Association of Region‐Specific Cardiac Adiposity With Dysglycemia and New‐Onset Diabetes

Author:

Sung Kuo‐Tzu123ORCID,Kuo Jen‐Yuan124,Yun Chun‐Ho145,Lin Yueh‐Hung123,Tsai Jui‐Peng12,Lo Chi‐In12,Hsiao Chih‐Chung12,Lai Yau‐Huei146,Tsai Cheng‐Ting124ORCID,Hou Charles Jia‐Yin124ORCID,Su Cheng‐Huang124,Yeh Hung‐I124ORCID,Chien Chen‐Yen247,Hung Ta‐Chuan124,Hung Chung‐Lieh128ORCID

Affiliation:

1. Division of Cardiology Department of Internal Medicine MacKay Memorial Hospital Taipei Taiwan

2. Department of Medicine MacKay Medical College New Taipei City Taiwan

3. Institute of Clinical MedicineNational Yang Ming Chao Tung University Taipei Taiwan

4. MacKay Medicine Nursing, and Management College Taipei Taiwan

5. Division of Radiology MacKay Memorial Hospital Taipei Taiwan

6. Division of Cardiology Department of Internal Medicine MacKay Memorial Hospital Hsinchu Taiwan

7. Cardiovascular Division Department of Surgery MacKay Memorial Hospital Taipei Taiwan

8. Institute of Biomedical SciencesMacKay Medical College New Taipei City Taiwan

Abstract

Background Visceral adipose tissue is assumed to be an important indicator for insulin resistance and diabetes beyond overweight/obesity. We hypothesized that region‐specific visceral adipose tissue may regulate differential biological effects for new‐onset diabetes regardless of overall obesity. Methods and Results We quantified various visceral adipose tissue measures, including epicardial adipose tissue, paracardial adipose tissue, interatrial fat, periaortic fat, and thoracic aortic adipose tissue in 1039 consecutive asymptomatic participants who underwent multidetector computed tomography. We explored the associations of visceral adipose tissue with baseline dysglycemic indices and new‐onset diabetes. Epicardial adipose tissue, paracardial adipose tissue, interatrial fat, periaortic fat, and thoracic aortic adipose tissue were differentially and independently associated with dysglycemic indices (fasting glucose, postprandial glucose, HbA1c, and homeostasis model assessment of insulin resistance) beyond anthropometric measures. The superimposition of interatrial fat and thoracic aortic adipose tissue on age, sex, body mass index, and baseline homeostasis model assessment of insulin resistance expanded the likelihood of baseline diabetes (from 67.2 to 86.0 and 64.4 to 70.8, P for ∆ ꭕ 2 : <0.001 and 0.011, respectively). Compared with the first tertile, the highest interatrial fat tertile showed a nearly doubled risk for new‐onset diabetes (hazard ratio, 2.09 [95% CI, 1.38–3.15], P <0.001) after adjusting for Chinese Visceral Adiposity Index. Conclusions Region‐specific visceral adiposity may not perform equally in discriminating baseline dysglycemia or diabetes, and showed differential predictive performance in new‐onset diabetes. Our data suggested that interatrial fat may serve as a potential marker for new‐onset diabetes.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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