Fuchs R L, Kane J F
J Bacteriol. 1985 Apr;162(1):98-101. doi: 10.1128/jb.162.1.98-101.1985.
Histidine ammonia-lyase catalyzes the first step in histidine catabolism, the deamination of histidine to urocanate and ammonia. In vitro experiments have shown that histidine ammonia-lyase also can catalyze the reverse (amination) reaction, histidine synthesis, relatively efficiently under extreme reaction conditions (4 M NH4OH, pH 10). An Escherichia coli hisB deletion strain was transformed with a pBR322 derivative plasmid (pCB101) containing the entire Klebsiella aerogenes histidine utilization (hut) operon to determine whether the catabolic histidine ammonia-lyase could function biosynthetically in vivo to satisfy the histidine auxotrophy. Although the initial construct did not grow on media containing urocanate and ammonia as a source of histidine, spontaneous mutants possessing this ability were isolated. Four mutants characterized grew at doubling times of 4 h compared with 1 h when histidine was present, suggesting that histidine synthesis, although unequivocally present, remained growth limiting. Each mutant contained a plasmid-encoded mutation which eliminated urocanase activity, the second enzyme in the Hut catabolic pathway. This genetic block led to the accumulation of high intracellular levels of urocanate, which was subsequently converted to histidine via histidine ammonia-lyase, thus satisfying the histidine auxotrophic requirement.
组氨酸解氨酶催化组氨酸分解代谢的第一步,即组氨酸脱氨生成尿刊酸和氨。体外实验表明,在极端反应条件下(4 M氢氧化铵,pH 10),组氨酸解氨酶也能相对高效地催化逆反应(氨基化反应),即组氨酸合成。用含有产气克雷伯菌组氨酸利用(hut)操纵子的pBR322衍生质粒(pCB101)转化大肠杆菌hisB缺失菌株,以确定分解代谢的组氨酸解氨酶在体内是否能发挥生物合成功能来满足组氨酸营养缺陷。尽管最初构建的菌株不能在以尿刊酸和氨作为组氨酸来源的培养基上生长,但分离出了具有这种能力的自发突变体。对四个突变体的表征显示,它们的倍增时间为4小时,而存在组氨酸时倍增时间为1小时,这表明尽管组氨酸合成明确存在,但仍然是生长限制因素。每个突变体都含有一个质粒编码的突变,该突变消除了尿刊酸酶活性,尿刊酸酶是Hut分解代谢途径中的第二种酶。这种基因阻断导致细胞内尿刊酸水平升高,随后尿刊酸通过组氨酸解氨酶转化为组氨酸,从而满足了组氨酸营养缺陷的需求。