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人类性别决定的脆弱转录阈值。II. SRY 利用在歧义边缘的水介导的夹子。

Tenuous transcriptional threshold of human sex determination. II. SRY exploits water-mediated clamp at the edge of ambiguity.

机构信息

Department of Biochemistry and Molecular Biology, Indiana University School of Medicine, Indianapolis, IN, United States.

Faculty of Life Sciences, Bar Ilan University, Ramat Gan, Israel.

出版信息

Front Endocrinol (Lausanne). 2022 Dec 2;13:1029177. doi: 10.3389/fendo.2022.1029177. eCollection 2022.

Abstract

Y-encoded transcription factor SRY initiates male differentiation in therian mammals. This factor contains a high-mobility-group (HMG) box, which mediates sequence-specific DNA binding with sharp DNA bending. A companion article in this issue described sex-reversal mutations at box position 72 (residue 127 in human SRY), invariant as Tyr among mammalian orthologs. Although not contacting DNA, the aromatic ring seals the domain's minor wing at a solvent-exposed junction with a basic tail. A seeming paradox was posed by the native-like biochemical properties of inherited Swyer variant Y72F: its near-native gene-regulatory activity is consistent with the father's male development, but at odds with the daughter's XY female somatic phenotype. Surprisingly, aromatic rings (Y72, F72 or W72) confer higher transcriptional activity than do basic or polar side chains generally observed at solvated DNA interfaces (Arg, Lys, His or Gln). Whereas biophysical studies (time-resolved fluorescence resonance energy transfer and heteronuclear NMR spectroscopy) uncovered only subtle perturbations, dissociation of the Y72F complex was markedly accelerated relative to wild-type. Studies of protein-DNA solvation by molecular-dynamics (MD) simulations of an homologous high-resolution crystal structure (SOX18) suggest that Y72 -OH anchors a network of water molecules at the tail-DNA interface, perturbed in the variant in association with nonlocal conformational fluctuations. Loss of the Y72 anchor among SRY variants presumably "unclamps" its basic tail, leading to (a) rapid DNA dissociation despite native affinity and (b) attenuated transcriptional activity at the edge of sexual ambiguity. Conservation of Y72 suggests that this water-mediated clamp operates generally among SRY and metazoan SOX domains.

摘要

Y 编码转录因子 SRY 启动了有胎盘哺乳动物的雄性分化。该因子包含一个高迁移率族(HMG)盒,介导具有尖锐 DNA 弯曲的序列特异性 DNA 结合。本期杂志中的一篇相关文章描述了盒位置 72(人 SRY 中的第 127 个残基)的性别反转突变,该位置在哺乳动物直系同源物中不变为 Tyr。尽管不与 DNA 接触,但芳香环在与碱性尾巴的溶剂暴露连接处以密封结构域的小翅膀。一个看似悖论的问题是遗传的 Swyer 变体 Y72F 具有类似于天然的生化特性:其近乎天然的基因调控活性与其父代的雄性发育一致,但与子代的 XY 女性体表型不一致。令人惊讶的是,芳香环(Y72、F72 或 W72)比通常在溶剂化 DNA 界面观察到的碱性或极性侧链(Arg、Lys、His 或 Gln)赋予更高的转录活性。虽然生物物理研究(时间分辨荧光共振能量转移和异核 NMR 光谱学)仅揭示了细微的扰动,但与野生型相比,Y72F 复合物的解离明显加速。通过同源高分辨率晶体结构(SOX18)的分子动力学(MD)模拟研究蛋白质-DNA 的溶剂化,表明 Y72-OH 在尾部-DNA 界面处锚定了一个水分子网络,该网络在变体中与非局部构象波动有关。SRY 变体中 Y72 锚的丢失可能会“松开”其碱性尾巴,导致(a)尽管具有天然亲和力,但 DNA 快速解离,以及(b)在性别模糊边缘的转录活性减弱。Y72 的保守性表明,这种水介导的夹子在 SRY 和后生动物 SOX 结构域中普遍存在。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bef/9771472/4c7a65ebe408/fendo-13-1029177-g001.jpg

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