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淋巴细胞功能抗原可稳定里德-施特恩贝格细胞与T细胞之间的凝集,但并非霍奇金里德-施特恩贝格细胞同型结合的原因。

Lymphocyte functional antigens stabilize agglutination between Reed-Sternberg cells and T cells, but are not responsible for homotypic binding of Hodgkin's Reed-Sternberg cells.

作者信息

Hsu S M, Hsu P L

机构信息

Department of Pathology, University of Arkansas for Medical Sciences, Little Rock.

出版信息

Am J Pathol. 1990 Sep;137(3):563-74.

Abstract

The neoplastic (Hodgkin's Reed-Sternberg [H-RS]) cells in Hodgkin's disease (HD) are known for their unique capacity to form rosettes with unprimed T cells. Recently, a family of leukocyte-adherence molecules (LFA-1 and LFA-2) has been identified on T lymphocytes. The molecules bind to intercellular-adhesion molecules (ICAMs) and to LFA-3, respectively, which are associated with antigen-presenting cells. In this study, the authors examined whether these molecules are responsible for the homotypic and heterotypic agglutination that occurs in the cultured H-RS cells HDLM-1, HDLM-1d, and KM-H2. Despite their similar expressions of LFA-3 and ICAM-1, the different H-RS cells tested showed different growth patterns in culture. HDLM-1 cells grew singly, whereas HDLM-1d and KM-H2 cells grew in clumps. The HDLM-1 cells formed clumps when mixed with peripheral-blood T lymphocytes, cells of two lymphoblastic T-cell lines (MOLT-3 and MOLT-4), and cells of two monocyte lines (ML-1 and U-937). The addition of anti-LFA and ICAM-1 antibodies to cultures did not result in disassembly of the homotypic clusters of HDLM-1d or KM-H2 cells and it did not cause any significant changes in the size of heterotypic clusters or in the timing of cluster formation of HDLM-1 cells with other types of cells. In all studies, the cell clusters formed during homotypic and heterotypic aggregation were disassembled only minimally by cell shearing with pipetting. The disaggregation by pipetting was slightly more prominent in the presence of antibodies than was that of control cultures. However, in no case did the use of monoclonal antibodies (MAbs) and cell shearing cause complete disaggregation of homotypic and heterotypic clusters. The result seems to suggest that binding between H-RS cells and T cells and between H-RS cells and monocytes is not mediated primarily by LFAs and ICAMs, but that the binding may be strengthened in the presence of these molecules.

摘要

霍奇金淋巴瘤(HD)中的肿瘤性(霍奇金-里德-施特恩伯格[H-RS])细胞以其与未致敏T细胞形成玫瑰花结的独特能力而闻名。最近,在T淋巴细胞上鉴定出了一类白细胞黏附分子(淋巴细胞功能相关抗原1[LFA-1]和淋巴细胞功能相关抗原2[LFA-2])。这些分子分别与细胞间黏附分子(ICAMs)和LFA-3结合,而ICAMs和LFA-3与抗原呈递细胞相关。在本研究中,作者研究了这些分子是否是HDLM-1、HDLM-1d和KM-H2这三种培养的H-RS细胞中发生的同型和异型凝集的原因。尽管它们的LFA-3和ICAM-1表达相似,但所测试的不同H-RS细胞在培养中表现出不同的生长模式。HDLM-1细胞单独生长,而HDLM-1d和KM-H2细胞则聚集成团生长。当HDLM-1细胞与外周血T淋巴细胞、两种淋巴母细胞T细胞系(MOLT-3和MOLT-4)的细胞以及两种单核细胞系(ML-1和U-937)的细胞混合时,会形成团块。向培养物中添加抗LFA和ICAM-1抗体并不会导致HDLM-1d或KM-H2细胞的同型簇解体,也不会使HDLM-1细胞与其他类型细胞形成的异型簇的大小或簇形成时间发生任何显著变化。在所有研究中,同型和异型聚集过程中形成的细胞簇通过移液管吹打进行细胞剪切时,仅轻微解体。在有抗体存在的情况下,通过移液管吹打进行的解聚比对照培养物中略为明显。然而,在任何情况下,使用单克隆抗体(MAbs)和细胞剪切都不会导致同型和异型簇完全解体。结果似乎表明,H-RS细胞与T细胞以及H-RS细胞与单核细胞之间的结合并非主要由LFA和ICAM介导,但在这些分子存在的情况下,结合可能会增强。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/203c/1877525/63072f65c634/amjpathol00105-0085-a.jpg

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