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大鼠模型中的癌症相关性贫血:吉田肉瘤的α2-巨球蛋白缩短红细胞存活期。

Cancer-related anemia in a rat model: alpha2-macroglobulin from Yoshida sarcoma shortens erythrocyte survival.

作者信息

Bhanushali Aparna A, Raghunathan R, Kalraiya Rajiv D, Mehta Narendra G

机构信息

Biochemistry and Molecular Biology Division, Cancer Research Institute, Tata Memorial Centre, Parel, Mumbai 400 012, India.

出版信息

Eur J Haematol. 2002 Jan;68(1):42-8. doi: 10.1034/j.1600-0609.2002.00543.x.

Abstract

Implantation of Yoshida ascites sarcoma in rats was found to lead to a reduction in the hemoglobin content, the erythrocyte count and the packed cell volume of blood to 30% of normal in 4 d; however, there was no decrease in the mean cell hemoglobin, the mean cell volume and the mean corpuscular hemoglobin concentration, or suppression of erythropoiesis. The red cells from the circulation of tumor-bearing animals, tagged with (51)Cr and injected intravenously in normal rats, showed significantly faster clearance than normal. The erythrocytes contaminating the tumor ascites exhibited extremely short survival, suggesting that one or more secreted tumor product(s) may be responsible for the effect. Incubation of red cells from normal rats in the cell-free ascites fluid, or with an isoform of alpha2-macroglobulin purified from it, also led to reduction in the survival; but the ascites fluid depleted specifically of alpha2-macroglobulin was without any effect. The erythrocytes exhibiting reduced survival showed a proportionate decrease in their cellular deformability. The study identifies a tumor product that is directly responsible for the causation of anemia in the host, and the mechanism by which it does so.

摘要

研究发现,给大鼠植入吉田腹水肉瘤会导致血红蛋白含量、红细胞计数和血细胞比容在4天内降至正常水平的30%;然而,平均红细胞血红蛋白、平均红细胞体积和平均红细胞血红蛋白浓度并未降低,也没有出现红细胞生成抑制。用(51)铬标记荷瘤动物循环中的红细胞并静脉注射到正常大鼠体内,其清除速度明显快于正常红细胞。污染肿瘤腹水的红细胞存活时间极短,这表明一种或多种肿瘤分泌产物可能是造成这种影响的原因。将正常大鼠的红细胞在无细胞腹水中孵育,或与从中纯化的α2-巨球蛋白同工型一起孵育,也会导致红细胞存活时间缩短;但特异性去除α2-巨球蛋白的腹水则没有任何作用。存活时间缩短的红细胞其细胞变形能力也相应降低。该研究确定了一种直接导致宿主贫血的肿瘤产物及其作用机制。

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