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将人滑膜移植到严重联合免疫缺陷小鼠体内。人外周血T细胞向移植的人滑膜和小鼠淋巴结的迁移。

Engraftment of human synovium into severe combined immune deficient mice. Migration of human peripheral blood T cells to engrafted human synovium and to mouse lymph nodes.

作者信息

Rendt K E, Barry T S, Jones D M, Richter C B, McCachren S S, Haynes B F

机构信息

Department of Medicine, Duke University Medical Center, Durham, NC.

出版信息

J Immunol. 1993 Dec 15;151(12):7324-36.

PMID:8258726
Abstract

To determine the feasibility of using the C.B-17 scid/scid (severe combined immune deficient, SCID) mouse as a recipient of human synovial xenografts, we have engrafted human synovium under the renal capsule of SCID mice, and determined synovial graft survival and histologic characteristics 4 to 7 wk after tissue implantation. Both normal and inflammatory synovial tissue grew well in SCID mice and maintained histologic and phenotypic components of the fresh synovial tissue before implantation. However, the number of T cells in synovial grafts decreased after implantation. To determine whether leukocytes could migrate to human synovial xenografts, either allogenic or autologous PBMC were injected in the peritoneum of SCID mice bearing synovial xenografts. We found that 7 days after i.p. injection of autologous or allogeneic PBMC, injected T cells had selectively migrated to human synovial grafts and to SCID mouse lymph nodes. Our data demonstrate that normal and inflammatory human synovial tissues will grow in SCID mice and serve as recipients for autologous and allogenic peripheral blood human T cells injected i.p. into engrafted mice.

摘要

为了确定将C.B-17 scid/scid(严重联合免疫缺陷,SCID)小鼠用作人滑膜异种移植物受体的可行性,我们将人滑膜植入SCID小鼠的肾包膜下,并在组织植入后4至7周确定滑膜移植物的存活情况和组织学特征。正常和炎性滑膜组织在SCID小鼠中生长良好,并保持植入前新鲜滑膜组织的组织学和表型成分。然而,植入后滑膜移植物中的T细胞数量减少。为了确定白细胞是否能迁移至人滑膜异种移植物,将同种异体或自体外周血单个核细胞(PBMC)注射到携带滑膜异种移植物的SCID小鼠腹膜内。我们发现,腹腔注射自体或同种异体PBMC 7天后,注射的T细胞已选择性迁移至人滑膜移植物和SCID小鼠淋巴结。我们的数据表明,正常和炎性人滑膜组织将在SCID小鼠中生长,并作为腹腔注射到植入小鼠体内的自体和同种异体人外周血T细胞的受体。

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