maximum.

Table 2

Demographic characteristics of the studies comparing relatives of patients with schizophrenia and healthy controls.

Study	Sample size		Age in years(SD)		Male in proportions (%)		Information of relatives	GM types of VBM	MRI strength	Smoothing FWHM
	Rel	Con	Rel	Con	Rel	Con
(17)	45	59	22.6 (3.92)	23.2 (2.58)	64.4	64.4	First-degree (siblings)	GM volume	3 T	8 mm
(6)	29	37	40.38 (15.84)	39.36 (9.97)	48.3	45.9	First-degree (parents and siblings)	GM volume	3 T	8 mm
(12)	186	122	27.5 (6.8)	27.5 (8.2)	45.7	50	First-degree (siblings)	GM density	1.5 T	4 mm
(7)	55	29	50.31 (5.1)	51.79 (5.58)	49.1	48.3	First-degree (parents)	GM density	3 T	6 mm
(13)	9	34	33.8 (13.1)	39.3 (9.5)	66.7	70.6	First-degree (MZ)	GM volume	1.5 T	8 mm
(15)^a	10	10	41.4 (3.7)	43.2 (6.3)	37.5	40	First-degree (parents)	GM density	3 T	8 mm
(15)^a	10	10	45.6 (6.2)	43.2 (6.3)	41.7	40	First-degree (parents)	GM density	3 T	8 mm
(14)	213	212	36.5 (9.75)	33.31 (9.86)	41.8	48.6	First-degree (siblings)	GM volume	1.5 T	10 mm
(16)	24	49	38.92 (12.9)	35.27 (11.1)	45.8	46.9	First- and second-degree	GM density	1.5 T	12 mm

(1) ^aTwo independent VBM comparisons between relatives of patients and healthy controls were conducted by Lui et al.

(2) SD, standard deviation; MZ, monozygotic twins; VBM, voxel-based morphometry; GM, gray matter; FWHM, full-width at half-maximum.

The results of ES-SDM analysis

All of the nine VBM comparisons showed GM changes in patients relative to the healthy controls. Compared to the healthy controls, patients showed decreased GM in the right cuneus, the right superior frontal gyrus, the right insula, and the left claustrum and increased GM in the bilateral putamen, the right parahippocampal gyrus, the left precentral gyrus, the left inferior temporal gyrus, and the right cerebellar tonsil (Figure 2A; Table 3).

Figure 2

Gray matter differences between patients (A) and relatives of patients (B) compared with healthy controls. Areas with increased gray matter relative to controls are displayed in red, and areas with decreased gray matter are displayed in blue.

Table 3

Gray matter differences between patients and healthy controls.

Regions	Maximum		Cluster		Cluster breakdown	Jack-knife sensitivity
	Talairach coordinates	Z value	Uncorrected P	No. of voxels		No. of analyses survived by the clusters
PATIENTS > CONTROLS
Right basal ganglia (Right lentiform nucleus, putamen)	20, 2, 4	2.287	0.000064226	85	Right putamen	9 out of 9
					Right caudate body
					Right caudate head
					Right lateral globus pallidus
Left basal ganglia (Left lentiform nucleus, putamen)	−22, −2, 8	2.283	0.000064226	77	Left putamen	8 out of 9
					Left caudate body
					Left lateral globus pallidus
Right parahippocampal gyrus	38, −26, −16	2.140	0.000166988	43	Right parahippocampal gyrus	8 out of 9
					Right inferior temporal gyrus
					Right fusiform gyrus
Left precentral gyrus	−38, −8, 46	2.055	0.000616570	21	Left precentral gyrus	8 out of 9
					Left middle frontal gyrus
Left inferior temporal gyrus(Left fusiform gyrus)**	−46, −12, −30	2.053	0.000616570	36	Left inferior temporal gyrus	8 out of 9
					Left fusiform gyrus
Right cerebellar tonsil	22, −54, −34	1.831	0.002581888	13	Right cerebellar tonsil	7 out of 9
PATIENTS < CONTROLS
Right cuneus	22, −98, −2	−3.877	0.000321130	90	Right cuneus	8 out of 9
					Right lingual gyrus
					Right middle occipital gyrus
					Right inferior occipital gyrus
Right superior frontal gyrus	28, 60, 4	−3.645	0.000552344	78	Right superior frontal gyrus	7 out of 9
					Right middle frontal gyrus
Right insula	42, 2, 12	−3.179	0.001451509	40	Right insula	8 out of 9
					Right superior temporal gyrus
					Right precentral gyrus
Left basal ganglia (Left clastrum)**	−30, 16, 2	−3.132	0.001592807	49	Left clastrum	7 out of 9
					Left superior temporal gyrus
					Left insula
					Left extra-nuclear

