Differential impact of glycation on apolipoprotein A-I of high-density lipoprotein: a review

Author:

Maarfi Farah1,Ahmad Saheem23ORCID,Alouffi Sultan23ORCID,Akasha Rihab23,Khan M Salman4,Rafi Zeeshan5,Basnet Hemashri1,Khan Mohd Yasir1ORCID

Affiliation:

1. Uttaranchal University Department of Biotechnology, School of Applied & Life Sciences (SALS), , Dehradun 248007, Uttarakhand , India

2. University of Hail Department of Medical Laboratory Sciences, College of Applied Medical Sciences, , Hail 2440 , Saudi Arabia

3. University of Hail Molecular Diagnostic & Personalized Therapeutic Unit, , Hail 2440 , Saudi Arabia

4. Integral University Department of Biosciences, IIRC-5, Clinical Biochemistry and Natural Product Research Lab, , Lucknow 226026, Uttar Pradesh , India

5. Integral University Department of Bioengineering, , Lucknow 226026, Uttar Pradesh , India

Abstract

AbstractHyperglycemia is a poorly controlled diabetic condition, affects about 70% of people all round the world. In the year 2015, about 41.5 crore people were diabetic and is expected to reach around 64.3 crore by the year 2040. Cardiovascular diseases (CVDs) are considered as one of the major risk factors that cause more than half of the death of diabetic patients and promote related comorbidities. Atherosclerosis and amyloidosis are the prime factors linked with CVDs. Apolipoprotein A-I (ApoA-I) of HDL have protective action against CVDs, participate in reverse cholesterol transport mechanism and lipid metabolism, but gets easily glycated under prolonged hyperglycemic aura, i.e. glycation. ApoA-I have a potent role in maintenance of glucose level, providing a compelling link between diabetes and CVDs. Increased protein glycation in people with diabetes promote atherosclerosis, which might play possible role in promotion of protein aggregation by altering the protein structure and its confirmation. Here, we intend to investigate the mechanistic behavior of ApoA-I under the menace of glycation and its impact on ApoA-I structure and function that possibly link with aggregation or amyloidosis.

Funder

Scientific Research Deanship at University of Ha’il

Publisher

Oxford University Press (OUP)

Subject

Biochemistry

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