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性发育障碍(DSD):最新进展。

Disorders of sex development (DSDs): an update.

机构信息

Departments of Pathology, Genetics, and Pediatrics, Albert Einstein College of Medicine, Bronx, New York 10461.

出版信息

J Clin Endocrinol Metab. 2014 May;99(5):1503-9. doi: 10.1210/jc.2013-3690. Epub 2014 Apr 23.

Abstract

CONTEXT

Disorders of sex development (DSDs) may arise from genetic defects in testis or ovary determination. Current analytical technologies and improved understanding of major regulatory pathways have cast new insight into the genetic basis for these disorders.

EVIDENCE ACQUISITION

A PubMed search was performed for the years 2011-13 using the terms "disorder of sex development," "gonadal dysgenesis," "ovarian dysgenesis," "array CGH," and "whole exome sequencing." Only articles from peer-reviewed journals were included.

EVIDENCE SYNTHESIS

Key themes that emerged included aberrant regulation of SOX9 via the hTES promoter in 46,XY gonadal DSDs, the role of the MAPK pathway in normal and aberrant gonadal development, and the role of new technologies in identification of gonadal DSDs.

CONCLUSIONS

With the advent of the robust new technologies of array comparative genomic hybridization and genomic sequencing in recent years, many new sex-determining genes have been identified. These genes have been organized into ovarian- and testicular-determining pathways that can block each other's activities. Identification of a mutation in a sex-determining gene in an individual affected with a DSD may warrant more extensive investigation for other phenotypic effects as well as genetic testing of other family members.

摘要

背景

性发育障碍(DSD)可能源于睾丸或卵巢决定的遗传缺陷。当前的分析技术和对主要调控途径的深入理解为这些疾病的遗传基础提供了新的认识。

证据获取

使用术语“性发育障碍”、“性腺发育不良”、“卵巢发育不良”、“阵列 CGH”和“全外显子测序”,在 2011-13 年间对 PubMed 进行了搜索。仅包括同行评审期刊的文章。

证据综合

出现的主要主题包括在 46,XY 性腺 DSD 中通过 hTES 启动子异常调节 SOX9、MAPK 途径在正常和异常性腺发育中的作用,以及新技术在鉴定性腺 DSD 中的作用。

结论

随着近年来强大的新型阵列比较基因组杂交和基因组测序技术的出现,许多新的性别决定基因已经被鉴定出来。这些基因已被组织成卵巢和睾丸决定途径,它们可以相互阻断。在患有 DSD 的个体中鉴定出性别决定基因的突变可能需要更广泛地调查其他表型效应以及对其他家庭成员进行基因测试。

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