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Multiple Genetic Mechanisms Lead to Loss of Functional TbAT1 Expression in Drug-Resistant Trypanosomes

机译:多种遗传机制导致抗药性锥虫中功能性TbAT1表达的丧失

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The P2 aminopurine transporter, encoded by TbAT1 in African trypanosomes in the Trypanosoma brucei group, carries melaminophenyl arsenical and diamidine drugs into these parasites. Loss of this transporter contributes to drug resistance. We identified the genomic location of TbAT1 to be in the subtelomeric region of chromosome 5 and determined the status of the TbAT1 gene in two trypanosome lines selected for resistance to the melaminophenyl arsenical, melarsamine hydrochloride (Cymelarsan), and in a Trypanosoma equiperdum clone selected for resistance to the diamidine, diminazene aceturate. In the Trypanosoma brucei gambiense STIB 386 melarsamine hydrochloride-resistant line, TbAT1 is deleted, while in the Trypanosoma brucei brucei STIB 247 melarsamine hydrochloride-resistant and T. equiperdum diminazene-resistant lines, TbAT1 is present, but expression at the RNA level is no longer detectable. Further characterization of TbAT1 in T. equiperdum revealed that a loss of heterozygosity at the TbAT1 locus accompanied loss of expression and that P2-mediated uptake of [3H]diminazene is lost in drug-resistant T. equiperdum. Adenine-inhibitable adenosine uptake is still detectable in a ΔTbat1 T. b. brucei mutant, although at a greatly reduced capacity compared to that of the wild type, indicating that an additional adenine-inhibitable adenosine permease, distinct from P2, is present in these cells.
机译:在布氏锥虫组的非洲锥虫中,由Tb AT1 编码的P2氨基嘌呤转运蛋白将三聚氰胺苯砷和二am药物携带到这些寄生虫中。该转运蛋白的丧失导致耐药性。我们确定了Tb AT1 的基因组位置位于5号染色体的亚端粒区域,并确定了在两个对三聚氰胺苯基有抗性的锥虫系中Tb AT1 基因的状态砷,盐酸美拉敏(Cymelarsan),以及在锥虫锥虫(Trypanosoma equiperdum)克隆中选择用于抵抗二am,醋酸二咪唑的抗性。在布氏冈比亚锥虫STIB 386耐盐酸美拉敏的品系中,删除了Tb AT1 ,而在布氏锥虫STIB 247盐酸耐美拉敏和T. equiperdum耐二咪唑的品系中,Tb 存在AT1 ,但无法再检测到RNA水平的表达。 T. er> AT1 在马齿T中的进一步表征表明,Tb AT1 位点杂合性的丧失伴随表达的丧失,P2介导的[ 3的摄取 H]二咪唑在抗药性马铃虫中丢失。在ΔTb at1 T中仍可检测到腺嘌呤抑制腺苷摄取。布鲁斯突变体,尽管与野生型相比具有大大降低的能力,这表明在这些细胞中存在另外的不同于P2的腺嘌呤抑制性腺苷通透酶。

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