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Role of Cytosolic Glyceraldehyde-3-Phosphate Dehydrogenase in Visceral Organ Infection by Leishmania donovani

机译:胞溶甘油醛-3-磷酸脱氢酶在利什曼原虫感染内脏器官感染中的作用

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The initial 7 steps of the glycolytic pathway from glucose to 3-phosphoglycerate are localized in the glycosomes in Leishmania, including step 6, catalyzed by the enzyme glyceraldehyde-3-phosphate dehydrogenase (GAPDH). In L. donovani and L. mexicana, there exists a second GAPDH enzyme present in the cytosol that is absent in L. braziliensis and that has become a pseudogene in L. major. To investigate the role of the cytosolic GAPDH (cGAPDH), an L. donovani cGAPDH-null mutant was generated, and conversely, the functional L. donovani cGAPDH was introduced into L. major and the resulting engineered parasites were characterized. The L. donovani cGAPDH-null mutant was able to proliferate at the same rate as the wild-type parasite in glucose-deficient medium. However, in the presence of glucose, the L. donovani cGAPDH-null mutant consumed less glucose and proliferated more slowly than the wild-type parasite and displayed reduced infectivity in visceral organs of experimentally infected mice. This demonstrates that cGAPDH is functional in L. donovani and is required for survival in visceral organs. Restoration of cGAPDH activity in L. major, in contrast, had an adverse effect on L. major proliferation in glucose-containing medium, providing a possible explanation of why it has evolved into a pseudogene in L. major. This study indicates that there is a difference in glucose metabolism between L. donovani and L. major, and this may represent an important factor in the ability of L. donovani to cause visceral disease.
机译:从葡萄糖到3-磷酸甘油酸酯的糖酵解途径的最初7个步骤位于利什曼原虫的糖体中,包括步骤6(由3-磷酸甘油醛脱氢酶(GAPDH)催化)。在杜氏乳酸杆菌和墨西哥乳杆菌中,存在于巴西溶胶中不存在的胞浆中存在第二种GAPDH酶,该酶已成为大乳酸杆菌的假基因。为了研究胞质GAPDH(cGAPDH)的作用,生成了多诺氏乳杆菌cGAPDH-null突变体,然后将功能性多诺氏乳杆菌cGAPDH引入到大乳酸杆菌中,并对得到的工程寄生虫进行了表征。在葡萄糖缺乏的培养基中,多诺氏乳杆菌cGAPDH-null突变体能够以与野生型寄生虫相同的速率增殖。但是,在存在葡萄糖的情况下,与野生型寄生虫相比,多诺氏乳杆菌cGAPDH-null突变体消耗的葡萄糖更少,并且增殖速度更慢,并且在实验感染小鼠的内脏器官中显示出降低的传染性。这证明cGAPDH在多诺氏乳杆菌中起作用,并且是内脏器官生存所必需的。相反,恢复大麦芽孢杆菌中的cGAPDH活性对含葡萄糖培养基中的大麦芽孢杆菌增殖具有不利影响,这可能解释了为什么它已在大麦芽孢杆菌中发展成假基因。这项研究表明,多诺氏乳酸杆菌和大麦芽孢杆菌之间的葡萄糖代谢存在差异,这可能代表了多诺氏乳酸杆菌引起内脏疾病的能力的重要因素。

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