Hemoglobin A1C as the Strongest Influencing Factor in relation to Vascular Stiffness in Type 2 Diabetes Mellitus - Metabolic Syndrome Patients

Deasy Ardiany; Soebagijo Adi; Ari Sutjahjo; Askandar Tjokroprawiro

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Paper

Hemoglobin A1C as the Strongest Influencing Factor in relation to Vascular Stiffness in Type 2 Diabetes Mellitus - Metabolic Syndrome Patients

In Proceedings of Surabaya International Physiology Seminar SIPS - Volume 1, 331-335, 2017 , Jawa Timur, Indonesia

Authors: Deasy Ardiany ; Soebagijo Adi ; Ari Sutjahjo and Askandar Tjokroprawiro

Affiliation: Department of Internal Medicine, Faculty of medicine Universitas Airlangga, Dr. Soetomo General Hospital and Surabaya, Indonesia

Keyword(s): Type 2 Diabetes Mellitus, Metabolic Syndrome, HbA1c, brachial-ankle pulse wave velocity (baPWV), Vascular Stiffness

Abstract: The risk of cardiovascular disease in type 2 diabetes mellitus (T2DM) will be high despite intensive glycemic control. This is because T2DM is often accompanied by the condition of metabolic syndrome (MetS). Endothelial dysfunction can be assessed by non-invasive pulse wave velocity (PWV) measurement, which is an arterial stiffness influencing factor. This research aimed to determine the correlation of influencing factors in regard to metabolic syndrome and HbA1c in relation to vascular stiffness as measured by baPWV value in T2DM-Mets. The research was conducted at the Diabetes Outpatient Clinic of Dr. Sutomo General Hospital Surabaya and six Primary Healthcare clinics in Surabaya from December 21, 2010 - March 21, 2012. Subjects fulfilling the inclusion and exclusion criteria were measured with regard to blood pressure, BMI, waist circumference, laboratory examination: Fasting plasma glucose, Post prandial glucose, Hemoglobin A1c and ba-PWV measurements with V Serra-1000 devices. A total of 33 patients with T2DM met the inclusion and exclusion criteria. The result of the statistical analysis shows that there is a significant correlation between the HbA1c value and ba-PWV (p = 0.036). Other influencing factors exhibited a non-significant correlation with vascular stiffness (p >0.05). The contribution of metabolic syndrome and HbA1c influencing factors was 4.6% with respect to vascular stiffness (Adjusted R2 = 0.046). Together the influencing factors in regard to metabolic syndrome and HbA1c had no significant effect on vascular stiffness (p = 0.584). HbA1c is the influencing factor that has the greatest effect on vascular stiffness. There was a significant correlation between HbA1c and vascular stiffness as measured by baPWV compared with other metabolic syndrome components. The contribution of influencing factors in regard to metabolic syndrome and HbA1c was 4.6% against vascular stiffness. Hemoglobin A1c is the influencing factor that has the greatest effect on vascular stiffness. (More)

The risk of cardiovascular disease in type 2 diabetes mellitus (T2DM) will be high despite intensive glycemic control. This is because T2DM is often accompanied by the condition of metabolic syndrome (MetS). Endothelial dysfunction can be assessed by non-invasive pulse wave velocity (PWV) measurement, which is an arterial stiffness influencing factor. This research aimed to determine the correlation of influencing factors in regard to metabolic syndrome and HbA1c in relation to vascular stiffness as measured by baPWV value in T2DM-Mets. The research was conducted at the Diabetes Outpatient Clinic of Dr. Sutomo General Hospital Surabaya and six Primary Healthcare clinics in Surabaya from December 21, 2010 - March 21, 2012. Subjects fulfilling the inclusion and exclusion criteria were measured with regard to blood pressure, BMI, waist circumference, laboratory examination: Fasting plasma glucose, Post prandial glucose, Hemoglobin A1c and ba-PWV measurements with V Serra-1000 devices. A total of 33 patients with T2DM met the inclusion and exclusion criteria. The result of the statistical analysis shows that there is a significant correlation between the HbA1c value and ba-PWV (p = 0.036). Other influencing factors exhibited a non-significant correlation with vascular stiffness (p >0.05). The contribution of metabolic syndrome and HbA1c influencing factors was 4.6% with respect to vascular stiffness (Adjusted R2 = 0.046). Together the influencing factors in regard to metabolic syndrome and HbA1c had no significant effect on vascular stiffness (p = 0.584). HbA1c is the influencing factor that has the greatest effect on vascular stiffness. There was a significant correlation between HbA1c and vascular stiffness as measured by baPWV compared with other metabolic syndrome components. The contribution of influencing factors in regard to metabolic syndrome and HbA1c was 4.6% against vascular stiffness. Hemoglobin A1c is the influencing factor that has the greatest effect on vascular stiffness.

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Paper citation in several formats:

Ardiany, D.; Adi, S.; Sutjahjo, A. and Tjokroprawiro, A. (2018). Hemoglobin A1C as the Strongest Influencing Factor in relation to Vascular Stiffness in Type 2 Diabetes Mellitus - Metabolic Syndrome Patients. In Proceedings of Surabaya International Physiology Seminar - SIPS; ISBN 978-989-758-340-7; ISSN 2184-3678, SciTePress, pages 331-335. DOI: 10.5220/0007338703310335

@conference{sips18,
author={Deasy Ardiany. and Soebagijo Adi. and Ari Sutjahjo. and Askandar Tjokroprawiro.},
title={Hemoglobin A1C as the Strongest Influencing Factor in relation to Vascular Stiffness in Type 2 Diabetes Mellitus - Metabolic Syndrome Patients},
booktitle={Proceedings of Surabaya International Physiology Seminar - SIPS},
year={2018},
pages={331-335},
publisher={SciTePress},
organization={INSTICC},
doi={10.5220/0007338703310335},
isbn={978-989-758-340-7},
issn={2184-3678},
}

TY - CONF

JO - Proceedings of Surabaya International Physiology Seminar - SIPS
TI - Hemoglobin A1C as the Strongest Influencing Factor in relation to Vascular Stiffness in Type 2 Diabetes Mellitus - Metabolic Syndrome Patients
SN - 978-989-758-340-7
IS - 2184-3678
AU - Ardiany, D.
AU - Adi, S.
AU - Sutjahjo, A.
AU - Tjokroprawiro, A.
PY - 2018
SP - 331
EP - 335
DO - 10.5220/0007338703310335
PB - SciTePress