Antarctic yeasts as a source of L-asparaginase: Characterization of a glutaminase-activity free L-asparaginase from psychrotolerant yeast Leucosporidium scottii L115

天冬酰胺酶 谷氨酰胺酶 酵母 酶分析 酶动力学 生物化学 比活度 天冬酰胺 氨基水解酶 变构调节 基质(水族馆) 背景(考古学) 化学 分子质量 生物 分子生物学 淋巴细胞白血病 谷氨酰胺 活动站点 白血病 氨基酸 遗传学 生态学 古生物学
作者
Ignácio Sánchez‐Moguel,Tales A. Costa-Silva,Omar Pillaca‐Pullo,Juan Carlos Flores-Santos,Rominne Karla Barros Freire,Gustavo Carretero,Júlia da Luz Bueno,David I. Camacho-Córdova,João H. P. M. Santos,Lara Durães Sette,Adalberto Pessoa
出处
期刊:Process Biochemistry [Elsevier BV]
卷期号:129: 121-132 被引量:1
标识
DOI:10.1016/j.procbio.2023.03.003
摘要

Microorganisms from extreme environments, such as the Antarctic ecosystems, have a great potential to produce enzymes with novel characteristics. Within this context, L-asparaginase (ASNase) obtained from yeast species has been poorly studied. In this study, yeasts isolated from samples collected at Admiralty Bay (King George Island, Antarctica) were tested to produce ASNase. From an initial screening of 40 strains, belonging to 13 different species, Leucosporidium scottii L115 produced an ASNase activity (LsASNase activity: 6.24 U g-1 of dry cell weight) with the lowest glutaminase activity. The LsASNase was purified 227-fold, with a specific activity of 137.01 U mg-1 at 37 °C, without glutaminase activity. Moreover, the maximum enzyme activity was observed at pH 7.5 and at a temperature of 55 °C. The enzyme is a multimer of 462 kDa, presenting a single band of 53 kDa molecular mass in reduced conditions; after PGNase F treatment, a single band of 45 kDa was observed. The enzymatic kinetic evaluation revealed an allosteric regulation of the enzyme and the kinetic parameters were determined at 37 °C, pH 7.0 as substrate affinity constant, K0.5 = 233 μM, kcat = 54.7 s−1 and Hill coefficient, nH = 1.52, demonstrating positive cooperativity by the enzyme and the substrate. This is the first study to report L. scottii as a source of glutaminase-activity free L-asparaginase, an acute lymphoblastic leukemia drug feature suitable for the treatment of asparagine synthetase negative cancer cells.

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