**Shared GM alterations in patients and their unaffected relatives.

Four of the nine VBM comparisons showed no significant GM changes in unaffected relatives of patients compared to healthy controls (12, 13, 15, 16). The studies that showed significant GM changes were comparable to the studies showing negative results in terms of mean sample size of unaffected relatives [70.0 ± 81.89 vs. 57.75 ± 85.75 (P = 0.836)] and proportion of males [46.29 vs. 46.32% (P = 0.993)], but not for the mean age of the unaffected relatives (37.32 ± 7.50 vs. 29.87 ± 5.16), which was significantly different (P < 0.001). The results of the ES-SDM analysis from the nine VBM comparisons are shown in Table 4 and Figure 2B. Compared to healthy controls, unaffected relatives demonstrated decreased GM in the left claustrum, the bilateral parahippocampal gyri, the left fusiform gyrus, the right inferior temporal gyrus, and the bilateral medial prefrontal cortices and increased GM in the right hippocampus, the right fusiform gyrus, the right precentral gyrus, and the right precuneus (Figure 2B).

Table 4

Gray matter differences between relatives of patients with schizophrenia and healthy controls.

Regions	Maximum		Cluster		Cluster breakdown	Jack-knife sensitivity
	Talairach coordinates	Z value	Uncorrected P	No. of voxels		No. of analyses survived by the clusters
RELATIVES > CONTROLS
Right hippocampus	24, −20, −20	2.219	0.000051381	59	Right parahippocampus	8 out of 9
					Right hippocampus
Right fusiform gyrus**	44, −30, −20	2.200	0.000077071	71	Right fusiform gyrus	8 out of 9
					Right inferior temporal gyrus
					Right parahippocampus
Right precentral gyrus	56, 2, 28	2.168	0.000089917	135	Right precentral gyrus	8 out of 9
					Right inferior temporal gyrus
					Right middle temporal gyrus
Right precuneus	10, −60, 32	1.902	0.000924855	73	Right precuneus	8 out of 9
					Right cingulate gyrus
RELATIVES < CONTROLS
Left basal ganglia (claustrum)**	−34, −4, −6	−2.549	∼0	81	Left lentiform nucleus, putamen	8 out of 9
					Left claustrum
					Left parahippocampal gyrus
					Left insula
Right parahippocampal gyrus	26, −48, −4	−2.405	0.000051381	77	Right parahippocampal gyrus	8 out of 9
					Right fusiform nucleus
					Right declive
					Right culmen
Left fusiform gyrus	−52, −42, −22	−2.144	0.000488118	52	Left fusiform gyrus	8 out of 9
					Left inferior temporal gyrus
					Left tuber
Bilateral medial prefrontal gyri	2, 58, 2	−2.029	0.000873475	51	Right medial frontal gyrus	7 out of 9
					Left medial frontal gyrus
Right inferior temporal gyrus	42, −64, −16	−1.950	0.001207405	53	Right declive	8 out of 9
					Right fusiform gyrus
Left parahippocampal gyrus	−26, −54, −6	−1.919	0.001374438	16	Left parahippocampal gyrus	8 out of 9
					Left fusiform gyrus

