Attenuated brain-derived neurotrophic factor and hypertrophic remodelling: The SABPA study
Research output: Contribution to journal › Research article › Contributed › peer-review
Contributors
Abstract
Brain-derived neurotrophic factor (BDNF) has been linked to neurological pathologies, but its role in cardiometabolic disturbances is limited. We aimed to assess the association between serum BDNF levels and structural endothelial dysfunction (ED) as determined by cross-sectional wall area (CSWA) and albumin/creatinine ratio (ACR) in black Africans. Ambulatory blood pressure (BP) and ultrasound CSWA values were obtained from 82 males and 90 females. Fasting blood and 8 h overnight urine samples were collected to determine serum BDNF and cardiometabolic risk markers, that is, glycated haemoglobin (HbA1c), lipids, inflammation and ACR. BDNF median split × gender interaction effects for structural ED justified stratification of BDNF into low and high (≤/>1.37 ng ml-1) gender groups. BDNF values (0.86-1.98 ng ml-1) were substantially lower than reference ranges (6.97-42.6 ng ml-1) in the African gender cohort, independent of age and body mass index. No relationship was revealed between BDNF and renal function and was opposed by an inverse relationship between BDNF and CSWA (r=-0.17; P=0.03) in the African cohort. Linear regression analyses revealed a positive relationship between systolic BP and structural remodelling in the total cohort and low-BDNF gender groups. In the high-BDNF females, HbA1C was associated with structural remodelling. Attenuated or possible downregulated BDNF levels were associated with hypertrophic remodelling, and may be a compensatory mechanism for the higher BP in Africans. In addition, metabolic risk and hypertrophic remodelling in women with high BDNF underpin different underlying mechanisms for impaired neurotrophin homeostasis in men and women.
Details
Original language | English |
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Pages (from-to) | 33-39 |
Number of pages | 7 |
Journal | Journal of human hypertension |
Volume | 29 |
Issue number | 1 |
Publication status | Published - 11 Jan 2015 |
Peer-reviewed | Yes |
External IDs
PubMed | 24898921 |
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ORCID | /0000-0001-8799-8202/work/171553505 |