DEFB119 将与男性不育症相关的精液微生物组网络扭曲的菌群失调分层。

IF 2.2 Q2 MULTIDISCIPLINARY SCIENCES PNAS nexus Pub Date : 2024-09-19 eCollection Date: 2024-10-01 DOI:10.1093/pnasnexus/pgae419
Jing Jin, Howard Chi Ho Yim, Hsiao Mei Ellie Chang, Yiwei Wang, Kathleen Hoi Kei Choy, Sze Yan Chan, Odai A M Alqawasmeh, Jinyue Liao, Xiao-Tao Jiang, David Yiu Leung Chan, Ellis Kin Lam Fok
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引用次数: 0

摘要

不育症与精液微生物群的改变有关。然而,菌群失调的发生仍存在争议,宿主因素的参与仍难以捉摸。本研究调查了男性不育症中精液微生物组的改变,并研究了生殖道特异性宿主抗菌肽DEFB119与精液微生物组和男性生育能力的关联和功能。虽然我们观察到细菌群落的属种、多样性和均匀度相当,但与对照组(n = 30)相比,精子图异常患者(n = 57)的元群落模块化程度明显下降。在男性不育患者的一个亚群(5 人)中观察到 DEFB119 明显升高。精液中 DEFB119 的升高与所观察到的细菌群落属种、多样性和均匀性的减少以及元群落的进一步扭曲有关。中介分析表明,DEFB119的升高和精液微生物群落的菌群失调参与了精子图异常的中介作用。功能实验表明,重组 DEFB119 能显著降低精子图异常患者精子的渐进运动能力。此外,DEFB119 对常见的精液和非精液物种具有物种特异性抗菌活性。我们的研究发现了一个重要的宿主因素,它介导了宿主与微生物组之间的相互作用,并将与男性不育相关的精液微生物组分层。这些结果可能会为男性不育症带来一种新的诊断方法,并为生殖道和其他器官系统的微生物组制定治疗方案。
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DEFB119 stratifies dysbiosis with distorted networks in the seminal microbiome associated with male infertility.

Infertility is associated with the alteration of the seminal microbiome. However, the onset of dysbiosis remains controversial and the involvement of host factors remains elusive. This study investigates the alterations of the seminal microbiome in male infertility and examines the association and function of DEFB119, a reproductive-tract-specific host antimicrobial peptide, on the seminal microbiome and male fertility. While we observed comparable genera, diversity and evenness of bacterial communities, a marked decrease in the modularity of the metacommunities was observed in patients with abnormal spermiogram (n = 57) as compared to the control (n = 30). A marked elevation of DEFB119 was observed in a subpopulation of male infertile patients (n = 5). Elevated seminal DEFB119 was associated with a decrease in the observed genera, diversity and evenness of bacterial communities, and further distortion of the metacommunities. Mediation analysis suggests the involvement of elevated DEFB119 and dysbiosis of the seminal microbiome in mediating the abnormalities in the spermiogram. Functional experiments showed that recombinant DEFB119 significantly decrease the progressive motility of sperm in patients with abnormal spermiogram. Moreover, DEFB119 demonstrated species-specific antimicrobial activity against common seminal and nonseminal species. Our work identifies an important host factor that mediates the host-microbiome interaction and stratifies the seminal microbiome associated with male infertility. These results may lead to a new diagnostic method for male infertility and regimens for formulating the microbiome in the reproductive tract and other organ systems.

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