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人类实体瘤中的自然杀伤细胞。

Natural killer cells in human solid tumors.

作者信息

Introna M, Mantovani A

出版信息

Cancer Metastasis Rev. 1983;2(4):337-50. doi: 10.1007/BF00048566.

Abstract

Natural killer (NK) cells have been studied in human neoplastic diseases in an effort to assess the role of these cells in the control of human neoplasia and to monitor the effects of therapeutic regimens expected to affect this reactivity. NK activity measured against susceptible cell lines is usually somewhat depressed in patients bearing advanced solid tumors, but not at early disease stages. Lymphoid cells associated with solid tumor tissues or effusions have usually low NK cytotoxicity, with considerable differences among histologic types (e.g., nasopharyngeal carcinoma versus other tumors) or at different sites involved by the same tumor (e.g., peritoneal effusions versus solid lesions in ovarian carcinoma). The low levels of NK activity of tumor-associated lymphoid cells are primarily related to a low frequency in the relevant effector cells at the tumor site, although suppression of the in vitro maintenance of cytotoxicity by in situ macrophages and lymphocytes has been described in a few patients. Treatment with immunopharmacologic agents, interferons in particular, has been reported to augment NK activity in cancer patients, but it is unclear how blood NK activity relates to tissue levels of this reactivity. Limited evidence indicates that blood NK levels need not be representative of the activity of tumor associated lymphoid cells. Most studies on NK cells in human neoplasia have dealt with reactivity against susceptible tissue culture lines, but freshly isolated human tumors are generally relatively resistant to these effector cells, particularly when autologous lymphoid cells are used. The resistance of fresh human neoplastic cells to NK activity has not been studied extensively and, together with the poor localization at the tumor site of NK effectors, it represents a major difficulty in envisaging a role for these cells in the control of established human neoplasia.

摘要

自然杀伤(NK)细胞已在人类肿瘤疾病中得到研究,旨在评估这些细胞在控制人类肿瘤形成中的作用,并监测预期会影响这种反应性的治疗方案的效果。针对易感细胞系测量的NK活性在患有晚期实体瘤的患者中通常会有所降低,但在疾病早期阶段则不会。与实体瘤组织或积液相关的淋巴细胞通常具有较低的NK细胞毒性,不同组织学类型(例如鼻咽癌与其他肿瘤)或同一肿瘤累及的不同部位(例如卵巢癌的腹腔积液与实体病变)之间存在相当大的差异。肿瘤相关淋巴细胞的NK活性水平较低主要与肿瘤部位相关效应细胞的频率较低有关,尽管在少数患者中已描述原位巨噬细胞和淋巴细胞对体外细胞毒性维持的抑制作用。据报道,用免疫药理学药物,特别是干扰素治疗可增强癌症患者的NK活性,但尚不清楚血液中的NK活性与这种反应性的组织水平之间的关系。有限的证据表明,血液中的NK水平不一定代表肿瘤相关淋巴细胞的活性。大多数关于人类肿瘤中NK细胞的研究都涉及对易感组织培养系的反应性,但新鲜分离的人类肿瘤通常对这些效应细胞相对耐药,特别是当使用自体淋巴细胞时。新鲜人类肿瘤细胞对NK活性的耐药性尚未得到广泛研究,并且与NK效应细胞在肿瘤部位的定位不佳一起,这代表了设想这些细胞在控制已形成的人类肿瘤中的作用的一个主要困难。

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