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一个新发现的调控射精功能的基因。

: A Newly Discovered Gene Regulating Ejaculation Function.

作者信息

Gao Jingjing, Gao Rui, Li Hu, Liu Xi, Gao Pan, Du Junhua, Jiang Hui, Zhang Xiansheng

机构信息

Department of Urology and Andrology, The First Affiliated Hospital of Anhui Medical University, Hefei, China.

Department of Andrology, The Third Hospital of Peking University, Beijing, China.

出版信息

Front Physiol. 2022 Feb 28;13:762272. doi: 10.3389/fphys.2022.762272. eCollection 2022.

Abstract

Ejaculation is a complex biphasic process involving a series of neurophysiological activities, such as the contraction of a large number of muscle groups and the ejaculation of semen from the urethra anterior. Due to the complexity of the process, many related factors have not been fully clarified, resulting in ejaculation dysfunction. As a common ejaculation dysfunction, lifelong premature ejaculation (LPE) is a problem for many people. Notably, gene polymorphism might play an important role in the etiology of LPE. However, the quest for identifying the actual genetic loci that contribute to LPE etiology has not been successful. Due to discrepancies in the design and methods of research, the correlation of most reports was not obtained in subjective replication experiments, and the conclusions may be inconsistent. In our study, three groups of ejaculation rats, namely, "rapid, normal, and delayed," were selected based on the animal model of premature ejaculation (PE) in rats and the theory of ejaculation. Among them, the rats in the "rapid" ejaculation group can be used to stimulate humans with PE. Subsequently, we used the rat brain tissue for whole-transcriptome sequencing to screen the differential genes among the three groups. We tried to identify the actual genetic loci that contribute to PE etiology and provide a theoretical basis for the targeted therapy of PE.

摘要

射精是一个复杂的双相过程,涉及一系列神经生理活动,如大量肌肉群的收缩以及精液从尿道前部射出。由于该过程的复杂性,许多相关因素尚未完全阐明,从而导致射精功能障碍。终身早泄(LPE)作为一种常见的射精功能障碍,困扰着许多人。值得注意的是,基因多态性可能在LPE的病因中起重要作用。然而,寻找导致LPE病因的实际基因位点的研究尚未成功。由于研究设计和方法存在差异,大多数报告的相关性在主观复制实验中未得到验证,结论可能不一致。在我们的研究中,基于大鼠早泄(PE)动物模型和射精理论,选择了三组射精大鼠,即“快速、正常和延迟”射精组。其中,“快速”射精组的大鼠可用于刺激患有PE的人类。随后,我们对大鼠脑组织进行全转录组测序,以筛选三组之间的差异基因。我们试图确定导致PE病因的实际基因位点,并为PE的靶向治疗提供理论依据。

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