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黏膜淋巴组织中低水平外周淋巴结相关血管地址素的表达:与传代AKR淋巴瘤播散的可能关联

Expression of low levels of peripheral lymph node-associated vascular addressin in mucosal lymphoid tissues: possible relevance to the dissemination of passaged AKR lymphomas.

作者信息

Bargatze R F, Streeter P R, Butcher E C

机构信息

Department of Pathology, Stanford University School of Medicine, California 94305.

出版信息

J Cell Biochem. 1990 Apr;42(4):219-27. doi: 10.1002/jcb.240420405.

Abstract

Lymphoid tumors display a wide variety of growth patterns in vivo, from that of a solitary extralymphoid tumor, to a general involvement of all lymphoid organs. Normal lymphocytes are uniquely mobile cells continuously recirculating between blood and lymph throughout much of their life cycle. Therefore, it is reasonable to propose that disseminating malignant lymphocytes may express recirculation characteristics or homing properties consistent with that of their normal lymphoid counterparts. Trafficking of lymphocytes involves the expression and recognition of both lymphocyte homing receptors and their opposing receptors on endothelium, the vascular addressins. These cell surface elements direct the tissue-selective localization of lymphocyte subsets in vivo into organized lymphoid organs and sites of chronic inflammation where specific binding events occur between lymphocytes and the endothelium of specialized high endothelial venules (HEV). In a recent murine study of 13 lymphoma lines, we found that lymphomas that bind well to high endothelial venules, in the Stamper-Woodruff in vitro assay (an assay of lymphocyte binding to venules in frozen sections of peripheral lymph nodes or Peyer's patches), spread hematogenously to all high endothelial venule bearing lymphoid organs, whereas non-binding lymphomas did not. In some cases lymphomas that bound with a high degree of selectivity to peripheral lymph node (PLN) high endothelial venules exhibited only limited organ preference of metastasis, involving the mucosal lymphoid organs Peyer's patches (PP) in addition to the peripheral lymph nodes of adoptive recipients. Here we demonstrate that Peyer's patch high endothelial venules express a low but functional level of peripheral lymph node addressin (MECA-79) that can be recognized by lymphomas expressing the peripheral lymph node homing receptor (MEL-14 antigen).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

淋巴瘤在体内呈现出多种生长模式,从孤立的淋巴外肿瘤到所有淋巴器官的广泛受累。正常淋巴细胞是独特的可移动细胞,在其生命周期的大部分时间里在血液和淋巴之间持续循环。因此,有理由提出,播散性恶性淋巴细胞可能表达与其正常淋巴对应物一致的再循环特征或归巢特性。淋巴细胞的迁移涉及淋巴细胞归巢受体及其在内皮细胞上的对应受体(血管地址素)的表达和识别。这些细胞表面分子在体内将淋巴细胞亚群组织选择性定位到有组织的淋巴器官和慢性炎症部位,在这些部位淋巴细胞与特殊的高内皮微静脉(HEV)内皮之间发生特异性结合事件。在最近一项对13个淋巴瘤系的小鼠研究中,我们发现,在斯坦珀-伍德拉夫体外试验(一种检测淋巴细胞与外周淋巴结或派尔集合淋巴结冰冻切片中小静脉结合的试验)中与高内皮微静脉结合良好的淋巴瘤,会通过血液扩散到所有带有高内皮微静脉的淋巴器官,而非结合性淋巴瘤则不会。在某些情况下,与外周淋巴结(PLN)高内皮微静脉高度选择性结合的淋巴瘤仅表现出有限的转移器官偏好,除了受体的外周淋巴结外,还累及黏膜淋巴器官派尔集合淋巴结(PP)。在此我们证明,派尔集合淋巴结高内皮微静脉表达低水平但有功能的外周淋巴结地址素(MECA-79),可被表达外周淋巴结归巢受体(MEL-14抗原)的淋巴瘤识别。(摘要截短于250词)

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