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    SOX7-enforced expression promotes the expansion of adult blood progenitors and blocks B-cell development.

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    Authors
    Cuvertino, Sara
    Lacaud, Georges
    Kouskoff, Valerie
    Affiliation
    Stem Cell Hematopoiesis Group, Cancer Research UK Manchester Institute
    Issue Date
    2016-07
    
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    Abstract
    During embryogenesis, the three SOXF transcription factors, SOX7, SOX17 and SOX18, regulate the specification of the cardiovascular system and are also involved in the development of haematopoiesis. The ectopic expression of SOX17 in both embryonic and adult blood cells enhances self-renewal. Likewise, the enforced expression of SOX7 during embryonic development promotes the proliferation of early blood progenitors and blocks lineage commitment. However, whether SOX7 expression can also affect the self-renewal of adult blood progenitors has never been explored. In this study, we demonstrate using an inducible transgenic mouse model that the enforced expression of Sox7 ex vivo in bone marrow/stroma cell co-culture promotes the proliferation of blood progenitors which retain multi-lineage short-term engrafting capacity. Furthermore, SOX7 expression induces a profound block in the generation of B lymphocytes. Correspondingly, the ectopic expression of SOX7 in vivo results in dramatic alterations of the haematopoietic system, inducing the proliferation of blood progenitors in the bone marrow while blocking B lymphopoiesis. In addition, SOX7 expression induces extra-medullary haematopoiesis in the spleen and liver. Together, these data demonstrate that the uncontrolled expression of the transcription factor SOX7 in adult haematopoietic cells has dramatic consequences on blood homeostasis.
    Citation
    SOX7-enforced expression promotes the expansion of adult blood progenitors and blocks B-cell development. 2016, 6 (7): Open Biol
    Journal
    Open Biology
    URI
    http://hdl.handle.net/10541/618469
    DOI
    10.1098/rsob.160070
    PubMed ID
    27411892
    Type
    Article
    Language
    en
    ISSN
    2046-2441
    ae974a485f413a2113503eed53cd6c53
    10.1098/rsob.160070
    Scopus Count
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    All Paterson Institute for Cancer Research

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