Induction of megakaryocyte differentiation drives nuclear accumulation and transcriptional function of MKL1 via actin polymerization and RhoA activation

Smith, Elenoe C.; Teixeira, Alexandra M.; Chen, Rachel C.; Wang, Lin; Gao, Yuan; Hahn, Katherine L.; Krause, Diane S.

doi:10.1182/blood-2012-05-429993

Cited by 41 publications

(30 citation statements)

References 36 publications

(51 reference statements)

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“…15 Subsequent investigation of MKL1 function in hematopoietic cells has focused on megakaryocytes, and MKL1 deficiency in mice has been shown to result in cytoskeletal defects in this cell type disrupting differentiation, migration, and proplatelet formation. 9,10,16 Our study is the first to describe human MKL1 deficiency, and it demonstrates that although mild thrombocytopenia is associated with the condition, the major phenotype appears to relate to immunodeficiency.…”

Section: Discussionmentioning

confidence: 99%

Immunodeficiency and severe susceptibility to bacterial infection associated with a loss-of-function homozygous mutation of MKL1

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Malinova

Zenner

et al. 2015

Blood

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Key Points• MKL1 deficiency results in actin cytoskeletal disruption in myeloid and lymphoid cell lineages.• MKL1 deficiency impairs neutrophil migration associated with downregulation of myosin II.Megakaryoblastic leukemia 1 (MKL1), also known as MAL or myocardin-related transcription factor A (MRTF-A), is a coactivator of serum response factor, which regulates transcription of actin and actin cytoskeleton-related genes. MKL1 is known to be important for megakaryocyte differentiation and function in mice, but its role in immune cells is unexplored. Here we report a patient with a homozygous nonsense mutation in the MKL1 gene resulting in immunodeficiency characterized predominantly by susceptibility to severe bacterial infection. We show that loss of MKL1 protein expression causes a dramatic loss of filamentous actin (F-actin) content in lymphoid and myeloid lineage immune cells and widespread cytoskeletal dysfunction. MKL1-deficient neutrophils displayed reduced phagocytosis and almost complete abrogation of migration in vitro. Similarly, primary dendritic cells were unable to spread normally or to form podosomes. Silencing of MKL1 in myeloid cell lines revealed that F-actin assembly was abrogated through reduction of globular actin (G-actin) levels and disturbed expression of multiple actin-regulating genes. Impaired migration of these cells was associated with failure of uropod retraction likely due to altered contractility and adhesion, evidenced by reduced expression of the myosin light chain 9 (MYL9) component of myosin II complex and overexpression of CD11b integrin. Together, our results show that MKL1 is a nonredundant regulator of cytoskeleton-associated functions in immune cells and fibroblasts and that its depletion underlies a novel human primary immunodeficiency. (Blood. 2015;126(13):1527-1535

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Section: Discussionmentioning

confidence: 99%

Immunodeficiency and severe susceptibility to bacterial infection associated with a loss-of-function homozygous mutation of MKL1

Record

Malinova

Zenner

et al. 2015

Blood

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“…The results shown in Figure 9 indicate that several of the promegakaryocytic effects of BET inhibition occur through IGF2BP3 megakaryocyte morphogenesis. MKL1 undergoes upregulation, nuclear translocation, and transcriptional activation during megakaryopoiesis (46). Mkl1-deficient murine megakaryocytes display defects in polyploidization, enlargement, proliferation control, and proplatelet production (14,47,48), thus phenocopying normal human neonatal megakaryocytes.…”

Section: Discussionmentioning

confidence: 99%

Neonatal expression of RNA-binding protein IGF2BP3 regulates the human fetal-adult megakaryocyte transition

Elagib¹,

Lu²,

Mosoyan³

et al. 2017

Journal of Clinical Investigation

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“…27,28 The MPL-TR isoform, generated by exclusion of exons 9 and 10, is the sole isoform shared by humans and mice, and interspecies conservation of isoforms often predicts physiologic importance. 22 Mpl-FL is insufficient to rescue Mpl 2/2 HSC engraftment when expressed by a transgene using the c-Mpl promoter, thus supporting a necessary physiologic role for alternatively spliced Mpl isoforms.…”

Section: Org Frommentioning

confidence: 99%

Ott1 (Rbm15) regulates thrombopoietin response in hematopoietic stem cells through alternative splicing of c-Mpl

Xiao

Laha

Das

et al. 2015

Blood

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• Ott1 regulates the alternative splicing of Mpl-TR, a truncated isoform of c-Mpl, which modulates Thpomediated signaling.• Mpl-TR expression impairs HSC engraftment.Thrombopoietin (Thpo) signaling through the c-Mpl receptor promotes either quiescence or proliferation of hematopoietic stem cells (HSCs) in a concentration-dependent manner; however, in vivo Thpo serum levels are responsive to platelet mass rather than HSC demands, suggesting additional regulation exists. Ott1 (Rbm15), a spliceosomal component originally identified as a fusion partner in t(1;22)-associated acute megakaryocytic leukemia, is also essential for maintaining HSC quiescence under stress. Ott1 controls the alternative splicing of a dominant negative isoform, Mpl-TR, capable of inhibiting HSC engraftment and attenuating Thpo signaling. Ott1, which associates with Hdac3 and the histone methyltransferase, Setd1b, binds to both c-Mpl RNA and chromatin and regulates H4 acetylation and H3K4me3 marks. Histone deacetylase or histone methyltransferase inhibition also increases Mpl-TR levels, suggesting that Ott1 uses an underlying epigenetic mechanism to control alternative splicing of c-Mpl. Manipulation of Ott1-dependent alternative splicing may therefore provide a novel pharmacologic avenue for regulating HSC quiescence and proliferation in response to Thpo. (Blood. 2015;125(6):941-948)

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Induction of megakaryocyte differentiation drives nuclear accumulation and transcriptional function of MKL1 via actin polymerization and RhoA activation

Cited by 41 publications

References 36 publications

Immunodeficiency and severe susceptibility to bacterial infection associated with a loss-of-function homozygous mutation of MKL1

Immunodeficiency and severe susceptibility to bacterial infection associated with a loss-of-function homozygous mutation of MKL1

Neonatal expression of RNA-binding protein IGF2BP3 regulates the human fetal-adult megakaryocyte transition

Ott1 (Rbm15) regulates thrombopoietin response in hematopoietic stem cells through alternative splicing of c-Mpl

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