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单次或多次来源的同种异体细胞毒性T淋巴细胞的颅内给药:原发性脑肿瘤的长期治疗

Intracranial administrations of single or multiple source allogeneic cytotoxic T lymphocytes: chronic therapy for primary brain tumors.

作者信息

Kruse C A, Schiltz P M, Bellgrau D, Kong Q, Kleinschmidt-DeMasters B K

机构信息

University of Colorado Health Sciences Center, Department of Surgery, Denver.

出版信息

J Neurooncol. 1994;19(2):161-8. doi: 10.1007/BF01306458.

Abstract

Previous investigations by our group demonstrated the efficacy of single source allogeneic cytotoxic T lymphocytes (CTLs) given multiple times in reducing or curing tumor burden in the rat 9L gliosarcoma model. In this study, the lack of toxicity to normal brain when single source allogeneic CTLs were intracranially administered multiple times is documented. Additionally, the efficacy and lack of toxicity of allogeneic CTLs from multiple sources, each given once is documented. CTLs sensitized to Fischer antigen were prepared from major histocompatibility complex incompatible DA, PVG, Sprague-Dawley and Wistar-Furth rat lymphocytes. CTLs from multiple donors were administered one time each to Fischer rats bearing established 9L tumor at staggered intervals over a two week period and survival was monitored in relation to a sham treated group. Additional groups of nontumor-bearing rats received either multiple source allogeneic CTLs or single source DA anti Fischer CTLs in the same treatment regimen. Histological evaluation of the nontumor-bearing brains receiving either single or multiple source allogeneic CTL infusions showed minimal localized brain damage confined to the cannulation tract. No neuronal loss or inflammatory reaction was seen either adjacent to or remote from the administration site. Brains from the long-term survivors of the tumor-bearing animals showed no residual neoplasm; the instillation site had focal sterile abscesses; gliosis and neuronal loss did not extend into adjacent brain. The safety and potential of chronic, local allogeneic CTL administration, derived from multiple donors, as adjuvant local therapy for brain tumors was demonstrated.

摘要

我们小组之前的研究表明,多次给予单一来源的同种异体细胞毒性T淋巴细胞(CTL)可减轻或治愈大鼠9L胶质肉瘤模型中的肿瘤负担。在本研究中,记录了多次颅内给予单一来源的同种异体CTL时对正常脑组织无毒性。此外,还记录了来自多个来源的同种异体CTL(每种给予一次)的疗效和无毒性情况。用主要组织相容性复合体不相容的DA、PVG、Sprague-Dawley和Wistar-Furth大鼠淋巴细胞制备对Fischer抗原致敏的CTL。在两周内,以交错的时间间隔,将来自多个供体的CTL分别一次性给予患有9L肿瘤的Fischer大鼠,并与假治疗组比较监测其存活率。另外几组无肿瘤大鼠在相同治疗方案下接受多来源同种异体CTL或单来源DA抗Fischer CTL。对接受单来源或多来源同种异体CTL输注的无肿瘤大鼠脑进行组织学评估,结果显示局部脑损伤最小,局限于插管路径。在给药部位附近或远处均未观察到神经元丢失或炎症反应。荷瘤动物长期存活者的大脑未显示残留肿瘤;滴注部位有局灶性无菌脓肿;胶质增生和神经元丢失未扩展至邻近脑区。本研究证明了来自多个供体的慢性局部同种异体CTL给药作为脑肿瘤辅助局部治疗的安全性和潜力。

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