Proplatelet formation is regulated by the Rho/ROCK pathway

Chang, Yunhua; Aurade, Frédéric; Larbret, Frédéric; Zhang, Yanyan; Couédic, Jean-Pierre Le; Momeux, Laurence; Larghero, Jérôme; Bertoglio, Jacques; Louache, Fawzia; Cramer, Elisabeth M.; Vainchenker, William; Debili, Najet

doi:10.1182/blood-2006-04-020024

Cited by 153 publications

(200 citation statements)

References 42 publications

(48 reference statements)

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“…Depending on the experiments, MKs were sorted according to CD41, or CD41 and CD42 expression using Influx flow cytometer (BD, Mountain View, CA) 42 .…”

Section: Methodsmentioning

confidence: 99%

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RUNX1-induced silencing of non-muscle myosin heavy chain IIB contributes to megakaryocyte polyploidization

et al. 2012

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megakaryocytes are unique mammalian cells that undergo polyploidization (endomitosis) during differentiation, leading to an increase in cell size and protein production that precedes platelet production. Recent evidence demonstrates that endomitosis is a consequence of a late failure in cytokinesis associated with a contractile ring defect. Here we show that the non-muscle myosin IIB heavy chain (mYH10) is expressed in immature megakaryocytes and specifically localizes in the contractile ring. mYH10 downmodulation by short hairpin RnA increases polyploidization by inhibiting the return of 4n cells to 2n, but other regulators, such as of the G1/s transition, might regulate further polyploidization of the 4n cells. Conversely, re-expression of mYH10 in the megakaryocytes prevents polyploidization and the transition of 2n to 4n cells. During polyploidization, mYH10 expression is repressed by the major megakaryocyte transcription factor RunX1. Thus, RunX1-mediated silencing of mYH10 is required for the switch from mitosis to endomitosis, linking polyploidization with megakaryocyte differentiation.

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“…Depending on the experiments, MKs were sorted according to CD41, or CD41 and CD42 expression using Influx flow cytometer (BD, Mountain View, CA) 42 .…”

Section: Methodsmentioning

confidence: 99%

“…Immunofluorescence was performed on CD41 + MK sorted at day 6 of human culture 42 or day 2 of murine culture derived from Lin − liver fetal cells. Cells were examined under the Zeiss LSM.…”

mentioning

confidence: 99%

RUNX1-induced silencing of non-muscle myosin heavy chain IIB contributes to megakaryocyte polyploidization

et al. 2012

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“…31,32 Recent findings have shown that NMMHC-IIA attenuates proplatelet formation, 33,34 which occurs in terminally mature megakaryocytes where most of the cytoplasm is converted into lengthy beaded extensions. 35 Thus, NMMHC-IIA might restrain thrombopoiesis until megakaryocytes accumulate sufficient quantities of the materials required for optimal platelet assembly; loss of myosin-IIA function could trigger precocious proplatelet formation, whereas gain-of-function mutations might limit platelet production.…”

Section: Discussionmentioning

confidence: 99%

Differential expression of wild-type and mutant NMMHC-IIA polypeptides in blood cells suggests cell-specific regulation mechanisms in MYH9 disorders