**Shared GM alterations in patients and their unaffected relatives.

Discussion

Using ES-SDM meta-analysis of VBM studies in schizophrenia patients and their unaffected relatives, the current study confirmed that schizophrenia patients and their unaffected relatives share brain abnormalities, including reduced GM in the left claustrum and increased GM in the right fusiform gyrus. However, the patients also showed other deficits, including decreased GM in the right cuneus, the right superior frontal gyrus, and the right insula, as well as increased GM in the bilateral putamen, the right parahippocampal gyrus, the left precentral gyrus, the left inferior temporal gyrus, and the right cerebellar tonsil (Table 3). Their unaffected relatives also demonstrated reduced GM in other regions including the bilateral parahippocampal gyri, the left fusiform gyrus, the right inferior temporal gyri, and the medial prefrontal cortices and increased GM in the right hippocampus, the right precentral gyrus, and the right precuneus (Table 4). Thus, the current study provides evidence to support the hypothesis that GM changes in schizophrenia patients and their unaffected relatives are largely different, but share some subtle overlap.

One of the most interesting findings of the present meta-analysis is that both schizophrenia patients and their unaffected relatives shared GM changes in the left claustrum and the right fusiform gyrus, suggesting subtle genetic anatomical brain deficits in schizophrenia. In fact, the claustrum belongs to the basal ganglia which plays a critical role in the cortical-subcortical model for the pathogenesis of schizophrenia, in which prefrontal cortex dysfunction leads to disinhibited dopaminergic activity, enhanced subcortical dopamine neurotransmission in the basal ganglia, and psychosis (23, 24). The shared deficits of the basal ganglia in both patients and relatives suggest a genetic structural trait of schizophrenia, possibly reflecting endogenous overactivity of the striatal dopamine system (25). Thus, the deficits of the basal ganglia may be a core feature and a risk factor for the schizophrenia. (26) However, another possible reason for the increase GM volume of the basal ganglia in schizophrenia patients was related to the antipsychotic treatment which was reported to be the target of antipsychotic medication and found increased volume after treatment (27). The increased GM volume in the fusiform gyrus in both patients and relatives has seldom been reported and may represent a protective or compensatory phenomenon. The function of the right fusiform gyrus have been implicated in face-processing tasks requiring perception of faces and objects (28). In fact, the functional deficits of the right fusiform gyrus were also reported in both schizophrenia patients and their siblings, and these abnormalities could reflect reduced language-related lateralization in individuals with schizophrenia and their high-risk siblings (29). Another previous study indicated that loss of fusiform gyrus volume was negatively correlated with improvement in neurocognitive function as well as social cognition (30). Our study provided further evidences to support the possible genetic related GM changes of the right fusiform in schizophrenia.

However, it should be noted that the shared changes of GM volume are subtle, which suggests that the anatomical correlates of genetic liability may be small. Therefore, it may be not possible to pinpoint any single factor as being by itself necessary and sufficient to cause a psychiatric disorder. Most likely, the affected patients have multiple risk factors in different combinations that vary individually from patient to patient (31). Thus, heightened genetic risk for the unaffected first-degree relatives of schizophrenia may be reflected in small changes to cognitive functioning (9), as well as in brain structural changes. Schizophrenia is thought to result from a combination of multiple factors, such as genes, environment, antipsychotics, substance abuse, and comorbidities. However, Lui et al. observed that familial parents have more neuroanatomical abnormalities than sporadic parents (15). Furthermore, brain volume differences in twins discordant for schizophrenia were more pronounced in monozygotic than in dizygotic twins, compared with healthy control twins (32–34). This evidence suggests that the genetic contribution to brain volume alterations in schizophrenia may be subtle but prominent in subjects with a high genetic load, i.e., monozygotic discordant twins or familial parents rather than healthy siblings of patients with schizophrenia. In addition, one single factor could have multiple effects. Thus, a single gene could cause different phenotypes, depending on various interactions at the gene–gene and gene-environmental levels (genetic pleiotropism) (31). This theory is supported by recent studies that reported that the same genetic variants can cause both bipolar disorder and schizophrenia (35, 36). Furthermore, the shared GM in the left claustrum could be regarded with suspicion as this deep GM area is rather delicate and thus might be prone to image-registration errors.

