Chambers Jeremy W, Kearns Margaret T, Morris Meredith T, Morris James C
Department of Genetics and Biochemistry, Clemson University, 51 New Cherry Street, Clemson, SC 29634, USA.
J Biol Chem. 2008 May 30;283(22):14963-70. doi: 10.1074/jbc.M802124200. Epub 2008 Apr 3.
Glycolysis is essential to Trypanosoma brucei, the protozoan parasite that causes African sleeping sickness in humans and nagana in cattle. Hexokinase (HK), the first enzyme in glycolysis, catalyzes the phosphorylation of glucose to form glucose 6-phosphate. T. brucei harbors two HKs that are 98% identical at the amino acid level, T. brucei hexokinase 1 (TbHK1) and TbHK2. Recombinant TbHK1 (rTbHK1) has HK activity, whereas rTbHK2 does not. Unlike other eukaryotic HKs, TbHK1 is not subject to inhibition by ADP and glucose 6-phosphate. However, TbHK1 is inhibited by myristate, a critical fatty acid in T. brucei biology. We report here that rTbHKs, similar to authentic TbHK, form oligomers. Myristate dissociated these assemblies when incubated with either ATP or glucose. Furthermore, oligomer disruption was reversible by removal of myristate. Mixing of rTbHK1 and rTbHK2 monomers followed by reassembly yielded enzyme with an approximately 3-fold increase in specific activity compared with similarly treated rTbHK1 alone. Surprisingly, reassembly of rTbHK2 with an inactive rTbHK1 variant yielded an active HK, revealing for the first time that rTbHK2 is competent for HK activity. Finally, pyrophosphate inhibits active reassembled rTbHK2 oligomers but not oligomeric rTbHK1, suggesting that the two enzymes have distinct regulatory mechanisms.
糖酵解对于布氏锥虫至关重要,这种原生动物寄生虫会导致人类患非洲昏睡病以及牛患那加那病。己糖激酶(HK)是糖酵解的第一种酶,催化葡萄糖磷酸化形成6-磷酸葡萄糖。布氏锥虫含有两种在氨基酸水平上有98%同一性的己糖激酶,即布氏锥虫己糖激酶1(TbHK1)和TbHK2。重组TbHK1(rTbHK1)具有己糖激酶活性,而rTbHK2没有。与其他真核己糖激酶不同,TbHK1不受ADP和6-磷酸葡萄糖的抑制。然而,TbHK1受到肉豆蔻酸的抑制,肉豆蔻酸是布氏锥虫生物学中的一种关键脂肪酸。我们在此报告,rTbHKs与天然TbHK一样形成寡聚体。当与ATP或葡萄糖一起孵育时,肉豆蔻酸会使这些聚集体解离。此外,通过去除肉豆蔻酸,寡聚体的破坏是可逆的。将rTbHK1和rTbHK2单体混合后再重新组装,与单独对类似处理的rTbHK1相比,产生的酶比活性增加了约3倍。令人惊讶的是,rTbHK2与无活性的rTbHK1变体重新组装产生了一种有活性的己糖激酶,首次揭示rTbHK2具有己糖激酶活性。最后,焦磷酸抑制有活性的重新组装的rTbHK2寡聚体,但不抑制寡聚体rTbHK1,这表明这两种酶具有不同的调节机制。