FA 核心泛素连接酶在 DNA 上关闭 ID 夹的结构。

Structure of the FA core ubiquitin ligase closing the ID clamp on DNA.

机构信息

Structural Biology Program, Memorial Sloan Kettering Cancer Center, New York, NY, USA.

Howard Hughes Medical Institute, Memorial Sloan Kettering Cancer Center, New York, NY, USA.

出版信息

Nat Struct Mol Biol. 2021 Mar;28(3):300-309. doi: 10.1038/s41594-021-00568-8. Epub 2021 Mar 8.

DOI:10.1038/s41594-021-00568-8

PMID:33686268

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8378520/

Abstract

The Fanconi anemia (FA) pathway is essential for the repair of DNA interstrand crosslinks. Central to the pathway is the FA core complex, a ubiquitin ligase of nine subunits that monoubiquitinates the FANCI-FANCD2 (ID) DNA clamp. The 3.1 Å structure of the 1.1-MDa human FA core complex, described here, reveals an asymmetric assembly with two copies of all but the FANCC, FANCE and FANCF subunits. The asymmetry is crucial, as it prevents the binding of a second FANCC-FANCE-FANCF subcomplex that inhibits the recruitment of the UBE2T ubiquitin conjugating enzyme, and instead creates an ID binding site. A single active site then ubiquitinates FANCD2 and FANCI sequentially. We also present the 4.2-Å structures of the human core-UBE2T-ID-DNA complex in three conformations captured during monoubiquitination. They reveal the core-UBE2T complex remodeling the ID-DNA complex, closing the clamp on the DNA before ubiquitination. Monoubiquitination then prevents clamp opening after release from the core.

摘要

范可尼贫血（FA）途径对于修复 DNA 链间交联至关重要。该途径的核心是 FA 核心复合物，这是一个由九个亚基组成的泛素连接酶，可单泛素化 FANCI-FANCD2（ID）DNA 夹。本文描述了 3.1 Å 分辨率的 1.1 MDa 人源 FA 核心复合物结构，揭示了一种非对称组装，除了 FANCC、FANCE 和 FANCF 亚基外，所有亚基都有两个拷贝。这种不对称性至关重要，因为它可以防止第二个 FANCC-FANCE-FANCF 亚复合物的结合，从而抑制 UBE2T 泛素连接酶的募集，而是创建一个 ID 结合位点。然后，单个活性位点依次泛素化 FANCD2 和 FANCI。我们还展示了在单泛素化过程中捕获的三种构象下的人源核心-UBE2T-ID-DNA 复合物的 4.2 Å 结构。它们揭示了核心-UBE2T 复合物重塑 ID-DNA 复合物，在泛素化之前将夹关闭在 DNA 上。单泛素化后，在从核心释放后阻止夹的打开。

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