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The proteasome regulates collagen-induced platelet aggregation via nuclear-factor-kappa-B (NFĸB) activation

Thrombosis Research, ISSN: 0049-3848, Vol: 148, Page: 15-22
2016
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Article Description

Platelets possess critical hemostatic functions in the system of thrombosis and hemostasis, which can be affected by a multitude of external factors. Previous research has shown that platelets have the capacity to synthesize proteins de novo and more recently a multicatalytic protein complex, the proteasome, has been discovered in platelets. Due to its vital function for cellular integrity, the proteasome has become a therapeutic target for anti -proliferative drug therapies in cancer. Clinically thrombocytopenia is a frequent side-effect, but the aggregatory function of platelets also appears to be affected. Little is known however about underlying regulatory mechanisms and functional aspects of proteasome inhibition on platelets. Our study aims to investigate the role of the proteasome in regulating collagen-induced platelet aggregation and its interaction with NFkB in this context.

Bibliographic Details

Grundler, Katharina; Rotter, Raffaela; Tilley, Sloane; Pircher, Joachim; Czermak, Thomas; Yakac, Mustaf; Gaitzsch, Erik; Massberg, Steffen; Krötz, Florian; Sohn, Hae-Young; Pohl, Ulrich; Mannell, Hanna; Kraemer, Bjoern F

Elsevier BV

Medicine

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