It should also be noted that the most common deficits in GM volume in the patient group involved the cortical-striatal regions, which is consistent with a previous meta-analysis (2). The superior frontal gyrus, which showed reduced GM volume in our study, belongs to the prefrontal cortex, which is frequently thought to be a key structure in schizophrenia. The superior frontal gyrus plays an important role in managing many executive functions, such as working memory, response inhibition, and goal-directed behaviors. These cognitive abilities are typically disturbed in schizophrenia. In line with previous volumetric studies (37), we also found decreased GM in the insula, which has been suggested to be linked to clinical features such as reality distortion (38). In addition to the decreased GM, increased GM was also revealed in the patient group in the bilateral basal ganglia, the right fusiform gyrus, the left inferior temporal gyrus, the left precentral gyrus, and the right cerebellar tonsil. These findings are not surprising, as increased GM volume has also been reported in previous studies (39–42). A recent study of the largest sample of drug-naive first-episode of schizophrenia patients also revealed wide-spread increases in GM (42). The increased GM in the basal ganglia was consistent with most of the findings in an independent study of schizophrenia patients (43, 44). However, negative findings (45) or even decreased volumes of basal ganglia (46) GM have also been reported. The increased putamen GM may be partly attributed to exposure to antipsychotic medication, which is supported by the results of recent studies that showed increased putamen (47, 48) in first-episode drug-naïve schizophrenics after several weeks of antipsychotic treatment. Most studies included in the present meta-analysis investigated medicated schizophrenia patients, except for two studies (15, 17). Thus, the increased GM reported here could be related to antipsychotics.

Unlike the consistently positive findings in the patient groups, nearly half of the VBM comparisons (four out of nine) did not find structural differences between unaffected relatives and healthy controls. This finding suggests that the anatomical correlates of genetic liability may be weak. However, another possible reason for the negative findings in relatives is that the moderate changes in the relatives may be missed when using VBM (38). Our results of unaffected relatives are mostly consistent with Palaniyappan et al., who performed a meta-analysis of VBM studies seeking to identify the neuroanatomical correlates of genetic liability in schizophrenia. Though the primary studies that were pooled in that meta-analysis largely overlap with the studies that we identified, there are some important differences. We did not include Job et al. (49) or Marcelis et al. (50) in the present meta-analysis, as the unaffected relatives and schizophrenia patients in those two studies came from different families; thus, the patients and unaffected relatives shared no biological relationship. Furthermore, we included two other recently published studies (6, 17). The studies that showed significant GM changes were comparable to the studies showing negative results in terms of mean sample size of unaffected relatives and proportion of males, but the mean age of unaffected relatives was different.

Unexpectedly, the present meta-analysis of unaffected relatives also displayed wide-spread GM changes throughout the whole-brain (Table 4), though many areas are different from those of the patients. The left claustrum, the bilateral parahippocampal gyri, the left fusiform gyrus, the right inferior temporal gyrus and the bilateral medial prefrontal cortices emerged as the most significant loci with GM reductions in unaffected relatives compared to controls. The GM reduction was qualitatively consistent with some liability literature. For example, GM decreases in the parahippocampal gyrus and the medial prefrontal gyrus have been reported in previous studies of unaffected relatives of schizophrenia patients (13, 16, 51). The parahippocampal region is considered to be a part of the limbic lobe. Together with the amygdala, the parahippocampal gyrus assumes an important role in emotional processing and goal-directed processes (52). Furthermore, a recent functional study also provided evidence that hippocampal-parahippocampal dysfunction is related to genetic risk of developing schizophrenia (53). Our meta-analysis, however, did not find a grossly decreased volume of the hippocampus, which is has been reported as a pronounced change in non-psychotic first-degree relatives of schizophrenia patients in previous studies using ROI analysis (10). However, the conclusion of the previous meta-analysis was strongly influenced by a publication bias that most studies selectively measured morphometric changes in the hippocampus. Thus, the discrepancy may partly result from the different methods. VBM provides an unbiased approach to establish the presence of regional changes in GM by surveying the whole-brain.

