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低温电镜揭示了一个近乎完整的 PCNA 加载过程和人类替代 clamp loader CTF18-RFC 的独特特征。

Cryo-EM reveals a nearly complete PCNA loading process and unique features of the human alternative clamp loader CTF18-RFC.

机构信息

Department of Structural Biology, Van Andel Institute, Grand Rapids, MI 49503.

DNA Replication Laboratory, The Rockefeller University, New York, NY 10065.

出版信息

Proc Natl Acad Sci U S A. 2024 Apr 30;121(18):e2319727121. doi: 10.1073/pnas.2319727121. Epub 2024 Apr 26.

Abstract

The DNA sliding clamp PCNA is a multipurpose platform for DNA polymerases and many other proteins involved in DNA metabolism. The topologically closed PCNA ring needs to be cracked open and loaded onto DNA by a clamp loader, e.g., the well-studied pentameric ATPase complex RFC (RFC1-5). The CTF18-RFC complex is an alternative clamp loader found recently to bind the leading strand DNA polymerase ε and load PCNA onto leading strand DNA, but its structure and the loading mechanism have been unknown. By cryo-EM analysis of in vitro assembled human CTF18-RFC-DNA-PCNA complex, we have captured seven loading intermediates, revealing a detailed PCNA loading mechanism onto a 3'-ss/dsDNA junction by CTF18-RFC. Interestingly, the alternative loader has evolved a highly mobile CTF18 AAA+ module likely to lower the loading activity, perhaps to avoid competition with the RFC and to limit its role to leading strand clamp loading. To compensate for the lost stability due to the mobile AAA+ module, CTF18 has evolved a unique β-hairpin motif that reaches across RFC2 to interact with RFC5, thereby stabilizing the pentameric complex. Further, we found that CTF18 also contains a separation pin to locally melt DNA from the 3'-end of the primer; this ensures its ability to load PCNA to any 3'-ss/dsDNA junction, facilitated by the binding energy of the E-plug to the major groove. Our study reveals unique structural features of the human CTF18-RFC and contributes to a broader understanding of PCNA loading by the alternative clamp loaders.

摘要

DNA 滑动夹 PCNA 是 DNA 聚合酶和许多其他参与 DNA 代谢的蛋白质的多用途平台。拓扑闭合的 PCNA 环需要被夹加载器打开并加载到 DNA 上,例如,研究充分的五聚体 ATP 酶复合物 RFC(RFC1-5)。最近发现 CTF18-RFC 复合物是一种替代的夹加载器,它可以结合领头链 DNA 聚合酶 ε 并将 PCNA 加载到领头链 DNA 上,但它的结构和加载机制尚不清楚。通过体外组装的人 CTF18-RFC-DNA-PCNA 复合物的 cryo-EM 分析,我们捕获了七个加载中间体,揭示了 CTF18-RFC 通过 3'-ss/dsDNA 连接点将 PCNA 加载到 DNA 上的详细机制。有趣的是,替代加载器已经进化出一个高度移动的 CTF18 AAA+ 模块,可能会降低加载活性,也许是为了避免与 RFC 的竞争并限制其在领头链夹加载中的作用。为了弥补由于移动 AAA+ 模块而导致的稳定性丧失,CTF18 已经进化出一个独特的β发夹模体,该模体跨越 RFC2 与 RFC5 相互作用,从而稳定五聚体复合物。此外,我们发现 CTF18 还包含一个分离钉,用于将 DNA 从引物的 3'-末端局部融化;这确保了它能够将 PCNA 加载到任何 3'-ss/dsDNA 连接点,这得益于 E-插塞与主沟的结合能。我们的研究揭示了人类 CTF18-RFC 的独特结构特征,并有助于更广泛地理解替代夹加载器对 PCNA 的加载。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e42a/11067034/40793a9fb358/pnas.2319727121fig01.jpg

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