溶血磷脂酸受体lpa(2)(Edg4)和lpa(1)/lpa(2)(Edg2/Edg4)基因敲除小鼠的特征:信号缺陷但无明显可归因于lpa(2)的表型异常。
Characterization of lpa(2) (Edg4) and lpa(1)/lpa(2) (Edg2/Edg4) lysophosphatidic acid receptor knockout mice: signaling deficits without obvious phenotypic abnormality attributable to lpa(2).
作者信息
Contos James J A, Ishii Isao, Fukushima Nobuyuki, Kingsbury Marcy A, Ye Xiaoqin, Kawamura Shuji, Brown Joan Heller, Chun Jerold
机构信息
Department of Pharmacology, Neurosciences and Biomedical Sciences Programs, School of Medicine, University of California, San Diego, La Jolla 92093-0636, USA.
出版信息
Mol Cell Biol. 2002 Oct;22(19):6921-9. doi: 10.1128/MCB.22.19.6921-6929.2002.
Lysophosphatidic acid (LPA), a bioactive lipid produced by several cell types including postmitotic neurons and activated platelets, is thought to be involved in various biological processes, including brain development. Three cognate G protein-coupled receptors encoded by lpa(1)/lp(A1)/Edg-2/Gpcr26, lpa(2)/lp(A2)/Edg-4, and lpa(3)/lp(A3)/Edg-7 mediate the cellular effects of LPA. We have previously shown that deletion of lpa(1) in mice results in craniofacial dysmorphism, semilethality due to defective suckling behavior, and generation of a small fraction of pups with frontal hematoma. To further investigate the role of these receptors and LPA signaling in the organism, we deleted lpa(2) in mice. Homozygous knockout (lpa(2)((-/-))) mice were born at the expected frequency and displayed no obvious phenotypic abnormalities. Intercrosses allowed generation of lpa(1)((-/-)) lpa(2)((-/-)) double knockout mice, which displayed no additional phenotypic abnormalities relative to lpa(1)((-/-)) mice except for an increased incidence of perinatal frontal hematoma. Histological analyses of lpa(1)((-/-)) lpa(2)((-/-)) embryonic cerebral cortices did not reveal obvious differences in the proliferating cell population. However, many LPA-induced responses, including phospholipase C activation, Ca(2+) mobilization, adenylyl cyclase activation, proliferation, JNK activation, Akt activation, and stress fiber formation, were absent or severely reduced in embryonic fibroblasts derived from lpa(1)((-/-)) lpa(2)((-/-)) mice. Except for adenylyl cyclase activation [which was nearly abolished in lpa(1)((-/-)) fibroblasts], these responses were only partially affected in lpa(1)((-/-)) and lpa(2)((-/-)) fibroblasts. Thus, although LPA(2) is not essential for normal mouse development, it does act redundantly with LPA(1) to mediate most LPA responses in fibroblasts.
溶血磷脂酸(LPA)是一种由多种细胞类型产生的生物活性脂质,包括有丝分裂后的神经元和活化的血小板,被认为参与多种生物学过程,包括大脑发育。由lpa(1)/lp(A1)/Edg-2/Gpcr26、lpa(2)/lp(A2)/Edg-4和lpa(3)/lp(A3)/Edg-7编码的三种同源G蛋白偶联受体介导LPA的细胞效应。我们之前已经表明,小鼠中lpa(1)的缺失会导致颅面畸形、因哺乳行为缺陷导致的半致死性,以及一小部分患有额叶血肿的幼崽的产生。为了进一步研究这些受体和LPA信号在生物体中的作用,我们在小鼠中删除了lpa(2)。纯合敲除(lpa(2)((-/-))小鼠以预期频率出生,且未表现出明显的表型异常。杂交产生了lpa(1)((-/-)) lpa(2)((-/-))双敲除小鼠,与lpa(1)((-/-))小鼠相比,除围产期额叶血肿发生率增加外,未表现出其他额外的表型异常。对lpa(1)((-/-)) lpa(2)((-/-))胚胎大脑皮层的组织学分析未发现增殖细胞群体有明显差异。然而,在源自lpa(1)((-/-)) lpa(2)((-/-))小鼠的胚胎成纤维细胞中,许多LPA诱导的反应,包括磷脂酶C激活、Ca(2+)动员、腺苷酸环化酶激活、增殖、JNK激活、Akt激活和应力纤维形成,均不存在或严重减少。除了腺苷酸环化酶激活(在lpa(1)((-/-))成纤维细胞中几乎被完全消除)外,这些反应在lpa(1)((-/-))和成纤维细胞中仅受到部分影响。因此,虽然LPA(2)对于正常小鼠发育不是必需的,但它确实与LPA(1)协同作用,以介导成纤维细胞中的大多数LPA反应。
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