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引流人类恶性肿瘤的各个淋巴结产生淋巴因子的差异。

Variations in lymphokine generation by individual lymph nodes draining human malignant tumors.

作者信息

Wen D R, Hoon D S, Chang C, Cochran A J

机构信息

Division of Surgical Oncology, Jonsson Comprehensive Cancer Center, Los Angeles, California.

出版信息

Cancer Immunol Immunother. 1989;30(5):277-82. doi: 10.1007/BF01744894.

Abstract

Individual lymph nodes draining tumors vary in their degree of immunological activity. Cell suspensions from tumor-free nodes located relatively near to tumors are spontaneously less reactive and respond poorly to exogenous stimulation by mitogens and lymphokines. Diminished spontaneous uptake of tritiated thymidine by lymph node cells not exposed to exogenous stimulation suggests that tumor-proximate immune suppression exists in vivo and is not purely a laboratory artefact. The present study was undertaken to explore that possibility further. Fluid in which cell suspensions from tumor-free nodes were prepared, and supernatants from short-term cultures of nodes located at different distances from tumors were compared for their capacity to inhibit the in vitro migration of the human lymphoblastoid cell line QIMR-WIL. Inhibitory activity of fluids from individual nodes was related to their position relative to the tumor and their immune competence, assessed by the responses to mitogens of cell suspensions prepared from them. Cell suspension fluids from 92/111 nodes (83%) significantly inhibited the migration of QIMR-WIL, at a level similar (44 +/- 14%) to that induced by the supernatants of mixed lymphocyte cultures (43 +/- 17%). Fluids from the nodes of melanoma patients were more inhibitory than those from breast cancer patients (49 +/- 12% and 37 +/- 13%, respectively, P = 0.003). The inhibitory activity of the different nodes of individual node groups varied significantly in 25 of 33 patients (76%), the node nearest the tumor generating least inhibitory activity (indexing the greatest immune suppression) in 20 of these 25 patients (80%). The strength of migration-inhibitory activity was concordant with the responsiveness to mitogen stimulation in up to 14 of 18 patients (78%). Studies of molecular size and heat stability indicated that the inhibitory factors had characteristics consistent with common migration-inhibitory lymphokines such as leukocyte-migration-inhibitory factor, macrophage-inhibitory factor and interleukin-2. Our findings further support the hypothesis that lymph nodes nearest to tumors are relatively immune-suppressed in vivo.

摘要

引流肿瘤的各个淋巴结在免疫活性程度上存在差异。来自相对靠近肿瘤的无瘤淋巴结的细胞悬液自发反应性较低,对丝裂原和淋巴因子的外源性刺激反应不佳。未暴露于外源性刺激的淋巴结细胞对氚标记胸腺嘧啶核苷的自发摄取减少,这表明肿瘤附近存在体内免疫抑制,并非纯粹是实验室假象。本研究旨在进一步探索这种可能性。比较了制备无瘤淋巴结细胞悬液所用的液体,以及来自距肿瘤不同距离的淋巴结短期培养物的上清液对人淋巴母细胞系QIMR-WIL体外迁移的抑制能力。各个淋巴结液体的抑制活性与其相对于肿瘤的位置及其免疫能力有关,免疫能力通过由其制备的细胞悬液对丝裂原的反应来评估。92/111个淋巴结(83%)的细胞悬液能显著抑制QIMR-WIL的迁移,其抑制水平与混合淋巴细胞培养上清液诱导的水平相似(44±14%对43±17%)。黑色素瘤患者淋巴结的液体比乳腺癌患者淋巴结的液体抑制作用更强(分别为49±12%和37±13%,P = 0.003)。在33例患者中的25例(76%),各个淋巴结组的不同淋巴结的抑制活性差异显著,在这25例患者中的20例(80%),最靠近肿瘤的淋巴结产生的抑制活性最低(表明免疫抑制最强)。在18例患者中的14例(78%),迁移抑制活性的强度与对丝裂原刺激的反应性一致。分子大小和热稳定性研究表明,抑制因子具有与常见的迁移抑制性淋巴因子如白细胞迁移抑制因子、巨噬细胞抑制因子和白细胞介素-2一致的特征。我们的研究结果进一步支持了以下假说:在体内,最靠近肿瘤的淋巴结相对处于免疫抑制状态。

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