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A Functional Proteomic Method for the Enrichment of Peripheral Membrane Proteins Reveals the Collagen Binding Protein Hsp47 Is Exposed on the Surface of Activated Human Platelets

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NIAID Data Ecosystem2026-03-06 收录
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https://figshare.com/articles/dataset/A_Functional_Proteomic_Method_for_the_Enrichment_of_Peripheral_Membrane_Proteins_Reveals_the_Collagen_Binding_Protein_Hsp47_Is_Exposed_on_the_Surface_of_Activated_Human_Platelets/2852122
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Platelets are small blood cells vital for hemostasis. Following vascular damage, platelets adhere to collagens and activate, forming a thrombus that plugs the wound and prevents blood loss. Stimulation of the platelet collagen receptor glycoprotein VI (GPVI) allows recruitment of proteins to receptor-proximal signaling complexes on the inner-leaflet of the plasma membrane. These proteins are often present at low concentrations; therefore, signaling-complex characterization using mass spectrometry is limited due to high sample complexity. We describe a method that facilitates detection of signaling proteins concentrated on membranes. Peripheral membrane proteins (reversibly associated with membranes) were eluted from human platelets with alkaline sodium carbonate. Liquid-phase isoelectric focusing and gel electrophoresis were used to identify proteins that changed in levels on membranes from GPVI-stimulated platelets. Immunoblot analysis verified protein recruitment to platelet membranes and subsequent protein phosphorylation was preserved. Hsp47, a collagen binding protein, was among the proteins identified and found to be exposed on the surface of GPVI-activated platelets. Inhibition of Hsp47 abolished platelet aggregation in response to collagen, while only partially reducing aggregation in response to other platelet agonists. We propose that Hsp47 may therefore play a role in hemostasis and thrombosis.
创建时间:
2009-06-05
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