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The follow-up of Chinese patients in mut-type methylmalonic acidemia identified through expanded newborn screening
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  • Shiying Ling,
  • Shengnan Wu,
  • Ruixue Shuai,
  • Yue Yu,
  • Wenjuan Qiu,
  • Haiyan Wei,
  • Chiju Yang,
  • Peng Xu,
  • Hui Zou,
  • Jizhen Feng,
  • Tingting Niu,
  • Haili Hu,
  • Huiwen Zhang,
  • Lili Liang,
  • Yu Wang,
  • Ting Chen,
  • Feng Xu,
  • Xuefan Gu,
  • Lianshu Han
Shiying Ling
Shanghai Jiaotong University School of Medicine Xinhua Hospital

Corresponding Author:lingshiying9757@163.com

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Shengnan Wu
Zhengzhou University Medical College
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Ruixue Shuai
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Yue Yu
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Wenjuan Qiu
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Haiyan Wei
Zhengzhou University Medical College
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Chiju Yang
Jining Medical University
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Peng Xu
Jining Medical University
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Hui Zou
Shandong Provincial Hospital
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Jizhen Feng
Shijiazhuang Medical College
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Tingting Niu
Shandong University
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Haili Hu
Hefei University
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Huiwen Zhang
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Lili Liang
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Yu Wang
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Ting Chen
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Feng Xu
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Xuefan Gu
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Lianshu Han
Shanghai Jiaotong University School of Medicine Xinhua Hospital
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Abstract

Background: Isolated methylmalonic acidemia (MMA), an autosomal recessive disorder of propionate metabolism, is usually caused by mutations in the methylmalonyl-CoA mutase gene (mut-type MMA). Because no universal consensus was made on whether mut-type MMA should be included in newborn screening (NBS), we aimed to compare the outcome of this disorder detected by NBS with that detected clinically and investigate the influence of NBS on the disease course. Methods: In this study, 168 patients with mut-type MMA diagnosed by NBS were compared to 210 patients diagnosed after disease onset while NBS was not performed. Clinical data of these patients from 7 metabolic centers in China were analyzed retrospectively, including initial manifestations, biochemical metabolites, the responsiveness of vitamin B12 therapy, and gene variation, to explore different factors on the long-term outcome. Results: Among patients diagnosed through NBS, 77 patients (45.8%) remained asymptomatic and 87 patients (53.4%) showed favorable neurocognitive outcomes. In contrast with individuals diagnosed clinically, only 30 cases (16.2%) developed healthily. In our comparison of patients whether detected by NBS, the age at diagnosis, the incidence of disease onset, the responsiveness of vitamin B12, age at the start of vitamin B12 treatment, levels of biochemical features before and after treatment, and the long-term prognosis were remarkably different ( P<0.01). The presence of disease onset and the blood C3/C2 ratio were more associated with poor outcomes of patients whether identified by NBS. Importantly, after considering NBS, the odd ratio of disease onset for poor outcome decreased and the unresponsiveness to vitamin B12 increased. Conclusion: Through preventing major disease-related events and allowing an earlier treatment initiation, NBS is beneficial for the prognosis of infants with mut-type MMA.