IGFBP7 and left ventricular mass regression: a sub‐analysis of the EMPA‐HEART CardioLink‐6 randomized clinical trial

Author:

Puar Pankaj123,Mistry Nikhil45,Connelly Kim A.25678ORCID,Yan Andrew T.67ORCID,Quan Adrian12ORCID,Teoh Hwee129ORCID,Pan Yi12,Verma Raj110,Hess David A.2311ORCID,Verma Subodh12312ORCID,Mazer C. David245813ORCID

Affiliation:

1. Division of Cardiac Surgery St. Michael's Hospital, Unity Health Toronto Toronto Ontario Canada

2. Keenan Research Centre for Biomedical Science in the Li Ka Shing Knowledge Institute of St. Michael's Hospital Toronto Ontario Canada

3. Department of Pharmacology and Toxicology University of Toronto Toronto Ontario Canada

4. Department of Anesthesia St. Michael's Hospital, Unity Health Toronto Toronto Ontario Canada

5. Institute of Medical Science University of Toronto Toronto Ontario Canada

6. Division of Cardiology St. Michael's Hospital, Unity Health Toronto Toronto Ontario Canada

7. Department of Medicine University of Toronto Toronto Ontario Canada

8. Department of Physiology University of Toronto Toronto Ontario Canada

9. Division of Endocrinology and Metabolism St. Michael's Hospital, Unity Health Toronto Toronto Ontario Canada

10. Royal College of Surgeons in Ireland Dublin Ireland

11. Department of Physiology and Pharmacology University of Western Ontario London Ontario Canada

12. Department of Surgery University of Toronto Toronto Ontario Canada

13. Department of Anesthesiology and Pain Medicine University of Toronto Toronto Ontario Canada

Abstract

AbstractAimsGiven recent suggestions that serum levels of insulin‐like growth factor‐binding protein 7 (IGFBP7) may identify patients who derive greater cardiorenal benefits from treatment with sodium‐glucose transport 2 inhibitors (SGLT2i), this exploratory sub‐analysis of the EMPA‐HEART CardioLink‐6 randomized controlled trial evaluated the association between serum levels of IGFBP7 and empagliflozin‐mediated left ventricular mass regression.Methods and resultsThe EMPA‐HEART CardioLink‐6 trial used gold‐standard cardiac magnetic resonance imaging to detect change in left ventricular mass indexed to body surface area (LVMi) following 6 months of treatment with empagliflozin or matching placebo in 97 patients with type 2 diabetes and coronary artery disease. Serum samples were collected at baseline and analysed for IGFBP7 using an enzyme‐linked immunosorbent assay. A multivariate linear regression model was used to assess the association between IGFBP7 and baseline LVMi. A linear model adjusting for baseline differences in LVMi was used to test the relationship between baseline IGFBP7 level, change in LVMi over 6 months, and treatment arm. Of the 97 patients enrolled, 74 had complete covariate data and were included in our analysis. No association between baseline IGFBP7 and baseline LVMi was found [baseline LVMi: 0.14 g/m2 (95% CI: −0.29 g/m2 to 0.57 g/m2) per 1 ng/mL higher baseline IGFBP7]. In addition, no difference between patients treated with empagliflozin versus matching placebo was found when evaluating the association between serum IGFBP7, 6 month change in LVMi, and treatment arm [empagliflozin 6 month change in LVMi: 0.25 g/m2 (95% CI: −0.17 g/m2 to 0.67 g/m2) per 1 ng/mL higher IGFBP7 vs. matching placebo 6 month change in LVMi: 0.07 g/m2 (95% CI: −0.21 g/m2 to 0.35 g/m2) per 1 ng/mL higher IGFBP7; Pinteraction = 0.49]. Additional sensitivity analysis assessing IGFBP7 as a categorical variable (above/below the median) showed no significant association between IGFBP7, 6 month change in LVMi, and treatment arm.ConclusionsOur study provides insight into the generalizability of IGFBP7 as a surrogate marker of cardiac remodelling in patients with type 2 diabetes and coronary artery disease. Our results suggest that SGLT2i‐mediated reverse cardiac remodelling may be independent of IGFBP7 levels. Further investigations evaluating the association between IGFBP7 and SGLT2i are suggested to understand if and how IGFBP7 levels may modulate benefits received from SLGT2i.

Funder

Boehringer Ingelheim

Publisher

Wiley

Subject

Cardiology and Cardiovascular Medicine

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