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谷氨酰胺拮抗剂阿西维辛诱导新鲜分离的人髓系白血病细胞和HL-60细胞的单核细胞样分化。

Monocytoid differentiation of freshly isolated human myeloid leukemia cells and HL-60 cells induced by the glutamine antagonist acivicin.

作者信息

Nichols K E, Chitneni S R, Moore J O, Weinberg J B

机构信息

VA Medical Center, Division of Hematology/Oncology, Durham, NC.

出版信息

Blood. 1989 Oct;74(5):1728-37.

PMID:2790198
Abstract

Previously we showed that starvation of HL-60 promyelocytic leukemia cells for a single essential amino acid induced irreversible differentiation into more mature monocyte-like cells. Although not an essential amino acid, glutamine is important in the growth of normal and neoplastic cells. The glutamine analogue, alpha S,5S-alpha-amino-3-chloro-4,5-dihydro-5-isoxazoleacetic acid (acivicin) inhibits several glutamine-utilizing enzymes and therefore depletes cells of certain metabolic end products. The current study was designed to examine in vitro the effects of acivicin on growth and differentiation of several established human myeloid leukemia cell lines, including the HL-60 cell line, and of freshly isolated cells from patients with acute nonlymphocytic leukemia (ANLL). Four-day culture of HL-60 cells with acivicin at concentrations of 0.1 to 10.0 micrograms/mL (0.56 to 56 nmol/L) decreased cell growth by 33% to 88% as compared with untreated control cells. Viability of cells was greater than 92% for untreated cells and 93% to 41% for acivicin-treated cells. Cells treated with acivicin differentiated along a monocytic pathway as shown by increased H2O2 production and alpha-naphthyl butyrate esterase (NSE) content. Differentiation was time and dose dependent, and was irreversible. Changes in H2O2 production and NSE content were partially abrogated by co-culture with 10 mmol/L exogenous cytidine and guanosine but not by co-culture with other nucleosides or glutamine. At these concentrations of acivicin, differentiation was associated with expression of the N-formyl-methyl-leucyl-phenylalanine-receptor (FMLP-R) on 8% to 29% of cells as compared with 8% for control cells. Acivicin potentiated the differentiating effects of interferon-gamma, tumor necrosis factor, dihydroxyvitamin D3, dimethylsulfoxide, and retinoic acid. Culture of cells from the U937 (monoblastic), K562 (erythroleukemia), and KG-1 (myeloblastic) cell lines resulted in decreased growth and viability, but not consistently in differentiation. Acivicin decreased survival of freshly isolated ANLL cells and increased their H2O2 production and NSE content. These results suggest that the glutamine analogue acivicin may be useful as a differentiating agent with antileukemia activity in patients with ANLL.

摘要

先前我们发现,使HL-60早幼粒细胞白血病细胞缺乏单一必需氨基酸会诱导其不可逆地分化为更成熟的单核细胞样细胞。谷氨酰胺虽然不是必需氨基酸,但对正常细胞和肿瘤细胞的生长很重要。谷氨酰胺类似物αS,5S-α-氨基-3-氯-4,5-二氢-5-异恶唑乙酸(阿西维辛)可抑制几种利用谷氨酰胺的酶,从而使细胞的某些代谢终产物耗竭。本研究旨在体外检测阿西维辛对几种已建立的人髓系白血病细胞系(包括HL-60细胞系)以及急性非淋巴细胞白血病(ANLL)患者新鲜分离细胞的生长和分化的影响。用浓度为0.1至10.0微克/毫升(0.56至56纳摩尔/升)的阿西维辛对HL-60细胞进行为期四天的培养,与未处理的对照细胞相比,细胞生长减少了33%至88%。未处理细胞的活力大于92%,阿西维辛处理细胞的活力为93%至41%。用阿西维辛处理的细胞沿单核细胞途径分化,表现为过氧化氢(H2O2)生成增加和α-萘丁酸酯酶(NSE)含量增加。分化具有时间和剂量依赖性,且是不可逆的。与10毫摩尔/升外源性胞苷和鸟苷共培养可部分消除H2O2生成和NSE含量的变化,但与其他核苷或谷氨酰胺共培养则不能。在这些阿西维辛浓度下,与对照细胞的8%相比,8%至29%的细胞上表达了N-甲酰基-甲基-亮氨酰-苯丙氨酸受体(FMLP-R)。阿西维辛增强了干扰素-γ、肿瘤坏死因子、二羟基维生素D3、二甲基亚砜和视黄酸的分化作用。对U937(单核细胞样)、K562(红白血病)和KG-1(髓母细胞样)细胞系的细胞进行培养导致生长和活力下降,但分化并不一致。阿西维辛降低了新鲜分离的ANLL细胞的存活率,并增加了它们的H2O2生成和NSE含量。这些结果表明,谷氨酰胺类似物阿西维辛可能作为一种具有抗白血病活性的分化剂用于ANLL患者。

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