多囊卵巢综合征女性中罕见的抗勒氏激素蛋白改变变异的功能分析。

IF 3.6 2区 医学 Q2 DEVELOPMENTAL BIOLOGY Molecular human reproduction Pub Date : 2023-04-29 DOI:10.1093/molehr/gaad011
L Meng, A McLuskey, A Dunaif, J A Visser
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引用次数: 0

摘要

最近,在多囊卵巢综合征(PCOS)女性中发现了罕见的杂合AMH蛋白改变变异,导致抗勒氏激素(AMH)信号减少。然而,确切的功能机制尚不清楚。在这里,我们分析了这些AMH变异的加工、分泌和信号传导。在小鼠颗粒细胞系KK-1中对6个pcos特异性AMH变异(V12G、P151S、P270S、P352S、P362S、H506Q)和1个对照特异性AMH变异(A519V)进行了功能分析。与野生型(wt) AMH信号相比,人类(h) AMH- 151s和hAMH-506Q的AMH信号减少了约90%。hAMH-151S或hAMH-506Q与wt-hAMH的共表达可剂量依赖性地抑制wt-hAMH信号传导。Western blotting显示,细胞裂解液中检测到hAMH-151S和hAMH-506Q蛋白,上清中未检测到。共聚焦显微镜显示,与表达wt-hAMH的细胞相比,表达hAMH-151S和hAMH-506Q的HEK293细胞具有更高的细胞AMH蛋白水平和内质网(ER)保留。使用两个AMH ELISA试剂盒,在细胞裂解液中检测到hAMH-151S,而在上清中仅检测到极低水平的hAMH-151S。hAMH-362S和hAMH-519V均可通过自动AMH酶联免疫吸附试验检测到,但手工酶联免疫吸附试验显示免疫活性严重降低。令人惊讶的是,hAMH-506Q在细胞裂解液和上清液中均检测不到。然而,在PCOS病例中,P151S和H506Q变异的杂合携带者在两种检测中仍可检测到AMH。因此,P151S和H506Q破坏AMH的正常加工和分泌,导致内质网滞留。此外,AMH变异可损害AMH免疫活性。当多囊卵巢综合征患者血清AMH水平相对较低时,可考虑AMH变异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Functional analysis of rare anti-Müllerian hormone protein-altering variants identified in women with PCOS.

Recently, rare heterozygous AMH protein-altering variants were identified in women with polycystic ovary syndrome (PCOS), causing reduced anti-Müllerian hormone (AMH) signaling. However, the exact functional mechanism remains unknown. Here, we analyzed the processing, secretion, and signaling of these AMH variants. Functional analysis of six PCOS-specific AMH variants (V12G, P151S, P270S, P352S, P362S, H506Q) and one control-specific variant (A519V) was performed in the mouse granulosa cell-line KK-1. Human (h) AMH-151S and hAMH-506Q have ∼90% decreased AMH signaling compared to wild-type (wt) AMH signaling. Coexpression of hAMH-151S or hAMH-506Q with wt-hAMH dose-dependently inhibited wt-hAMH signaling. Western blotting revealed that hAMH-151S and hAMH-506Q proteins were detected in the cell lysate but not in the supernatant. Confocal microscopy showed that HEK293 cells expressing hAMH-151S and hAMH-506Q had higher cellular AMH protein levels with endoplasmic reticulum (ER) retention compared to cells expressing wt-hAMH. Using two AMH ELISA kits, hAMH-151S was detected in the cell lysate, while only very low levels were detected in the supernatant. Both hAMH-362S and hAMH-519V were detectable using the automated AMH ELISA but showed severely reduced immunoactivity in the manual ELISA. Surprisingly, hAMH-506Q was undetectable in both the cell lysate and supernatant using either ELISA. However, in PCOS cases, heterozygous carriers of the P151S and H506Q variants still had detectable AMH in both assays. Thus, P151S and H506Q disrupt normal processing and secretion of AMH, causing ER retention. Additionally, AMH variants can impair the AMH immunoactivity. An AMH variant may be considered when serum AMH levels are relatively low in PCOS cases.

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来源期刊
Molecular human reproduction
Molecular human reproduction 生物-发育生物学
CiteScore
8.30
自引率
0.00%
发文量
37
审稿时长
6-12 weeks
期刊介绍: MHR publishes original research reports, commentaries and reviews on topics in the basic science of reproduction, including: reproductive tract physiology and pathology; gonad function and gametogenesis; fertilization; embryo development; implantation; and pregnancy and parturition. Irrespective of the study subject, research papers should have a mechanistic aspect.
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