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细胞外基质对转基因小鼠乳腺细胞中β-乳球蛋白/人血清白蛋白基因表达的双重调控

Dual regulation of beta-lactoglobulin/human serum albumin gene expression by the extracellular matrix in mammary cells from transgenic mice.

作者信息

Ilan N, Barash I, Faerman A, Shani M

机构信息

Institute of Animal Science, Volcani Center, ARO, Bet Dagan, Israel.

出版信息

Exp Cell Res. 1996 Apr 10;224(1):28-38. doi: 10.1006/excr.1996.0108.

Abstract

Mammary explants and epithelial cell cultures from transgenic mice carrying the human serum albumin (HSA) gene or minigenes behind the regulatory sequences of the ovine beta-lactoglobulin gene were analyzed. Previously we demonstrated that mammary explants from virgin female transgenic mice synthesize and secrete high levels of HSA during the first day in culture. Here we present a detailed analysis of endogenous and transgene expression during the first 20 h of mammary explant cultures. We show that HSA genes as well as endogenous milk protein genes are rapidly induced upon explantation. Unexpectedly, HSA was synthesized also in mammary explants from strains that do not secrete HSA into the milk, indicating the existence of a cryptic potential to express the transgene. Histological examination revealed that some luminal epithelial cells detached from the underlying extracellular matrix (ECM) soon after explantation. Epithelial cell cultures from nonsecreting strains grown on plastic rapidly induced transgene expression and secreted higher levels of HSA into the medium compared to cells grown on collagen. These results suggest that tissue organization and most likely the interaction of epithelial cells with the ECM are intimately involved in the control of HSA transgene expression.

摘要

对携带人血清白蛋白(HSA)基因或在绵羊β-乳球蛋白基因调控序列后的小基因的转基因小鼠的乳腺外植体和上皮细胞培养物进行了分析。之前我们证明,来自处女雌性转基因小鼠的乳腺外植体在培养的第一天合成并分泌高水平的HSA。在此,我们对乳腺外植体培养的前20小时内的内源性和转基因表达进行了详细分析。我们发现,外植体接种后,HSA基因以及内源性乳蛋白基因会迅速被诱导表达。出乎意料的是,在那些不向乳汁中分泌HSA的品系的乳腺外植体中也合成了HSA,这表明存在表达转基因的潜在隐性能力。组织学检查显示,一些腔上皮细胞在接种后不久就从下面的细胞外基质(ECM)上脱离。与在胶原蛋白上生长的细胞相比,在塑料上生长的非分泌品系的上皮细胞培养物能迅速诱导转基因表达,并向培养基中分泌更高水平的HSA。这些结果表明,组织结构以及上皮细胞与ECM之间很可能存在的相互作用密切参与了HSA转基因表达的调控。

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