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贝司他汀在正常及环磷酰胺骨髓抑制小鼠中的造血及血液学特性

Hematopoietic and hematologic properties of bestatin in normal and cyclophosphamide myelosuppressed mice.

作者信息

Talmadge J E, Black P L, Pelus L M, Abe F

机构信息

SmithKline Beecham Pharmaceuticals, King of Prussia, PA 19406-0939.

出版信息

Biomed Pharmacother. 1990;44(2):85-91. doi: 10.1016/0753-3322(90)90109-m.

Abstract

Bestatin is a potent inhibitor of aminopeptidase, an enzyme found in abundance in the membrane of monocytes and macrophages. Following binding of bestatin to cells in the histiocytic lineage, the production of colony stimulating activity is upregulated (both in vitro and in vivo) with subsequent increases in hematopoietic and hematologic parameters. We report that the frequency and absolute numbers of CFU-GM as well as entry of CFU-GM into S phase (a measure of progenitor cell activity) is upregulated by treatment of animals with bestatin. This results in an increase in bone marrow cellularity in cyclophosphamide suppressed mice and an increase in the absolute neutrophil count in normal and suppressed mice. The therapeutic application of this hematopoietic modulator has been demonstrated in combination cyclophosphamide and bestatin therapeutic protocols. Because this indication for bestatin has only recently been recognized, few clinical studies have been undertaken utilizing appropriate surrogates of hematopoietic activity. However, preliminary clinical evidence of hematopoietic activity by this non-toxic dipeptide, as reviewed here, suggests that this may be an appropriate strategy for the treatment of myelosuppressed patients.

摘要

贝司他汀是氨肽酶的一种强效抑制剂,氨肽酶是一种在单核细胞和巨噬细胞膜中大量存在的酶。贝司他汀与组织细胞系中的细胞结合后,集落刺激活性的产生上调(在体外和体内均如此),随后造血和血液学参数增加。我们报告称,用贝司他汀治疗动物可上调CFU-GM的频率和绝对数量以及CFU-GM进入S期的情况(祖细胞活性的一种衡量指标)。这导致环磷酰胺抑制的小鼠骨髓细胞密度增加,正常和受抑制小鼠的绝对中性粒细胞计数增加。这种造血调节剂的治疗应用已在环磷酰胺与贝司他汀联合治疗方案中得到证实。由于贝司他汀的这一适应证最近才被认识到,很少有利用适当造血活性替代指标的临床研究。然而,如本文所综述的,这种无毒二肽具有造血活性的初步临床证据表明,这可能是治疗骨髓抑制患者的一种合适策略。

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