AUTHOR=Xiao Dongfan , Shi Congcong , Zhang Yinchun , Li Sitao , Ye Yuhao , Yuan Guilong , Miu Taohan , Ma Haiyan , Diao Shiguang , Su Chaoyun , Li Zhitao , Li Haiyan , Zhuang Guiying , Wang Yuanli , Lu Feiyan , Gu Xia , Zhou Wei , Xiao Xin , Huang Weiben , Wei Tao , Hao Hu 

TITLE=Using metabolic abnormalities of carriers in the neonatal period to evaluate the pathogenicity of variants of uncertain significance in methylmalonic acidemia

JOURNAL=Frontiers in Genetics

VOLUME=15

YEAR=2024

URL=https://www.frontiersin.org/journals/genetics/articles/10.3389/fgene.2024.1403913

DOI=10.3389/fgene.2024.1403913

ISSN=1664-8021

ABSTRACT=<sec><title>Objective</title><p>To accurately verify the pathogenicity of variants of uncertain significance (VUS) in <italic>MUT</italic> and <italic>MMACHC</italic> genes through mass spectrometry and <italic>silico</italic> analysis.</p></sec><sec><title>Methods</title><p>This multicenter retrospective study included 35 participating units (<ext-link ext-link-type="uri" xlink:href="http://ClinicalTrials.gov" xmlns:xlink="http://www.w3.org/1999/xlink">ClinicalTrials.gov</ext-link> ID: NCT06183138). A total of 3,071 newborns (within 7 days of birth) were sorted into carrying pathogenic/likely pathogenic (P/LP) variants and carrying VUS, non-variant groups. Differences in metabolites among the groups were calculated using statistical analyses. Changes in conservatism, free energy, and interaction force of <italic>MMUT</italic> and <italic>MMACHC</italic> variants were analyzed using <italic>silico</italic> analysis.</p></sec><sec><title>Results</title><p>The percentage of those carrying VUS cases was 68.15% (659/967). In the <italic>MMUT</italic> gene variant, we found that C3, C3/C2, and C3/C0 levels in those carrying the P/LP variant group were higher than those in the non-variant group (<italic>p</italic> &lt; 0.000). The conservative scores of those carrying the P/LP variant group were &gt;7. C3, C3/C0, and C3/C2 values of newborns carrying VUS (c.1159A&gt;C and c.1286A&gt;G) were significantly higher than those of the non-variant group and the remaining VUS newborns (<italic>p</italic> &lt; 0.005). The conservative scores of c.1159A&gt;C and c.1286A&gt;G calculated by ConSurf analysis were 9 and 7, respectively. Unfortunately, three MMA patients with c.1159A&gt;C died during the neonatal period; their C3, C3/C0, C3/C2, and MMA levels were significantly higher than those of the controls.</p></sec><sec><title>Conclusion</title><p>Common variants of methylmalonic acidemia in the study population were categorized as VUS. In the neonatal period, the metabolic biomarkers of those carrying the P/LP variant group of the <italic>MUT</italic> gene were significantly higher than those in the non-variant group. If the metabolic biomarkers of those carrying VUS are also significantly increased, combined with <italic>silico</italic> analysis the VUS may be elevated to a likely pathogenic variant. The results also suggest that mass spectrometry and <italic>silico</italic> analysis may be feasible screening methods for verifying the pathogenicity of VUS in other inherited metabolic diseases.</p></sec>