Pacific Northwest Research Institute, Seattle, Washington.
J Inherit Metab Dis. 2020 Jul;43(4):758-769. doi: 10.1002/jimd.12227. Epub 2020 Feb 27.
Defects in serine biosynthesis resulting from loss of function mutations in PHGDH, PSAT1, and PSPH cause a set of rare, autosomal recessive diseases known as Neu-Laxova syndrome (NLS) or serine-deficiency disorders. The diseases present with a broad range of phenotypes including lethality, severe neurological manifestations, seizures, and intellectual disability. However, because L-serine supplementation, especially if started prenatally, can ameliorate and in some cases even prevent symptoms, knowledge of pathogenic variants is medically actionable. Here, we describe a functional assay that leverages the evolutionary conservation of an enzyme in the serine biosynthesis pathway, phosphoserine aminotransferase, and the ability of the human protein-coding sequence (PSAT1) to functionally replace its yeast ortholog (SER1). Results from our quantitative, yeast-based assay agree well with clinical annotations and expectations based on the disease literature. Using this assay, we have measured the functional impact of the 199 PSAT1 variants currently listed in ClinVar, gnomAD, and the literature. We anticipate that the assay could be used to comprehensively assess the functional impact of all SNP-accessible amino acid substitution mutations in PSAT1, a resource that could aid variant interpretation and identify potential NLS carriers.
由于 PHGDH、PSAT1 和 PSPH 功能丧失突变导致丝氨酸生物合成缺陷,会引起一组罕见的常染色体隐性疾病,称为 Neu-Laxova 综合征(NLS)或丝氨酸缺乏症。这些疾病表现出广泛的表型,包括致死性、严重的神经表现、癫痫发作和智力残疾。然而,由于 L-丝氨酸补充,特别是如果在产前开始,可以改善,在某些情况下甚至可以预防症状,因此了解致病性变异是有医学意义的。在这里,我们描述了一种功能测定方法,该方法利用了丝氨酸生物合成途径中酶磷酸丝氨酸氨基转移酶的进化保守性,以及人类蛋白编码序列(PSAT1)能够替代其酵母同源物(SER1)的功能。我们基于酵母的定量测定结果与临床注释以及基于疾病文献的预期非常吻合。使用该测定方法,我们已经测量了 ClinVar、gnomAD 和文献中目前列出的 199 种 PSAT1 变体的功能影响。我们预计该测定方法可用于全面评估 PSAT1 中所有 SNP 可及的氨基酸取代突变的功能影响,这将有助于变异解释并识别潜在的 NLS 携带者。