Kunishima

Hamaguchi

Saito

2008

Blood

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MYH9 disorders such as May-Hegglin anomaly are characterized by macrothrombocytopenia and cytoplasmic granulocyte inclusion bodies that result from mutations in MYH9, the gene for nonmuscle myosin heavy chain-IIA (NMMHC-IIA). We examined the expression of mutant NMMHC-IIA polypeptide in peripheral blood cells from patients with MYH9 5770delG and 5818delG mutations. A specific antibody to mutant NMMHC-IIA (NT629) was raised against the abnormal carboxyl-terminal residues generated by 5818delG. NT629 reacted to recombinant 5818delG NMMHC-IIA but not to wild-type NMMHC-IIA, and did not recognize any cellular components of normal peripheral blood cells. Immunofluorescence and immunoblotting revealed that mutant NMMHC-IIA was present and sequestrated only in inclusion bodies within neutrophils, diffusely distributed throughout lymphocyte cytoplasm, sparsely localized on a diffuse cytoplasmic background in monocytes, and uniformly distributed at diminished levels only in large platelets. Mutant NMMHC-IIA did not translocate to lamellipodia in surface activated platelets. Wild-type NMMHC-IIA was homogeneously distributed among megakaryocytes derived from the peripheral blood CD34 ؉ cells of patients, but coarse mutant NMMHC-IIA was heterogeneously scattered without abnormal aggregates in the cytoplasm. We show the differential expression of mutant NMMHC IntroductionMYH9 disorders are autosomal dominant macrothrombocytopenias characterized by giant platelets, thrombocytopenia, and Döhle body-like inclusion bodies in the cytoplasm of granulocytes. [1][2][3] These disorders are caused by heterozygous mutations in MYH9, which encodes nonmuscle myosin heavy chain-IIA (NMMHC-IIA), and include the May-Hegglin anomaly, Sebastian, Fechtner, and Epstein syndromes, Alport-like syndrome with macrothrombocytopenia, and nonsyndromic deafness (DFNA17). [4][5][6] An MYH9 mutation is always associated with macrothrombocytopenia and granulocyte inclusion bodies from birth, but it does not predict the development of Alport manifestations, including nephritis, deafness, and cataracts. A mutation of MYH9 alone does not seem to cause associated Alport manifestations, and unknown genetic and/or epigenetic factors might influence the phenotypic consequences of MYH9 mutations. [7][8][9][10] Although the molecular mechanisms of hematologic abnormalities are under investigation, those of the kidney, cochlea, and lens are completely unknown.We previously showed that NMMHC-IIA polypeptide accumulates in neutrophil cytoplasm and forms inclusion bodies in patients with MYH9 disorders. The nature of the cytoplasmic accumulation can be classified according to the number, size, and shape of accumulated NMMHC-IIA granules, into types I, II, and III. Type I comprises 1 or 2 large (0.5-2 m), intensely stained, oval-to spindle-shaped cytoplasmic NMMHC-IIA-positive granules. Type II comprises up to 20 circular to oval cytoplasmic spots (Յ 1 m). Type III appears as speckled staining. Furthermore, the pattern of localization correlates with the site of MYH9 ...

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“…In the erythroblast, myosin II could function in an actomyosin contractile apparatus responsible for maintaining a normal cell shape during cell condensation. Rho/ROCK-1 pathway has been shown to be involved in other differentiation systems, including proplatelet formation through MLC2 phosphorylation, 30 and keratinocyte differentiation through stratification and enlargement of cell size. 31 Recent findings also define a cytoskeleton-independent function for ROCK in regulating morphogenesis and cell size Figure 7 ROCK-1 is the main MLC2-regulating kinase.…”

Section: Discussionmentioning

confidence: 99%

“…Retrovirus MIGR-GFP and the retrovirus expressing the dominant-negative form of Rho MIGR RhoA-N19, were produced as described. 30 Erythroid cell infection. CD34 þ cells isolated from cord blood were cultured for 5 days as described then infected by shRNA GIPZ lentiviruses or MIGR-GFP retroviruses.…”

Section: Methodsmentioning

confidence: 99%

Caspase-activated ROCK-1 allows erythroblast terminal maturation independently of cytokine-induced Rho signaling

et al. 2010

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Stem cell factor (SCF) and erythropoietin are strictly required for preventing apoptosis and stimulating proliferation, allowing the differentiation of erythroid precursors from colony-forming unit-E to the polychromatophilic stage. In contrast, terminal maturation to generate reticulocytes occurs independently of cytokine signaling by a mechanism not fully understood. Terminal differentiation is characterized by a sequence of morphological changes including a progressive decrease in cell size, chromatin condensation in the nucleus and disappearance of organelles, which requires transient caspase activation. These events are followed by nucleus extrusion as a consequence of plasma membrane and cytoskeleton reorganization. Here, we show that in early step, SCF stimulates the Rho/ROCK pathway until the basophilic stage. Thereafter, ROCK-1 is activated independently of Rho signaling by caspase-3-mediated cleavage, allowing terminal maturation at least in part through phosphorylation of the light chain of myosin II. Therefore, in this differentiation system, final maturation occurs independently of SCF signaling through caspase-induced ROCK-1 kinase activation.

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Proplatelet formation is regulated by the Rho/ROCK pathway

Cited by 153 publications

References 42 publications

RUNX1-induced silencing of non-muscle myosin heavy chain IIB contributes to megakaryocyte polyploidization

RUNX1-induced silencing of non-muscle myosin heavy chain IIB contributes to megakaryocyte polyploidization

Differential expression of wild-type and mutant NMMHC-IIA polypeptides in blood cells suggests cell-specific regulation mechanisms in MYH9 disorders

Caspase-activated ROCK-1 allows erythroblast terminal maturation independently of cytokine-induced Rho signaling

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