Clot retraction is mediated by factor XIII-dependent fibrin-αIIbβ3-myosin axis in platelet sphingomyelin-rich membrane rafts

Kasahara, Kohji; Kaneda, Mizuho; Miki, Takeo; Iida, Kei; Sekino-Suzuki, Naoko; Kawashima, Ichiro; Suzuki, Hidenori; Shimonaka, Motoyuki; Arai, Morio; Ohno‐Iwashita, Yoshiko; Kojima, Soichi; Abe, Mitsuhiro; Kobayashi, Toshihide; Okazaki, Toshiro; Souri, Masayoshi; Ichinose, Akitada; Yamamoto, Naomasa

doi:10.1182/blood-2013-04-491290

Cited by 77 publications

(83 citation statements)

References 36 publications

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“…The isolated cells from freshly drawn blood were sandwiched between two carriers. Platelets were prepared from freshly drawn blood as previously reported (Kasahara et al, 2013). The platelet-rich plasma was activated with 0.5 units/ml thrombin (Sigma-Aldrich) for 3 min at 37˚C.…”

Section: Methodsmentioning

confidence: 99%

Transbilayer lipid distribution in nano scale

Murate

Abe

Kasahara

et al. 2015

Journal of Cell Science

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110

107

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There is a limited number of methods to examine transbilayer lipid distribution in biomembranes. We employed freeze-fracture replicalabelling immunoelectron microscopy in combination with lipidbinding proteins and a peptide to examine both transbilayer distribution and lateral distribution of various phospholipids in mammalian cells. Our results indicate that phospholipids are exclusively distributed either in the outer or inner leaflet of human red blood cell (RBC) membranes. In contrast, in nucleated cells, such as human skin fibroblasts and neutrophils, sphingomyelin was distributed in both leaflets while exhibiting characteristic lipid domains in the inner leaflet. Similar to RBCs, lipid asymmetry was maintained both in resting and thrombin-activated platelets. However, the microparticles released from thrombin-activated platelets lost membrane asymmetry. Our results suggest that the microparticles were shed from platelet plasma membrane domains enriched with phosphatidylserine and/or phosphatidylinositol at the outer leaflet. These findings underscore the strict regulation and cell-type specificity of lipid asymmetry in the plasma membrane.

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Section: Methodsmentioning

confidence: 99%

Transbilayer lipid distribution in nano scale

Murate

Abe

Kasahara

et al. 2015

Journal of Cell Science

Self Cite

110

107

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“…Sphingomyelin-rich rafts localize in the central region of adhering platelets with thrombin, whereas cholesterol-rich rafts localize evenly on the membrane. Sphingomyelin-rich rafts act as platforms of fibrin-mediated outside-in signals, leading to clot retraction (19). These observations suggest that lipid rafts are compositionally and functionally heterogeneous (20).…”

Section: Heterogeneity In Lipid Raftsmentioning

confidence: 81%

Lipid Rafts and Anti-Glycolipid Antibodies

Kasahara¹

2014

TIGG

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Lipid rafts are dynamic assemblies of glycosphingolipids, cholesterol, and proteins that can be stabilized into platforms in- A. IntroductionLipid rafts are dynamic assemblies of glycosphingolipids, sphingomyelin, cholesterol, and proteins that can be stabilized into platforms involved in the regulation of a number of vital cellular processes (1). Low-density, detergent-resistant membrane fractions can be isolated from cells by sucrose density gradient centrifugation. These membrane fractions are rich in glycosphingolipids, sphingomyelin, cholesterol, and a variety of signaling molecules.

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“…Lipid rafts are about 10-200 nm in lipidordered microdomains enriched with sphingomyelin, glycosphingolipids and cholesterol (Rabani, Davani, Gambert-Nicot, Meneveau and Montange, 2016;Thomas et al, 2014). It is now established that some platelet proteins, such as P2Y12 (Savi et al, 2006) and FXIII (Kasahara et al, 2013)need to be on lipid rafts to be functional.…”

Section: Proteomics: the Current Center Of Attentionmentioning

confidence: 99%

“…Lipidomics provided a good tool for identification of plasma membrane fractions and characterization of these microdomains (Figure 4) by establishing the ratio of cholesterol/sphingomyelin in lipid raft microdomains (Koumanov et al, 2005;Wolf and Quinn, 2008). These microdomains are the focus of attention in membrane biological research and are implicated in cardiovascular diseases through their participation in platelet activation (Kasahara et al, 2013;Savi et al, 2006), monocyte membrane reorganization (Salvary et al, 2012) and in the mechanisms mediating drug effects (García and Senis, 2011;Zinzalla and Thurston, 2009 ! 8 Figure 4.…”

Section: Rabanimentioning

confidence: 99%

Translational Approaches In Cardiovascular Diseases by Omics

Davani¹

2018

Current Issues in Molecular Biology

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Cardiovascular diseases are among the leading causes of morbidity and mortality. Despite scientific and technical progress in risk prediction, diagnostics, prognostication and therapy of cardiovascular pathologies, new biomarkers and therapeutic targets remain the subject of intense research to reduce the burden of these diseases.High throughput analyses, termed "omics", are a promising avenue of research. These recently developed technical fields have revolutionized biological and medical research in a very short time. By their interdisciplinary nature, these new methods have already provided a wide vision of cell and tissue pathways and functions. Here, we review how these methods can help to discover new biomarkers and therapeutic targets in cardiovascular diseases.

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Clot retraction is mediated by factor XIII-dependent fibrin-αIIbβ3-myosin axis in platelet sphingomyelin-rich membrane rafts

Cited by 77 publications

References 36 publications

Transbilayer lipid distribution in nano scale

Transbilayer lipid distribution in nano scale

Lipid Rafts and Anti-Glycolipid Antibodies

Translational Approaches In Cardiovascular Diseases by Omics

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