女性精神分裂症的新性别特异性潜在机制:加速偏斜的 X 染色体失活。
A new sex-specific underlying mechanism for female schizophrenia: accelerated skewed X chromosome inactivation.
机构信息
Beijing Institute of Brain Disorders, Laboratory of Brain Disorders, Ministry of Science and Technology, Collaborative Innovation Center for Brain Disorders, Capital Medical University, Beijing, China.
The National Clinical Research Center for Mental Disorders & Beijing Key Laboratory of Mental Disorders, Beijing Anding Hospital, Capital Medical University, Beijing, China.
出版信息
Biol Sex Differ. 2020 Jul 17;11(1):39. doi: 10.1186/s13293-020-00315-6.
BACKGROUND
X chromosome inactivation (XCI) is the mechanism by which the X-linked gene dosage is adjusted between the sexes. Evidence shows that many sex-specific diseases have their basis in X chromosome biology. While female schizophrenia patients often have a delayed age of disease onset and clinical phenotypes that are different from those of males, it is unknown whether the sex differences in schizophrenia are associated with X-linked gene dosage and the choice of X chromosome silencing in female cells. Previous studies demonstrated that sex chromosome aneuploidies may be related to the pathogeneses of some psychiatric diseases. Here, we examined the changes in skewed XCI in patients with schizophrenia.
METHODS
A total of 109 female schizophrenia (SCZ) patients and 80 age- and sex-matched healthy controls (CNTLs) were included in this study. We evaluated clinical features including disease onset age, disease duration, clinical symptoms by the Positive and Negative Syndrome Scale (PANSS) and antipsychotic treatment dosages. The XCI skewing patterns were analyzed by the methylation profile of the HUMARA gene found in DNA isolated from SCZ patient and CNTL leukocytes in the three age groups.
RESULTS
First, we found that the frequency of skewed XCI in SCZ patients was 4 times more than that in the age- and sex-matched CNTLs (p < 0.01). Second, we found an earlier onset of severe XCI skewing in the SCZ patients than in CNTLs. Third, we demonstrated a close relationship between the severity of skewed XCI and schizophrenic symptoms (PANSS score ≥ 90) as well as the age of disease onset. Fourth, we demonstrated that the skewed XCI in SCZ patients was not transmitted from the patients' mothers.
LIMITATIONS
The XCI skewing pattern might differ depending on tissues or organs. Although this is the first study to explore skewed XCI in SCZ, in the future, samples from different tissues or cells in SCZ patients might be important for understanding the impact of skewed XCI in this disease.
CONCLUSION
Our study, for the first time, investigated skewed XCI in female SCZ patients and presented a potential mechanism for the sex differences in SCZ. Our data also suggested that XCI might be a potential target for the development of female-specific interventions for SCZ.
背景
X 染色体失活(XCI)是一种调节雌雄个体间 X 连锁基因剂量的机制。有证据表明,许多与性别相关的疾病都与 X 染色体生物学有关。女性精神分裂症患者的发病年龄往往较晚,且临床表型与男性不同,但尚不清楚精神分裂症的性别差异是否与 X 连锁基因剂量以及女性细胞中 X 染色体失活的选择有关。先前的研究表明,性染色体非整倍体可能与一些精神疾病的发病机制有关。在这里,我们研究了精神分裂症患者中 X 染色体失活偏倚的变化。
方法
本研究共纳入 109 名女性精神分裂症(SCZ)患者和 80 名年龄和性别匹配的健康对照者(CNTLs)。我们评估了临床特征,包括发病年龄、病程、阳性和阴性症状量表(PANSS)的临床症状以及抗精神病药物的剂量。通过对 SCZ 患者和 CNTL 白细胞中分离的 DNA 中 HUMARA 基因的甲基化谱分析 XCI 偏倚模式。
结果
首先,我们发现 SCZ 患者 XCI 偏倚的频率是年龄和性别匹配的 CNTLs 的 4 倍(p < 0.01)。其次,我们发现 SCZ 患者的严重 XCI 偏倚发病年龄早于 CNTLs。第三,我们证明了 XCI 偏倚的严重程度与精神分裂症症状(PANSS 评分≥90)以及发病年龄密切相关。第四,我们证明 SCZ 患者的 XCI 偏倚不是从患者母亲那里遗传的。
局限性
XCI 偏倚模式可能因组织或器官而异。尽管这是首次研究 SCZ 中的 XCI 偏倚,但在未来,来自 SCZ 患者不同组织或细胞的样本对于了解 XCI 偏倚对这种疾病的影响可能很重要。
结论
我们的研究首次研究了女性精神分裂症患者的 XCI 偏倚,并提出了精神分裂症性别差异的潜在机制。我们的数据还表明,XCI 可能是女性特异性精神分裂症干预措施的潜在靶点。
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