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Current Understanding on the Genetic Basis of Key Metabolic Disorders: A Review

期刊

BIOLOGY-BASEL
卷 11, 期 9, 页码 -

出版社

MDPI
DOI: 10.3390/biology11091308

关键词

bioinformatics; biomarkers; epigenetics; genetic modifications; genome editing; genome wide association studies

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资金

  1. Universiti Malaysia Sabah [DKC 2009]

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Metabolic disorders present a challenge to healthcare systems, and changes in lifestyle and genetic factors have a significant impact on these disorders. Diabetes Mellitus and Familial hypercholesterolemia are the most extensively researched disorders. Current therapeutic approaches rely on substrate reduction, dietary restrictions, exercise, and mental health maintenance, but there are also emerging personalized therapies targeting individual genes. The treatment of rare metabolic disorders is still in its early stages due to insufficient research and development investment, but there are advances in personalized therapeutics based on gene silencing and related technologies. Data acquisition through various platforms has allowed for a better understanding of metabolic disorders and led to interventions targeting genetic causes, lifestyle changes, and dietary regulation.
Metabolic disorders (MD) are a challenge to healthcare systems; the emergence of the modern socio-economic system has led to a profound change in lifestyles in terms of dietary habits, exercise regimens, and behavior, all of which complement the genetic factors associated with MD. Diabetes Mellitus and Familial hypercholesterolemia are two of the 14 most widely researched MD, as they pose the greatest challenge to the public healthcare system and have an impact on productivity and the economy. Research findings have led to the development of new therapeutic molecules for the mitigation of MD as well as the invention of experimental strategies, which target the genes themselves via gene editing and RNA interference. Although these approaches may herald the emergence of a new toolbox to treat MD, the current therapeutic approaches still heavily depend on substrate reduction, dietary restrictions based on genetic factors, exercise, and the maintenance of good mental health. The development of orphan drugs for the less common MD such as Krabbe, Farber, Fabry, and Gaucher diseases, remains in its infancy, owing to the lack of investment in research and development, and this has driven the development of personalized therapeutics based on gene silencing and related technologies. Advances in data acquisition via high resolution genomic, transcriptomic, proteomic and metabolomic platforms have driven the discovery of the underlying factors associated with metabolic disorders (MD) and led to interventions that target the underlying genetic causes as well as lifestyle changes and dietary regulation. The review focuses on fourteen of the most widely studied inherited MD, which are familial hypercholesterolemia, Gaucher disease, Hunter syndrome, Krabbe disease, Maple syrup urine disease, Metachromatic leukodystrophy, Mitochondrial encephalopathy lactic acidosis stroke-like episodes (MELAS), Niemann-Pick disease, Phenylketonuria (PKU), Porphyria, Tay-Sachs disease, Wilson's disease, Familial hypertriglyceridemia (F-HTG) and Galactosemia based on genome wide association studies, epigenetic factors, transcript regulation, post-translational genetic modifications and biomarker discovery through metabolomic studies. We will delve into the current approaches being undertaken to analyze metadata using bioinformatic approaches and the emerging interventions using genome editing platforms as applied to animal models.

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