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7,12-二甲基苯并(a)蒽诱导的骨髓毒性在选择用于高或低急性炎症反应的小鼠中有所不同:与芳烃受体多态性的关系。

7,12-Dimethylbenz(a)anthracene-induced myelotoxicity differs in mice selected for high or low acute inflammatory response: relationship with aryl hydrocarbon receptor polymorphism.

作者信息

Katz Iana Suly Santos, Albuquerque Layra Lucy, Suppa Alessandra Paes, de Siqueira Débora Mathias, Rossato Cristiano, da Silva Graziela Batista, Jensen José Ricardo, Starobinas Nancy, Cabrera Wafa Hanna Koury, De Franco Marcelo, Borelli Primavera, Ibañez Olga Martinez, Ribeiro Orlando Garcia

机构信息

Laboratório de Imunogenética, Instituto Butantan, Av Dr Vital Brazil, 1500, CEP 05503-900, São Paulo, SP, Brazil. Email:

出版信息

Int J Toxicol. 2014 Mar-Apr;33(2):130-42. doi: 10.1177/1091581814522837. Epub 2014 Feb 20.

Abstract

Polycyclic aromatic hydrocarbons, such as 7,12-dimethylbenz(a)anthracene (DMBA), are environmental pollutants that exert multiple toxic and carcinogenic effects. Studies showed that these effects are mediated by activation of the aryl hydrocarbon receptor (AhR) and modulated by allelic variants of Ahr gene. Here, we investigated the effects of DMBA treatment in the inflammatory response and bone marrow (BM) hematopoietic function of maximal acute inflammatory response (AIRmax) and minimal acute inflammatory response (AIRmin) heterogeneous mouse lines selected for high and low acute inflammatory responsiveness, respectively. The phenotypic selection resulted in the segregation of the Ahr(d) and Ahr(b1) alleles that confer low and high receptor ligand-binding affinity, respectively, in AIRmax and AIRmin mice. We observed a reduction in BM mature granulocyte population in AIRmin mice 24 hours after DMBA treatment while both blast and immature myeloid cells were increased. Proliferation and differentiation of BM myeloid cells in response to in vitro granulocyte-macrophage colony-stimulating factor stimulus were impaired in AIRmin-treated mice. These DMBA effects on myeloid BM cells (BMCs) affected the in vivo leukocyte migration to an inflammatory site induced by polyacrylamide beads (Biogel P-100, Bio-Rad, France) injection in AIRmin mice. On the other hand, these alterations were not observed in DMBA-treated AIRmax mice. These data indicate that DMBA affects myeloid cell differentiation and inflammatory response and Ahr(b1) allele in the genetic background of AIRmin mice contributes to this effect.

摘要

多环芳烃,如7,12 - 二甲基苯并(a)蒽(DMBA),是具有多种毒性和致癌作用的环境污染物。研究表明,这些作用是由芳烃受体(AhR)的激活介导的,并受Ahr基因的等位基因变异调节。在此,我们研究了DMBA处理对分别为高急性炎症反应性和低急性炎症反应性而选择的最大急性炎症反应(AIRmax)和最小急性炎症反应(AIRmin)异种小鼠品系的炎症反应和骨髓(BM)造血功能的影响。表型选择导致在AIRmax和AIRmin小鼠中分别分离出具有低和高受体配体结合亲和力的Ahr(d)和Ahr(b1)等位基因。我们观察到,DMBA处理24小时后,AIRmin小鼠的骨髓成熟粒细胞数量减少,而原始细胞和未成熟髓细胞均增加。在体外粒细胞 - 巨噬细胞集落刺激因子刺激下,AIRmin处理小鼠的骨髓髓细胞增殖和分化受损。DMBA对骨髓髓细胞(BMCs)的这些作用影响了AIRmin小鼠体内白细胞向由聚丙烯酰胺珠(Biogel P - 100,Bio - Rad,法国)注射诱导的炎症部位的迁移。另一方面,在DMBA处理的AIRmax小鼠中未观察到这些改变。这些数据表明,DMBA影响髓细胞分化和炎症反应,并且AIRmin小鼠遗传背景中的Ahr(b1)等位基因促成了这种作用。

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