Small proline-rich protein 1A is a gp130 pathway- and stress-inducible cardioprotective protein |
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Authors: | Pradervand Sylvain Yasukawa Hideo Muller Olivier G Kjekshus Harald Nakamura Tomoyuki St Amand Tara R Yajima Toshitaka Matsumura Kiyoyuki Duplain Hervé Iwatate Mitsuo Woodard Sarah Pedrazzini Thierry Ross John Firsov Dmitri Rossier Bernard C Hoshijima Masahiko Chien Kenneth R |
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Affiliation: | UCSD Institute of Molecular Medicine, University of California, San Diego, La Jolla, CA, USA. |
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Abstract: | The interleukin-6 cytokines, acting via gp130 receptor pathways, play a pivotal role in the reduction of cardiac injury induced by mechanical stress or ischemia and in promoting subsequent adaptive remodeling of the heart. We have now identified the small proline-rich repeat proteins (SPRR) 1A and 2A as downstream targets of gp130 signaling that are strongly induced in cardiomyocytes responding to biomechanical/ischemic stress. Upregulation of SPRR1A and 2A was markedly reduced in the gp130 cardiomyocyte-restricted knockout mice. In cardiomyocytes, MEK1/2 inhibitors prevented SPRR1A upregulation by gp130 cytokines. Furthermore, binding of NF-IL6 (C/EBPbeta) and c-Jun to the SPRR1A promoter was observed after CT-1 stimulation. Histological analysis revealed that SPRR1A induction after mechanical stress of pressure overload was restricted to myocytes surrounding piecemeal necrotic lesions. A similar expression pattern was found in postinfarcted rat hearts. Both in vitro and in vivo ectopic overexpression of SPRR1A protected cardiomyocytes against ischemic injury. Thus, this study identifies SPRR1A as a novel stress-inducible downstream mediator of gp130 cytokines in cardiomyocytes and documents its cardioprotective effect against ischemic stress. |
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Keywords: | gp130 IL-6 cytokines myocardium stress SPRR1A |
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