Literature DB >> 27088856

Per2 induction limits lymphoid-biased haematopoietic stem cells and lymphopoiesis in the context of DNA damage and ageing.

Jianwei Wang1, Yohei Morita1, Bing Han1, Silke Niemann2, Bettina Löffler3, K Lenhard Rudolph1,4.   

Abstract

Ageing-associated impairments in haemato-lymphopoiesis are associated with DNA damage accumulation and reduced maintenance of lymphoid-biased (Ly-biased) compared with myeloid-biased (My-biased) haematopoietic stem cells (HSCs). Here, in vivo RNAi screening identifies period circadian clock 2 (Per2) as a critical factor limiting the maintenance of HSCs in response to DNA damage and ageing. Under these conditions, Per2 is activated predominantly in Ly-biased HSCs and stimulates DNA damage signalling and p53-dependent apoptosis in haematopoietic cells. Per2 deletion ameliorates replication stress and DNA damage responses in haematopoietic cells, thereby improving the maintenance of Ly-biased HSCs, lymphopoiesis, and immune function in ageing mice without increasing the accumulation of DNA damage. Per2-deficient mice retain Batf/p53-dependent induction of differentiation of HSCs in response to DNA damage and exhibit an elongated lifespan. Together, these results identify Per2 as a negative regulator of Ly-biased HSCs and immune functions in response to DNA damage and ageing.

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Year:  2016        PMID: 27088856     DOI: 10.1038/ncb3342

Source DB:  PubMed          Journal:  Nat Cell Biol        ISSN: 1465-7392            Impact factor:   28.824


  58 in total

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  23 in total

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Journal:  Mol Biol Rep       Date:  2021-10-12       Impact factor: 2.316

Review 3.  Dysfunctional telomeres and hematological disorders.

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Review 5.  Circadian Clocks and Cancer: Timekeeping Governs Cellular Metabolism.

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7.  Genomic deletion of GIT2 induces a premature age-related thymic dysfunction and systemic immune system disruption.

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8.  SMYD2 lysine methyltransferase regulates leukemia cell growth and regeneration after genotoxic stress.

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10.  Calorie restriction effects on circadian rhythms in gene expression are sex dependent.

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