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通过骨髓移植恢复猫科动物Chediak-Higashi综合征中性粒细胞和血小板的功能。

Restoration of neutrophil and platelet function in feline Chediak-Higashi syndrome by bone marrow transplantation.

作者信息

Colgan S P, Hull-Thrall M A, Gasper P W, Gould D H, Rose B J, Fulton R, Blanquaert A M, Bruyninckx W J

机构信息

Department of Pathology, College of Veterinary Medicine and Biomedical Sciences, Colorado State University, Fort Collins 80523.

出版信息

Bone Marrow Transplant. 1991 May;7(5):365-74.

PMID:2070146
Abstract

Allogeneic bone marrow transplantation (BMT) was successfully performed in four Chediak-Higashi (CHS) syndrome affected cats. Preparatory regimens included selective intestinal flora decontamination, fractionated total body irradiation for myeloablation, and prophylactic treatment for graft-versus-host disease with cyclosporin A. Neutrophil chemotaxis under-agarose and whole-blood platelet aggregation/secretion were characterized prior to BMT and after engraftment of donor-origin marrow cells. Liver and kidney biopsies were obtained and evaluated by light and electron microscopy before, and at 6 months post-BMT to determine what effect BMT might have on abnormal lysosome fusion in hepatocytes and renal tubule cells. The platelet storage pool defect was resolved by day 40 post-BMT. In vitro neutrophil migration in all cats appeared to improve with time after BMT and complete restoration was evident by day 175 post-BMT. No apparent differences were evident in either the liver or the kidney at 6 months post-BMT. One cat developed seizures and one developed posterior paresis 5 months post-BMT; neurologic impairment ultimately resulted in death of two cats at 6 and 8 months post-BMT, respectively. Neurologic lesions in both cats were characterized by non-suppurative encephalitis. Allogeneic BMT successfully corrected the neutrophil migration defect and platelet storage pool deficiency but had no effect on lysosome distribution in liver and kidney cells of CHS cats.

摘要

对四只患有切-希二氏(CHS)综合征的猫成功进行了异基因骨髓移植(BMT)。预处理方案包括选择性肠道菌群去污、分次全身照射以进行骨髓消融,以及用环孢素A对移植物抗宿主病进行预防性治疗。在BMT前以及供体来源骨髓细胞植入后,对琼脂糖下中性粒细胞趋化性和全血血小板聚集/分泌进行了表征。在BMT前和BMT后6个月获取肝脏和肾脏活检组织,并通过光学显微镜和电子显微镜进行评估,以确定BMT可能对肝细胞和肾小管细胞中异常溶酶体融合产生何种影响。BMT后第40天,血小板储存池缺陷得到解决。BMT后,所有猫的体外中性粒细胞迁移似乎随时间有所改善,在BMT后第175天明显完全恢复。BMT后6个月,肝脏和肾脏均未出现明显差异。一只猫在BMT后5个月出现癫痫发作,另一只出现后肢轻瘫;神经功能障碍最终分别导致两只猫在BMT后6个月和8个月死亡。两只猫的神经病变均以非化脓性脑炎为特征。异基因BMT成功纠正了中性粒细胞迁移缺陷和血小板储存池缺乏,但对CHS猫肝脏和肾脏细胞中的溶酶体分布没有影响。

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