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使用共刺激阻断和供体淋巴细胞输注而不进行骨髓消融的同种异体新生小鼠骨髓移植减轻小鼠溶酶体贮积病。

Attenuation of murine lysosomal storage disease by allogeneic neonatal bone marrow transplantation using costimulatory blockade and donor lymphocyte infusion without myeloablation.

作者信息

Lessard Mark D, Alley Travis L, Proctor Jennifer L, Levy Beth, Galvin Nancy, Vogler Carole A, Soper Brian W

机构信息

The Jackson Laboratory, Box 95, 600 Main Street, Bar Harbor, ME 04609, USA.

出版信息

Clin Immunol. 2006 May;119(2):166-79. doi: 10.1016/j.clim.2005.12.015. Epub 2006 Feb 17.

Abstract

Treatment of nonmalignant childhood disorders by bone marrow transplantation (BMT) is limited by toxicity from preparatory regimens and immune consequences associated with engraftment of allogeneic donor cells. Using costimulatory blockade (anti-CD40L mAb and CTLA-4Ig) combined with high-dose BMT in nonablated neonates, we obtained engraftment and established tolerance using both partially MHC mismatched (H2g7 into H2b) and fully mismatched BM (H2s into H2b). Recipients were mucopolysaccharidosis type VII (MPS VII) mice with lysosomal storage disease in order to assess therapeutic outcome. Recipients treated with donor lymphocyte infusion (DLI) amplified microchimerism to full donor. Recipients without DLI maintained long-term engraftment, tolerance, and had extended life spans. DLI increased donor cell mediated replacement of beta-glucuronidase (GUSB) activity in all tissues and maintained clearance of lysosomes better than in non-DLI-treated mice. DLI amplification of partially mismatched BM and fully mismatched BM caused late onset chronic GvHD in 56% and 100% of recipients, respectively.

摘要

骨髓移植(BMT)治疗儿童非恶性疾病受到预处理方案毒性以及与异基因供体细胞植入相关的免疫后果的限制。在未进行清髓的新生儿中,我们使用共刺激阻断(抗CD40L单克隆抗体和CTLA-4Ig)联合大剂量BMT,通过部分MHC不匹配(H2g7植入H2b)和完全不匹配的骨髓(H2s植入H2b)均实现了植入并建立了耐受性。受体为患有溶酶体贮积病的VII型黏多糖贮积症(MPS VII)小鼠,以评估治疗效果。接受供体淋巴细胞输注(DLI)的受体将微嵌合体扩增至完全供体型。未接受DLI的受体维持了长期植入、耐受性,并延长了寿命。与未接受DLI治疗的小鼠相比,DLI增加了供体细胞介导的所有组织中β-葡萄糖醛酸酶(GUSB)活性的替代,并更好地维持了溶酶体的清除。部分不匹配骨髓和完全不匹配骨髓的DLI扩增分别在56%和100%的受体中导致迟发性慢性移植物抗宿主病(GvHD)。

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