Merck
CN

Cohesin mediates DNA loop extrusion by a "swing and clamp" mechanism.

Cell (2021-10-09)
Benedikt W Bauer, Iain F Davidson, Daniel Canena, Gordana Wutz, Wen Tang, Gabriele Litos, Sabrina Horn, Peter Hinterdorfer, Jan-Michael Peters
摘要

Structural maintenance of chromosomes (SMC) complexes organize genome topology in all kingdoms of life and have been proposed to perform this function by DNA loop extrusion. How this process works is unknown. Here, we have analyzed how loop extrusion is mediated by human cohesin-NIPBL complexes, which enable chromatin folding in interphase cells. We have identified DNA binding sites and large-scale conformational changes that are required for loop extrusion and have determined how these are coordinated. Our results suggest that DNA is translocated by a spontaneous 50 nm-swing of cohesin's hinge, which hands DNA over to the ATPase head of SMC3, where upon binding of ATP, DNA is clamped by NIPBL. During this process, NIPBL "jumps ship" from the hinge toward the SMC3 head and might thereby couple the spontaneous hinge swing to ATP-dependent DNA clamping. These results reveal mechanistic principles of how cohesin-NIPBL and possibly other SMC complexes mediate loop extrusion.

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葡萄糖氧化酶 来源于黑曲霉, Type VII, lyophilized powder, ≥100,000 units/g solid (without added oxygen)
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β-酪蛋白 来源于牛奶, BioUltra, ≥98% (PAGE)
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丙酮酸激酶/乳酸脱氢酶 来源于兔肌肉, For the Determination of ADP, buffered aqueous glycerol solution
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辅酶 A 三锂盐, ≥93%
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原儿茶酸3,4-双加氧酶 来源于假单胞菌 属, lyophilized powder, ≥3 units/mg solid