The regions that displayed GM increases, the right parahippocampus, the right fusiform gyrus, the right precentral gyrus, and the right precuneus, have been reported in previous studies. Increased volume of the bilateral parahippocampal gyrus and the temporal lobe (though middle temporal) have been reported in unaffected relatives of patients with schizophrenia (51, 54). Furthermore, Seidman et al. (55) found increased cerebral volume in a small group of relatives. Though the exact mechanism for these increases is still unknown, it is possible that they may represent a protective or compensatory mechanism in unaffected family members, although this hypothesis is highly speculative (14). To better understand brain structure changes between patients with schizophrenia and their unaffected relatives, substantial effort is needed to search for biomarkers associated with robust genetic liability.

We acknowledge several limitations of the current meta-analysis. First, the small sample size may limit the power of our analyses, in particular sub-analyses of groups at differential genetic risk for psychosis (i.e., first-degree relatives vs. twins). Another limitation is related to the VBM methodology. Although VBM provides an unbiased approach to investigate the GM differences throughout the brain, its limitations relate to the difficulty of spatially normalizing brains, the robustness of standard parametric tests, and the interpretation of the results (56). A recent study suggested that subtle surface anatomical changes may be important for the pathophysiology of schizophrenia, and these changes may be missed when using VBM (38). Furthermore, both GM density and volume were used in the included eight studies. Though the difference of density and volume were little for VBM study, we cannot exclude the possible bias caused by the approaches. Finally, most of the patients included in the present meta-analysis were medicated. Thus, it is impossible to exclude the influence of antipsychotics on brain morphology. Cross-sectional (20) study which compared genetic high-risk subjects and first-episode antipsychotic-naive schizophrenia patients or longitudinal design (57) of high-risk subjects who finally translate to psychosis will help to analysis the genetic liability to psychosis.

Altogether, the current meta-analysis shows wide-spread GM deficits, including increased and decreased GM in both schizophrenia patients and their unaffected biological relatives. However, patients and relatives only showed subtle overlap, suggesting that the anatomical correlates of genetic liability may be weak for schizophrenia. As limitations such as small sample size and medication status could affect the findings, the relationship between GM deficits and susceptibility to developing schizophrenia remains to be established. In the future, studies of antipsychotic-naïve patients with first-episode schizophrenia and their unaffected relatives may help to clarify the genetic and environmental susceptibility to schizophrenia.

Author Contributions

Su Lui and QiYong Gong contributed to the conceptual design of the study. Yuan Xiao and Wenjing Zhang performed the data analysis and wrote the manuscript. Su Lui and Li Yao helped perform the analysis and contribute to constructive discussions.

Conflict of Interest Statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

This study was supported by the National Natural Science Foundation (Grant Nos. 81222018, 81371527, 81030027, 81227002, and 81220108013), the Distinguished Young Scholars of Sichuan (Grant No. 2011JQ0005), the Programs for New Century Excellent Talents in University (Grant No. NCET-10-0596), the CMB Distinguished Professorship Award (No. F510000/G16916411), the National Key Technologies R&D Program (No: 2012BAI01B03), and the Program for Changjiang Scholars and Innovative Research Team in University (PCSIRT, Grant No. IRT1272) of China.

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