Defective DNA-damage repair induced by nuclear lamina dysfunction is a key mediator of smooth muscle cell aging. - Wikidata - awgldk - TriplyDB

Defective DNA-damage repair induced by nuclear lamina dysfunction is a key mediator of smooth muscle cell aging.

Defective DNA-damage repair induced by nuclear lamina dysfunction is a key mediator of smooth muscle cell aging.

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Lamins at a glance.Oxydative stress alters nuclear shape through lamins dysregulation: a route to senescence.Vein graft neointimal hyperplasia is exacerbated by CXCR4 signaling in vein graft-extrinsic cells.Mechanisms of vascular calcification in CKD-evidence for premature ageing?Disruption of PCNA-lamins A/C interactions by prelamin A induces DNA replication fork stalling.Prelamin A impairs 53BP1 nuclear entry by mislocalizing NUP153 and disrupting the Ran gradient

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Defective DNA-damage repair induced by nuclear lamina dysfunction is a key mediator of smooth muscle cell aging.

http://www.wikidata.org/entity/Q37958977

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Defective DNA-damage repair in ...... r of smooth muscle cell aging.

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Defective DNA-damage repair in ...... r of smooth muscle cell aging.

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Biochemical Society Transactions

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Defective DNA-damage repair in ...... r of smooth muscle cell aging.

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Catherine M Shanahan

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Derek T Warren

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The nuclear envelopathies and human diseases

Nesprin-2 is a multi-isomeric protein that binds lamin and emerin at the nuclear envelope and forms a subcellular network in skeletal muscle

PML regulates p53 stability by sequestering Mdm2 to the nucleolus

PML colocalizes with and stabilizes the DNA damage response protein TopBP1

Prelamin A acts to accelerate smooth muscle cell senescence and is a novel biomarker of human vascular aging

Mammalian SUN protein interaction networks at the inner nuclear membrane and their role in laminopathy disease processes

Recruitment of NBS1 into PML oncogenic domains via interaction with SP100 protein

Hutchinson-Gilford progeria mutant lamin A primarily targets human vascular cells as detected by an anti-Lamin A G608G antibody.

The DNA Damage Response: Making It Safe to Play with Knives

NBS1 and TRF1 colocalize at promyelocytic leukemia bodies during late S/G2 phases in immortalized telomerase-negative cells. Implication of NBS1 in alternative lengthening of telomeres

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1780-1785

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scholarly article

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10.1042/BST20110703

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6

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39

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2011-12-01T00:00:00Z

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22103525

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