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人角质形成细胞的自主生长需要表皮生长因子受体被占据。

Autonomous growth of human keratinocytes requires epidermal growth factor receptor occupancy.

作者信息

Pittelkow M R, Cook P W, Shipley G D, Derynck R, Coffey R J

机构信息

Department of Dermatology, Mayo Clinic/Foundation, Rochester, Minnesota 55905.

出版信息

Cell Growth Differ. 1993 Jun;4(6):513-21.

PMID:8373735
Abstract

In the studies reported here, we demonstrate that transforming growth factor alpha (TGF-alpha) or epidermal growth factor (EGF) is required for the establishment of small colonies of human keratinocytes at clonal densities, but once small (10-15 cells) colonies have formed, the continued growth of these colonies can proceed in the absence of exogenous TGF-alpha or EGF. Equivalent receptor-binding concentrations of TGF-alpha and EGF were equipotent in stimulating colony formation. We also demonstrate that the growth of keratinocytes at high densities proceeds in the absence of exogenous peptide growth factors or hormones. The expression of TGF-alpha mRNA and protein is regulated by both cell density and the presence of exogenous growth factors. The addition of an antibody which blocks the mitogenic effect of mature TGF-alpha had no effect on the autocrine/paracrine growth of these cells at either density. However, monoclonal antibodies which antagonize ligand activation of the EGF receptor inhibit the autonomous proliferation of keratinocytes at high density and abrogate the exogenous TGF-alpha/EGF-independent expansion of colonies at clonal density. The results of these experiments are among the first evidence to demonstrate that normal human epithelial cells in culture exhibit autocrine/paracrine-mediated proliferation. Exogenous growth factors initiate colonies of human keratinocytes that become self-perpetuating in culture. Keratinocytes regulate production of the mitogenic ligand, TGF-alpha, through a density-dependent mechanism, and cell density stringently controls proliferation.

摘要

在本文报道的研究中,我们证明,在克隆密度下建立人角质形成细胞小集落需要转化生长因子α(TGF-α)或表皮生长因子(EGF),但一旦小(10 - 15个细胞)集落形成,这些集落的持续生长在没有外源性TGF-α或EGF的情况下也能进行。TGF-α和EGF的等效受体结合浓度在刺激集落形成方面具有同等效力。我们还证明,在高密度下角质形成细胞的生长在没有外源性肽生长因子或激素的情况下也能进行。TGF-α mRNA和蛋白的表达受细胞密度和外源性生长因子的存在的调节。添加一种阻断成熟TGF-α促有丝分裂作用的抗体,对这些细胞在任何一种密度下的自分泌/旁分泌生长均无影响。然而,拮抗EGF受体配体激活的单克隆抗体抑制高密度下角质形成细胞的自主增殖,并消除克隆密度下集落的外源性TGF-α/EGF非依赖性扩增。这些实验结果是最早证明培养的正常人上皮细胞表现出自分泌/旁分泌介导的增殖的证据之一。外源性生长因子启动人角质形成细胞集落,这些集落在培养中变得自我维持。角质形成细胞通过密度依赖性机制调节促有丝分裂配体TGF-α的产生,并且细胞密度严格控制增殖。

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