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Cellular polarity modulates drug resistance in primary colorectal cancers via orientation of the multidrug resistance protein ABCB1

机译:细胞极性通过多药耐药蛋白ABCB1的方向调节原发性大肠癌的耐药性

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摘要

Colonic epithelial cells are highly polarised with a lumen‐facing apical membrane, termed the brush border, and a basal membrane in contact with the underlying extracellular matrix (ECM). This polarity is often maintained in cancer tissue in the form of neoplastic glands and has prognostic value. We compared the cellular polarity of several ex vivo spheroid colonic cancer cultures with their parental tumours and found that those grown as non‐attached colonies exhibited apical brush border proteins on their outer cellular membranes. Transfer of these cultures to an ECM, such as collagen, re‐established the centralised apical polarity observed in vivo. The multidrug resistance protein ABCB1 also became aberrantly polarised to outer colony membranes in suspension cultures, unlike cultures grown in collagen, where it was polarised to central lumens. This polarity switch was dependent on the presence of serum or selected serum components, including epidermal growth factor (EGF), transforming growth factor‐β1 (TGF‐β1) and insulin‐like growth factor‐1 (IGF‐1). The apical/basal orientation of primary cancer colon cultures cultured in collagen/serum was modulated by α2β1 integrin signalling. The polarisation of ABCB1 in colonies significantly altered drug uptake and sensitivity, as the outward polarisation of ABCB1 in suspension colonies effluxed substrates more effectively than ECM‐grown colonies with ABCB1 polarised to central lumens. Thus, serum‐free suspension colonies were more resistant to a variety of anti‐cancer drugs than ECM‐grown colonies. In conclusion, the local stroma, or absence thereof, can have profound effects on the sensitivity of colorectal cultures to drugs that are ABCB1 substrates. © 2018 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.
机译:结肠上皮细胞高度极化,具有面向内腔的顶膜(称为刷状缘)和与下层细胞外基质(ECM)接触的基底膜。这种极性通常以肿瘤性腺体的形式保持在癌组织中,并具有预后价值。我们将几种离体球状结肠癌培养物的细胞极性与其亲本肿瘤进行了比较,发现以非附着菌落形式生长的那些在其细胞外膜上均显示出顶端的刷状缘蛋白。这些文化转移到ECM,如胶原蛋白,重新建立了体内观察到的集中的顶端极性。在悬浮培养中,多药耐药蛋白ABCB1也异常地极化到外菌落膜,这与胶原蛋白中生长的培养物不同,在极化时它会极化到中心腔。这种极性转换取决于血清或所选血清成分的存在,包括表皮生长因子(EGF),转化生长因子β1(TGF-β1)和胰岛素样生长因子-1(IGF-1)。在胶原蛋白/血清中培养的原发癌结肠培养物的顶/基方向受α2β1整联蛋白信号调节。菌落中ABCB1的极化显着改变了药物的吸收和敏感性,因为悬浮菌落中ABCB1的向外极化比ECM生长的菌落中ABCB1极化到中心管腔更有效。因此,无血清的悬浮菌落比ECM生长的菌落对多种抗癌药物更具抵抗力。总之,局部基质或不存在基质可能对结直肠培养物对作为ABCB1底物的药物的敏感性产生深远影响。 ©2018作者。 John Wiley&Sons Ltd代表英国和爱尔兰病理学会出版的《病理学杂志》。

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