MAL/MRTF-A controls migration of non-invasive cells by upregulation of cytoskeleton-associated proteins

Leitner, Laura; Shaposhnikov, Dmitry; Mengel, Alexander; Descot, Arnaud; Julien, Sylvia; Hoffmann, Reinhard; Posern, Guido

doi:10.1242/jcs.092791

Cited by 65 publications

(58 citation statements)

References 52 publications

(96 reference statements)

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“…Furthermore, loss of CDH11 either in Cdh11 −/− mouse dermal fibroblasts or in shCDH11 human dermal fibroblasts abolished the expression of transcription factors known to affect ECM synthesis (Ueyama et al, 2003;Medjkane et al, 2009;Small et al, 2010;Leitner et al, 2011;Velasquez et al, 2013;Johnson et al, 2014;Parreno et al, 2014), such as MYOCD, MRTF-A, SRF and to a lesser extent MRTF-B. In agreement, knocking down either MYOCD or MRTF-A and -B decreased CDH11-mediated expression of collagen and elastin, but the effects of MRTF-A and -B were significantly stronger.…”

Section: Discussionmentioning

confidence: 56%

Cadherin-11 is a novel regulator of extracellular matrix synthesis and tissue mechanics

Row

Liu

Alimperti

et al. 2016

Journal of Cell Science

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We discovered that Cadherin-11 (CDH11) regulates collagen and elastin synthesis, both affecting the mechanical properties and contractile function of animal tissues. Using a Cdh11-null mouse model, we observed a significant reduction in the mechanical properties [Youngs' modulus and ultimate tensile strength (UTS)] of Cdh11 −/− as compared to wild-type (WT) mouse tissues, such as the aorta, bladder and skin. The deterioration of mechanical properties (Youngs' modulus and UTS) was accompanied by reduced collagen and elastin content in Cdh11 −/− mouse tissues as well as in cells in culture. Similarly, knocking down CDH11 abolished collagen and elastin synthesis in human cells, and consequently reduced their ability to generate force. Conversely, engagement of CDH11 through homophilic interactions, led to swift activation of the TGF-β and ROCK pathways as evidenced by phosphorylation of downstream effectors. Subsequently, activation of the key transcription factors, MRTF-A (also known as MKL1) and MYOCD led to significant upregulation of collagen and elastin genes. Taken together, our results demonstrate a novel role of adherens junctions in regulating extracellular matrix (ECM) synthesis with implications for many important biological processes, including maintenance of tissue integrity, wound healing and tissue regeneration.

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Section: Discussionmentioning

confidence: 56%

Cadherin-11 is a novel regulator of extracellular matrix synthesis and tissue mechanics

Row

Liu

Alimperti

et al. 2016

Journal of Cell Science

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“…In contrast, loss of MRTF-A reduced the levels of DSG1 messenger RNA (mRNA) in keratinocytes, suggesting that DSG1 is directly regulated by the SRF/MRTF-A complex . Another experiment showed that MRTF-A and SRF were recruited to cis-regulatory elements of the PKP2 gene to regulate its expression (Leitner et al 2011). Taken together, these data suggest that RhoA/MRTF-A signaling in keratinocytes affects the expression of desmosomal proteins directly and indirectly although the regulation via SRF/MRTF-A in response to mechanical strain has not been directly shown.…”

Section: Mechanosensitive Signaling Pathways In the Control Of Desmosmentioning

confidence: 93%

Desmosomes and Intermediate Filaments: Their Consequences for Tissue Mechanics

Hatzfeld

Keil

Magin

2017

Cold Spring Harb Perspect Biol

104

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Adherens junctions (AJs) and desmosomes connect the actin and keratin filament networks of adjacent cells into a mechanical unit. Whereas AJs function in mechanosensing and in transducing mechanical forces between the plasma membrane and the actomyosin cytoskeleton, desmosomes and intermediate filaments (IFs) provide mechanical stability required to maintain tissue architecture and integrity when the tissues are exposed to mechanical stress. Desmosomes are essential for stable intercellular cohesion, whereas keratins determine cell mechanics but are not involved in generating tension. Here, we summarize the current knowledge of the role of IFs and desmosomes in tissue mechanics and discuss whether the desmosome-keratin scaffold might be actively involved in mechanosensing and in the conversion of chemical signals into mechanical strength.

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“…1a-d) that MRFT-A induced hallmarks of angiogenesisthat is, migration and tube formation of cultured human microvascular endothelial cells-to a similar extent as T 4. The pro-angiogenic effect of MRTF-A was dependent on the G-acting-binding motif of T 4, as mutating this domain and annihilating G-acting binding abolished the T 4 effect on vessel growth, as did a short-hairpin RNA (shRNA) interfering simultaneously with MRTF-A and B transcription (MRTF-shRNA) 27 . Consistently, T 4 enhanced nuclear MRTF-A translocation (Fig.…”

Section: T 4 and Mrtf-mentioning

confidence: 99%

MRTF-A controls vessel growth and maturation by increasing the expression of CCN1 and CCN2

et al. 2014

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Gradual occlusion of coronary arteries may result in reversible loss of cardiomyocyte function (hibernating myocardium), which is amenable to therapeutic neovascularization. The role of myocardin-related transcription factors (MRTFs) co-activating serum response factor (SRF) in this process is largely unknown. Here we show that forced MRTF-A expression induces CCN1 and CCN2 to promote capillary proliferation and pericyte recruitment, respectively. We demonstrate that, upon G-actin binding, thymosin 4 (T 4), induces MRTF translocation to the nucleus, SRF-activation and CCN1/2 transcription. In a murine ischaemic hindlimb model, MRTF-A or T 4 promotes neovascularization, whereas loss of MRTF-A/B or CCN1-function abrogates the T 4 effect. We further show that, in ischaemic rabbit hindlimbs, MRTF-A as well as T 4 induce functional neovascularization, and that this process is inhibited by angiopoietin-2, which antagonizes pericyte recruitment. Moreover, MRTF-A improves contractile function of chronic hibernating myocardium of pigs to a level comparable to that of transgenic pigs overexpressing T 4 (T 4tg). We conclude that MRTF-A promotes microvessel growth (via CCN1) and maturation (via CCN2), thereby enabling functional improvement of ischaemic muscle tissue.

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MAL/MRTF-A controls migration of non-invasive cells by upregulation of cytoskeleton-associated proteins

Cited by 65 publications

References 52 publications

Cadherin-11 is a novel regulator of extracellular matrix synthesis and tissue mechanics

Cadherin-11 is a novel regulator of extracellular matrix synthesis and tissue mechanics

Desmosomes and Intermediate Filaments: Their Consequences for Tissue Mechanics

MRTF-A controls vessel growth and maturation by increasing the expression of CCN1 and CCN2

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