The mutation spectrum and ethnic distribution of non-hepatorenal tyrosinemia (types II, III)

Zahra Beyzaei; Sara Nabavizadeh; Sara Karimzadeh; Bita Geramizadeh

doi:10.1186/s13023-022-02579-0

Orphanet Journal of Rare Diseases (Dec 2022)

The mutation spectrum and ethnic distribution of non-hepatorenal tyrosinemia (types II, III)

Zahra Beyzaei,
Sara Nabavizadeh,
Sara Karimzadeh,
Bita Geramizadeh

Affiliations

Zahra Beyzaei: Transplant Research Center, Shiraz University of Medical Sciences
Sara Nabavizadeh: Transplant Research Center, Shiraz University of Medical Sciences
Sara Karimzadeh: Shiraz Medical School Library, Shiraz University of Medical Sciences
Bita Geramizadeh: Transplant Research Center, Shiraz University of Medical Sciences

DOI: https://doi.org/10.1186/s13023-022-02579-0
Journal volume & issue: Vol. 17, no. 1
pp. 1 – 6

Abstract

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Abstract Background Different types of non-hepatorenal tyrosinemia are among the rare forms of tyrosinemia. Tyrosinemia type II and III are autosomal recessive disorders caused by pathogenic variants in the tyrosine aminotransferase (TAT), and 4-hydroxyphenyl-pyruvate dioxygenas (HPPD) genes, respectively. There are still unclarified aspects in their clinical presentations, mutational spectrum, and genotype–phenotype correlation. Main body In this study, we evaluated the spectrum of TAT and HHPD gene mutations in patients with tyrosinemia type II and III. Moreover, biochemical and clinical findings are evaluated to establish a genotype–phenotype relationship in the above-mentioned patients. Thirty-three TAT variants have been reported in 42 families, consisting of 21 missense variants, 5 frameshift variants, 4 nonsense variants, 2 variants that primarily cause splicing site, and 1 skipping complete exon (large deletion). The most common variant is p.Arg57Ter, causing a splicing defect, and resulting in premature termination of translation, which was found in 10 patients from 3 families. In HPPD gene, eleven variants in 16 patients have been reported including 7 missense variants, 2 nonsense variants, 1 splice defect, and 1 frameshift variant so far. All variants are unique, except for p.Tyr160Cys, which is a missense variant found in two different patients. Regarding genotype–phenotype correlations, in 90% of tyrosinemia type II patients, positive clinical and biochemical correlations with a detected variant are observed. In HPPD gene, due to the small number of patients, it is not possible to make a definite conclusion. Conclusion This is the first large review of variants in TAT and HPPD, highlighting the wide spectrum of disease-causing mutations. Such information is beneficial for the establishment of a privileged mutation screening process in a specific region or ethnic group.

Published in Orphanet Journal of Rare Diseases

ISSN: 1750-1172 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://ojrd.biomedcentral.com

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