The Syndromic Triad of COVID-19, Type 2 Diabetes, and Malnutrition

Overview

Journal Front Nutr

Specialty Nutritional Sciences

Date 2023 Mar 10

PMID 36895277

Authors

Jeffrey I Mechanick

Elena A Christofides

Albert E Marchetti

Kristin K Hoddy

Jim Joachim

Refaat Hegazi

Osama Hamdy

Affiliations

Soon will be listed here.

Abstract

The coronavirus disease 2019 (COVID-19) pandemic challenges our collective understanding of transmission, prevention, complications, and clinical management of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Risk factors for severe infection, morbidity, and mortality are associated with age, environment, socioeconomic status, comorbidities, and interventional timing. Clinical investigations report an intriguing association of COVID-19 with diabetes mellitus and malnutrition but incompletely describe the triphasic relationship, its mechanistic pathways, and potential therapeutic approaches to address each malady and their underlying metabolic disorders. This narrative review highlights common chronic disease states that interact epidemiologically and mechanistically with the COVID-19 to create a syndromic phenotype-the COVID-Related Cardiometabolic Syndrome-linking cardiometabolic-based chronic disease drivers with pre-, acute, and chronic/post-COVID-19 disease stages. Since the association of nutritional disorders with COVID-19 and cardiometabolic risk factors is well established, a syndromic triad of COVID-19, type 2 diabetes, and malnutrition is hypothesized that can direct, inform, and optimize care. In this review, each of the three edges of this network is uniquely summarized, nutritional therapies discussed, and a structure for early preventive care proposed. Concerted efforts to identify malnutrition in patients with COVID-19 and elevated metabolic risks are needed and can be followed by improved dietary management while simultaneously addressing dysglycemia-based chronic disease and malnutrition-based chronic disease.

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Moldovan A, Moga I, Moga T, Ghitea E, Babes K, Ghitea T In Vivo. 2023; 37(5):2284-2295.

PMID: 37652474 PMC: 10500484. DOI: 10.21873/invivo.13331.

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