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P物质对平滑肌细胞的反应性受整合素配体血小板反应蛋白调节。

Substance P responsiveness of smooth muscle cells is regulated by the integrin ligand, thrombospondin.

作者信息

Dahm L M, Bowers C W

机构信息

Division of Neurosciences, Beckman Research Institute of the City of Hope, Duarte, CA 91010, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Feb 6;93(3):1276-81. doi: 10.1073/pnas.93.3.1276.

Abstract

The extracellular factors that determine a cell's responsiveness to neurotransmitters are of particular relevance for pharmacologically diverse cell types such as neurons and smooth muscle. We previously demonstrated that matrix-associated factors are capable of dramatically and specifically suppressing the responsiveness of smooth muscle to the neuropeptide, substance P. We now demonstrate that this influence of extracellular matrix on the pharmacological phenotype of smooth muscle cells can be blocked specifically by an Arg-Gly-Asp (RGD)-containing antagonist of integrins. Of a battery of integrin ligands tested, only thrombospondin mimicked the effect of the extracellular matrix on substance P responsiveness. This effect of thrombospondin was dose dependent, RGD sensitive, and blocked by an antibody directed against the RGD-containing region of thrombospondin. Because the mRNA for thrombospondin is present in the cells of the chicken amnion, this extracellular factor may normally suppress substance P responsiveness in amniotic smooth muscle. The results suggest a role for matrix-associated integrin ligands in the regulation of cellular responses to specific neurotransmitters and hormones and in the development and maintenance of tissue-specific pharmacological properties.

摘要

决定细胞对神经递质反应性的细胞外因子,对于神经元和平滑肌等药理学特性多样的细胞类型尤为重要。我们之前证明,与基质相关的因子能够显著且特异性地抑制平滑肌对神经肽P物质的反应性。我们现在证明,细胞外基质对平滑肌细胞药理学表型的这种影响可被一种含精氨酸-甘氨酸-天冬氨酸(RGD)的整合素拮抗剂特异性阻断。在所测试的一系列整合素配体中,只有血小板反应蛋白模拟了细胞外基质对P物质反应性的影响。血小板反应蛋白的这种作用具有剂量依赖性、RGD敏感性,并被一种针对血小板反应蛋白含RGD区域的抗体所阻断。由于鸡羊膜细胞中存在血小板反应蛋白的mRNA,这种细胞外因子可能正常情况下会抑制羊膜平滑肌中P物质的反应性。这些结果表明,与基质相关的整合素配体在调节细胞对特定神经递质和激素的反应以及组织特异性药理学特性的发育和维持中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0a26/40070/e3c3359da932/pnas01507-0326-a.jpg

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