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良性淋巴组织增生和B细胞非霍奇金淋巴瘤中的活化T细胞亚群。

Activated T-cell subsets in benign lymphoid hyperplasias and B-cell non-Hodgkin's lymphomas.

作者信息

Diaz J I, Edinger M G, Stoler M H, Tubbs R R

机构信息

Department of Pathology, Cleveland Clinic Foundation, Ohio 44195-5138.

出版信息

Am J Pathol. 1991 Sep;139(3):503-9.

Abstract

Activated tumor-infiltrating T lymphocytes (TIL-T) were quantitated prospectively in excisional biopsy specimens of 49 B-cell non-Hodgkin's lymphomas (NHL) of various grades and compared with eight benign lymphoid hyperplasias (BLH) to identify any potential difference in host T-cell response. Immunotyping of tissue-cell suspensions was done by three-color flow cytometry, which was complemented by immunocytology by using cytocentrifuged preparations. Two activated T-cell subsets were studied: acutely activated TIL-T (CD3+ CD25+ HLADr-) and chronically activated TIL-T (CD3+ CD25- HLADr+). Results showed an association of the more aggressive intermediate/high-grade B-cell NHL with a higher percentage of late-phase activated TIL-T and a progressive increase with the grade of malignancy: 10.29%, 23.25%, 33.87%, and 47.78% (means) for BLH and for low-, intermediate- and high-grade B-cell NHL, respectively. Differences for this subset were significant (P less than 0.050) for the following comparisons: hyperplasia versus intermediate-grade NHL (P less than 0.0012), hyperplasia versus high-grade NHL (P less than 0.0002), and low versus high-grade NHL (P less than 0.0080). The percentage of acutely activated TIL-T cells did not show a statistically significant difference between the groups. The results suggest a host T-cell response to proliferating neoplastic cells in B-cell NHL. Paradoxically, the response does not appear to be protective for the host since the intensity is directly proportional to the grade of malignancy. However, the recognition of this response may have clinical applications since its amplification with biological response modifiers may result in effective adoptive immunotherapy of B-cell NHL. Further clarification of the specificity and biologic significance of host T-cell activation in B-cell NHL will require functional studies of isolated lymphocytic subpopulations from neoplastic tissue.

摘要

对49例不同分级的B细胞非霍奇金淋巴瘤(NHL)切除活检标本中的活化肿瘤浸润性T淋巴细胞(TIL-T)进行前瞻性定量,并与8例良性淋巴组织增生(BLH)进行比较,以确定宿主T细胞反应的任何潜在差异。通过三色流式细胞术对组织细胞悬液进行免疫分型,并通过使用细胞离心涂片制剂的免疫细胞学进行补充。研究了两个活化的T细胞亚群:急性活化的TIL-T(CD3 + CD25 + HLA-Dr-)和慢性活化的TIL-T(CD3 + CD25- HLA-Dr +)。结果显示,侵袭性更强的中/高级别B细胞NHL与晚期活化TIL-T的更高百分比相关,并且随着恶性程度的增加而逐渐升高:BLH以及低、中、高级别B细胞NHL的均值分别为10.29%、23.25%、33.87%和47.78%。该亚群在以下比较中差异具有统计学意义(P小于0.050):增生与中级NHL(P小于0.0012)、增生与高级NHL(P小于0.0002)以及低级别与高级别NHL(P小于0.0080)。急性活化的TIL-T细胞百分比在各组之间未显示出统计学上的显著差异。结果提示宿主对B细胞NHL中增殖的肿瘤细胞有T细胞反应。矛盾的是,这种反应似乎对宿主没有保护作用,因为其强度与恶性程度成正比。然而,认识到这种反应可能具有临床应用价值,因为用生物反应调节剂增强这种反应可能导致B细胞NHL的有效过继免疫治疗。进一步阐明B细胞NHL中宿主T细胞活化的特异性和生物学意义将需要对肿瘤组织中分离的淋巴细胞亚群进行功能研究。

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