Literature DB >> 33996359

Saccharopinuria accompanied by hyperammonemia and hypercitrullinemia presented with elderly-onset epilepsy, progressive cognitive decline, and gait ataxia.

Ryohei Norioka1, Shinsuke Tobisawa1, Ryusei Nishigori2, Tomiko Kuhara3, Masahide Yazaki4, Masayoshi Nagao5, Toshihiro Ohura6, Yasuyuki Takai7, Asuka Funai1, Kazuhito Miyamoto1, Akihiro Kawata1, Kazushi Takahashi1.   

Abstract

We report a case of saccharopinuria with hyperammonemia and hypercitrullinemia in a Japanese woman who presented with elderly-onset epilepsy, progressive cognitive decline, and gait ataxia. Blood amino acid analysis revealed an increase in citrulline, cystine, and lysine levels, and urine amino acid analysis showed increased citrulline and cystine levels. Urine metabolomics revealed an increased saccharopine level, leading to the definitive diagnosis of saccharopinuria. In western blots of liver biopsy samples, normal citrin levels were observed, suggesting that adult-onset citrullinemia type 2 (CTLN2) was not present. In addition, decreased argininosuccinate synthetase (ASS) levels were observed, and ASS1 gene, a causative gene for citrullinemia type 1 (CTLN1), was analyzed, but no gene mutations were found. Because the causes of hypercitrullinemia were not clear, it might be secondary to saccharopinuria. Muscle biopsy findings of the biceps brachii revealed diminished cytochrome c oxidase (COX) activity, mitochondrial abnormalities on electron microscopy and p62- positive structures in immunohistochemical analyses. Saccharopinuria is generally considered a benign metabolic variant, but our case showed elevated lysine and saccharopine levels causing ornithine circuit damage, mitochondrial dysfunction, and autophagy disorders. This may lead to so far unknown neurological disorders. 2021, International Research and Cooperation Association for Bio & Socio - Sciences Advancement.

Entities:  

Keywords:  elderly-onset neurological disorders; hyperammonemia; hypercitrullinemia; metabolomics; saccharopinuria

Year:  2021        PMID: 33996359      PMCID: PMC8122307          DOI: 10.5582/irdr.2021.01003

Source DB:  PubMed          Journal:  Intractable Rare Dis Res        ISSN: 2186-3644


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