对小鼠 Pycr1 和 Pycr2 的基因分析。
Genetic analysis of Pycr1 and Pycr2 in mice.
机构信息
The Jackson Laboratory, Bar Harbor, ME 04609, USA.
Department of Pharmacology, Dalhousie University, Halifax, NS B3H 4R2, Canada.
出版信息
Genetics. 2021 May 17;218(1). doi: 10.1093/genetics/iyab048.
The final step in proline biosynthesis is catalyzed by three pyrroline-5-carboxylate reductases, PYCR1, PYCR2, and PYCR3, which convert pyrroline-5-carboxylate (P5C) to proline. Mutations in human PYCR1 and ALDH18A1 (P5C Synthetase) cause Cutis Laxa (CL), whereas mutations in PYCR2 cause hypomyelinating leukodystrophy 10 (HLD10). Here, we investigated the genetics of Pycr1 and Pycr2 in mice. A null allele of Pycr1 did not show integument or CL-related phenotypes. We also studied a novel chemically-induced mutation in Pycr2. Mice with recessive loss-of-function mutations in Pycr2 showed phenotypes consistent with neurological and neuromuscular disorders, including weight loss, kyphosis, and hind-limb clasping. The peripheral nervous system was largely unaffected, with only mild axonal atrophy in peripheral nerves. A severe loss of subcutaneous fat in Pycr2 mutant mice is reminiscent of a CL-like phenotype, but primary features such as elastin abnormalities were not observed. Aged Pycr2 mutant mice had reduced white blood cell counts and altered lipid metabolism, suggesting a generalized metabolic disorder. PYCR1 and -2 have similar enzymatic and cellular activities, and consistent with previous studies, both were localized in the mitochondria in fibroblasts. Both PYCR1 and -2 were able to complement the loss of Pro3, the yeast enzyme that converts P5C to proline, confirming their activity as P5C reductases. In mice, Pycr1; Pycr2 double mutants were sub-viable and unhealthy compared to either single mutant, indicating the genes are largely functionally redundant. Proline levels were not reduced, and precursors were not increased in serum from Pycr2 mutant mice or in lysates from skin fibroblast cultures, but placing Pycr2 mutant mice on a proline-free diet worsened the phenotype. Thus, Pycr1 and -2 have redundant functions in proline biosynthesis, and their loss makes proline a semi-essential amino acid. These findings have implications for understanding the genetics of CL and HLD10, and for modeling these disorders in mice.
脯氨酸生物合成的最后一步是由三个吡咯啉-5-羧酸还原酶(PYCR1、PYCR2 和 PYCR3)催化的,它们将吡咯啉-5-羧酸(P5C)转化为脯氨酸。人类 PYCR1 和 ALDH18A1(P5C 合酶)的突变导致松弛皮肤症(CL),而 PYCR2 的突变导致脱髓鞘性白质脑病 10 型(HLD10)。在这里,我们研究了小鼠中 Pycr1 和 Pycr2 的遗传学。Pycr1 的 null 等位基因没有表现出表皮或与 CL 相关的表型。我们还研究了一种新的化学诱导的 Pycr2 突变。Pycr2 隐性失功能突变的小鼠表现出与神经和神经肌肉疾病一致的表型,包括体重减轻、脊柱后凸和后肢扣状。周围神经系统基本不受影响,只有周围神经中的轴突轻度萎缩。Pycr2 突变小鼠严重缺乏皮下脂肪,使人联想到 CL 样表型,但未观察到弹性蛋白异常等主要特征。年老的 Pycr2 突变小鼠的白细胞计数减少,脂质代谢改变,提示存在全身性代谢紊乱。PYCR1 和 -2 具有相似的酶和细胞活性,与之前的研究一致,两者在成纤维细胞中都定位于线粒体。PYCR1 和 -2 都能够弥补酵母酶 Pro3 的缺失,该酶将 P5C 转化为脯氨酸,证实了它们作为 P5C 还原酶的活性。在小鼠中,与单突变体相比,Pycr1;Pycr2 双突变体的生存能力和健康状况较差,表明这些基因在很大程度上具有功能冗余性。与皮肤成纤维细胞培养物的裂解物相比,Pycr2 突变小鼠的血清中脯氨酸水平没有降低,前体也没有增加,但将 Pycr2 突变小鼠置于不含脯氨酸的饮食中会使表型恶化。因此,Pycr1 和 -2 在脯氨酸生物合成中具有冗余功能,它们的缺失使脯氨酸成为半必需氨基酸。这些发现对理解 CL 和 HLD10 的遗传学以及在小鼠中模拟这些疾病具有重要意义。
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