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首页> 外文期刊>Cancer prevention research. >Analysis of Immune Cells from Human Mammary Ductal Epithelial Organoids Reveals V delta 2(+) T Cells That Efficiently Target Breast Carcinoma Cells in the Presence of Bisphosphonate
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Analysis of Immune Cells from Human Mammary Ductal Epithelial Organoids Reveals V delta 2(+) T Cells That Efficiently Target Breast Carcinoma Cells in the Presence of Bisphosphonate

机译:人类乳腺导管上皮样器官的免疫细胞分析揭示了在双膦酸盐存在下有效靶向乳腺癌细胞的V delta 2(+)T细胞

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Developing strategies to enhance cancer prevention is a paramount goal, particularly given recent concerns about surgical treatment of preinvasive states such as ductal carcinoma in situ. Promoting effective immunosurveillance by leukocytes that scan for nascent neoplastic transformations represents a potential means to achieve this goal. Because most breast cancers arise within the ductal epithelium, enhancing protective immunosurveillance will likely necessitate targeting one or more of the distinctive lymphocyte types found in these sites under normal conditions. Here, we have characterized the intraepithelial lymphocyte compartment of non-cancerous human breast tissue and identified a subset of T lymphocytes that can be pharmacologically targeted to enhance their responses to breast cancer cells. Specifically, V45.2.' T cells were consistently present in preparations of mammary ductal epithelia] organoids and they proliferated in response to zoledronic acid, an aminobisphosphonate drug. V delta 2(+) T cells from breast ductal organoids produced the antitumor cytokine IFN gamma and efficiently killed bisphosphonate-pulsed breast carcinoma cells. These findings demonstrate the potential for exploiting the ability of Vo(2+) gamma delta T cells to respond to FDA-approved bisphosphonate drugs as a novel immunotherape-utic approach to inhibit the outgrowth of breast cancers. (C) 2016 AACR.
机译:制定增强癌症预防的策略是最重要的目标,尤其是考虑到最近对诸如导管癌等浸润前状态的外科治疗的关注。通过扫描新生肿瘤转化的白细胞促进有效的免疫监视,是实现这一目标的一种潜在手段。因为大多数乳腺癌都发生在导管上皮内,所以在正常情况下,增强保护性免疫监视可能有必要靶向在这些部位发现的一种或多种独特淋巴细胞类型。在这里,我们已经表征了非癌性人乳腺组织的上皮内淋巴细胞区室,并鉴定了可以被药理学靶向增强T细胞对乳腺癌细胞反应的T淋巴细胞的一个子集。具体来说,是V45.2。 T细胞始终存在于乳腺导管上皮类器官的制备物中,并且它们是响应氨基双膦酸盐药物唑来膦酸而增殖的。来自乳腺导管类器官的V delta 2(+)T细胞产生抗肿瘤细胞因子IFNγ,并有效杀死双膦酸酯脉冲的乳腺癌细胞。这些发现证明了利用Vo(2+)γ-δT细胞对FDA批准的双膦酸酯类药物作出反应的潜力,将其作为抑制乳腺癌生长的新型免疫疗法方法。 (C)2016 AACR。

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