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新鲜人骨髓瘤细胞在SCID小鼠中的长期植入。

Long-term engraftment of fresh human myeloma cells in SCID mice.

作者信息

Feo-Zuppardi F J, Taylor C W, Iwato K, Lopez M H, Grogan T M, Odeleye A, Hersh E M, Salmon S E

机构信息

Department of Internal Medicine, Arizona Cancer Center, College of Medicine, University of Arizona, Tucson 85724.

出版信息

Blood. 1992 Dec 1;80(11):2843-50.

PMID:1450409
Abstract

Using highly purified myeloma cells from patient bone marrow, we established human-murine myeloma chimeras in severe combined immunodeficiency (SCID) mice and documented secretion of monoclonal human immunoglobulins (Hulgs) in the mice for up to 299 days. Monoclonality of circulating Hulgs was found only when highly purified myeloma cells were injected intraperitoneally. In contrast, injection of unfractionated myeloma marrow led to the development of polyclonal Hulgs in the SCID mice. The criteria for myeloma engraftment included prolonged presence of monoclonal Hulgs in the sera of SCID mice and/or detection of human myeloma cells in their tissues by immunohistochemical examination. Ninety-one percent (10/11) of the fresh purified myeloma specimens engrafted in the SCID mice. Fifty-five percent (6/11) of the patient samples resulted in human B-cell grafts, and 45% (5/11) were identifiable as human myeloma chimeras. Pathologic studies showed that most human plasmacytes were located in the peritoneal cavity but metastatic infiltrates were also found in other organs in 69% of the SCID-human myeloma chimeras. This chimeric model should provide a useful tool for characterization of growth modulation and microenvironmental interactions as well as a means of testing new therapeutic approaches to multiple myeloma.

摘要

我们使用从患者骨髓中高度纯化的骨髓瘤细胞,在严重联合免疫缺陷(SCID)小鼠中建立了人鼠骨髓瘤嵌合体,并记录了小鼠体内单克隆人免疫球蛋白(Hulgs)的分泌长达299天。仅当腹腔注射高度纯化的骨髓瘤细胞时,才发现循环中的Hulgs具有单克隆性。相比之下,注射未分级的骨髓瘤骨髓会导致SCID小鼠体内产生多克隆Hulgs。骨髓瘤植入的标准包括SCID小鼠血清中持续存在单克隆Hulgs和/或通过免疫组织化学检查在其组织中检测到人骨髓瘤细胞。11份新鲜纯化的骨髓瘤标本中有91%(10/11)在SCID小鼠中植入成功。患者样本中有55%(6/11)形成了人B细胞移植,45%(5/11)可鉴定为人骨髓瘤嵌合体。病理研究表明,大多数人浆细胞位于腹腔,但在69%的SCID-人骨髓瘤嵌合体的其他器官中也发现了转移性浸润。这种嵌合模型应该为表征生长调节和微环境相互作用提供一个有用的工具,也是测试多发性骨髓瘤新治疗方法的一种手段。

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