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表皮生长因子和转化生长因子-β对胎儿肺中分子量为35,000的表面活性物质相关蛋白合成的不同影响。

Differential effects of epidermal growth factor and transforming growth factor-beta on synthesis of Mr = 35,000 surfactant-associated protein in fetal lung.

作者信息

Whitsett J A, Weaver T E, Lieberman M A, Clark J C, Daugherty C

出版信息

J Biol Chem. 1987 Jun 5;262(16):7908-13.

PMID:3495535
Abstract

Differentiation of pulmonary Type II epithelial cells in late gestation is associated with the synthesis of pulmonary surfactant required for adaptation to air breathing at birth. In the present work, induction of synthesis of a Type II epithelial cell protein, surfactant-associated glycoprotein of Mr = 35,000 (SAP-35) was studied in human fetal lung tissue obtained at 15-24 weeks of gestation. SAP-35 content increased during organ culture in the absence of exogenous hormones. Epidermal growth factor or triiodothyronine stimulated the induction of SAP-35 synthesis during culture. Stimulation by epidermal growth factor (EGF) was detected as early as 2 days and persisted for up to 5 days in culture. Response to EGF was dose-dependent (0.01-10 ng/ml) and was associated with enhanced incorporation of [35S]methionine into immunoprecipitable SAP-35. Increased SAP-35 synthesis was associated with increased SAP-35 RNA as assessed by Northern blot and hybridization assays with human SAP-35 cDNA. Effects of EGF were comparable to the induction of SAP-35 synthesis by 8-bromo-cAMP. In contrast to the stimulatory effect of EGF and triiodothyronine, SAP-35 content was inhibited by transforming growth factor-beta. Both the stimulatory and inhibitory effects of these agents on SAP-35 content were associated with concomitant changes in SAP-35 synthesis. These findings demonstrate multihormonal control of SAP-35 expression and strongly implicate both EGF and transforming growth factor-beta in the regulation of surfactant apoprotein synthesis.

摘要

妊娠后期肺Ⅱ型上皮细胞的分化与出生时适应空气呼吸所需的肺表面活性物质的合成有关。在本研究中,我们对妊娠15 - 24周获取的人胎儿肺组织中Ⅱ型上皮细胞蛋白(分子量为35,000的表面活性物质相关糖蛋白,即SAP - 35)合成的诱导情况进行了研究。在无外源性激素的器官培养过程中,SAP - 35含量增加。表皮生长因子或三碘甲状腺原氨酸在培养过程中刺激了SAP - 35合成的诱导。表皮生长因子(EGF)的刺激最早在培养2天时即可检测到,并在培养中持续长达5天。对EGF的反应呈剂量依赖性(0.01 - 10 ng/ml),且与[35S]甲硫氨酸掺入可免疫沉淀的SAP - 35增加有关。通过Northern印迹和与人SAP - 35 cDNA的杂交分析评估,SAP - 35合成增加与SAP - 35 RNA增加相关。EGF的作用与8 - 溴 - cAMP诱导的SAP - 35合成相当。与EGF和三碘甲状腺原氨酸的刺激作用相反,转化生长因子 - β抑制了SAP - 35含量。这些因子对SAP - 35含量的刺激和抑制作用均与SAP - 35合成的相应变化有关。这些发现证明了对SAP - 35表达的多激素控制,并强烈提示EGF和转化生长因子 - β均参与表面活性物质载脂蛋白合成的调节。

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