Liver lipid accumulation is a hallmark of non-alcoholic fatty liver disease (NAFLD), broadly associated with insulin resistance. Inositols (INS) are ubiquitous polyols implied in many physiological functions. They are produced endogenously, are present in many foods and in dietary supplements. Alterations in INS metabolism seems to play a role in diseases involving insulin resistance such as diabetes and polycystic ovary syndrome. Given its role in other metabolic syndromes, the hypothesis of an INS role as a supplement in NAFLD is intriguing. We performed a systematic review of the literature to find preclinical and clinical evidence of INS supplementation efficacy in NAFLD patients. We retrieved 10 studies on animal models assessing Myoinosiol or Pinitol deficiency or supplementation and one human randomized controlled trial (RCT). Overall, INS deficiency was associated with increased fatty liver in animals. Conversely, INS supplementation in animal models of fatty liver reduced hepatic triglycerides and cholesterol accumulation and maintained a normal ultrastructural liver histopathology. In the one included RCT, Pinitol supplementation obtained similar results. Pinitol significantly reduced liver fat, post-prandial triglycerides, AST levels, lipid peroxidation increasing glutathione peroxidase activity. These results, despite being limited, indicate the need for further evaluation of INS in NAFLD in larger clinical trials.

Inositol and Non-Alcoholic Fatty Liver Disease: A Systematic Review on Deficiencies and Supplementation / Pani, Arianna; Giossi, Riccardo; Menichelli, Danilo; Andrea Fittipaldo, Veronica; Agnelli, Francesca; Inglese, Elvira; Romandini, Alessandra; Roncato, Rossana; Pintaudi, Basilio; DEL SOLE, Francesco; Scaglione, Francesco. - In: NUTRIENTS. - ISSN 2072-6643. - 12:11(2020), pp. 1-13. [10.3390/nu12113379]

Inositol and Non-Alcoholic Fatty Liver Disease: A Systematic Review on Deficiencies and Supplementation

Danilo Menichelli;Alessandra Romandini;Francesco Del Sole;
2020

Abstract

Liver lipid accumulation is a hallmark of non-alcoholic fatty liver disease (NAFLD), broadly associated with insulin resistance. Inositols (INS) are ubiquitous polyols implied in many physiological functions. They are produced endogenously, are present in many foods and in dietary supplements. Alterations in INS metabolism seems to play a role in diseases involving insulin resistance such as diabetes and polycystic ovary syndrome. Given its role in other metabolic syndromes, the hypothesis of an INS role as a supplement in NAFLD is intriguing. We performed a systematic review of the literature to find preclinical and clinical evidence of INS supplementation efficacy in NAFLD patients. We retrieved 10 studies on animal models assessing Myoinosiol or Pinitol deficiency or supplementation and one human randomized controlled trial (RCT). Overall, INS deficiency was associated with increased fatty liver in animals. Conversely, INS supplementation in animal models of fatty liver reduced hepatic triglycerides and cholesterol accumulation and maintained a normal ultrastructural liver histopathology. In the one included RCT, Pinitol supplementation obtained similar results. Pinitol significantly reduced liver fat, post-prandial triglycerides, AST levels, lipid peroxidation increasing glutathione peroxidase activity. These results, despite being limited, indicate the need for further evaluation of INS in NAFLD in larger clinical trials.
2020
NAFLD; chiro-inositol; inositol; myoinositol; non-alcoholic fatty liver disease; systematic review
01 Pubblicazione su rivista::01a Articolo in rivista
Inositol and Non-Alcoholic Fatty Liver Disease: A Systematic Review on Deficiencies and Supplementation / Pani, Arianna; Giossi, Riccardo; Menichelli, Danilo; Andrea Fittipaldo, Veronica; Agnelli, Francesca; Inglese, Elvira; Romandini, Alessandra; Roncato, Rossana; Pintaudi, Basilio; DEL SOLE, Francesco; Scaglione, Francesco. - In: NUTRIENTS. - ISSN 2072-6643. - 12:11(2020), pp. 1-13. [10.3390/nu12113379]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1691716
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