Predictors of the efficacy of His bundle pacing in patients with a prolonged PR interval: A stratified analysis of the HOPE‐HF randomized controlled trial

Author:

Keene Daniel12,Kaza Nandita12,Srinivasan Divya2,Ali Nadine12,Tanner Mark3,Foley Paul4,Chandrasekaran Badri4,Moore Philip56,Adhya Shaumik7,Qureshi Norman8,Muthumala Amal69,Lane Rebecca10,Rinaldi Aldo11,Agarwal Sharad12,Leyva Francisco13,Behar Jonathan10,Bassi Sukh14,Ng Andre15,Scott Paul16,Prasad Rachana17,Swinburn Jon18,Tomson Joseph19,Sethi Amarjit20,Shah Jaymin20,Lim Phang Boon1,Kyriacou Andreas21,Thomas Dewi22,Chuen Jenny23,Kamdar Ravi24,Kanagaratnam Prapa1,Mariveles Myril2,Johnson Nicholas25,Falaschetti Emanuela25,Howard James P.1,Arnold Ahran12,Cleland John G.F.26,Francis Darrel P.1,Whinnett Zachary1,Shun‐Shin Matthew12

Affiliation:

1. National Heart and Lung Institute, Imperial College London London UK

2. Imperial College Healthcare NHS Trust London UK

3. West Sussex Hospitals NHS Trust West Sussex UK

4. Great Western Hospitals NHS Foundation Trust Swindon UK

5. West Hertfordshire Hospitals NHS Trust Hertfordshire UK

6. Barts Health NHS Trust London UK

7. Medway NHS Foundation Trust Kent UK

8. Wycombe General Hospital High Wycombe UK

9. North Middlesex University Hospital London UK

10. Royal Brompton and Harefield NHS Trust London UK

11. Guy's and St. Thomas's NHS Foundation Trust London UK

12. Royal Papworth Hospital NHS Foundation Trust Cambridge UK

13. University Hospitals Birmingham Birmingham UK

14. Sherwood Forest Hospitals NHS Foundation Trust Mansfield UK

15. Department of Cardiovascular Sciences University of Leicester Leicester UK

16. Kings College NHS Hospital London UK

17. Kettering General Hospital Northampton UK

18. Royal Berkshire NHS Foundation Trust Reading UK

19. Royal Free London Foundation NHS Trust London UK

20. London North West University Healthcare NHS Trust London UK

21. Sheffield Teaching Hospitals NHS Foundation Trust Sheffield UK

22. Morriston Hospital Regional Cardiac Centre Swansea UK

23. Nottingham University Hospitals NHS Trust Nottingham UK

24. Croydon NHS University Hospital London UK

25. Imperial College Trials Unit, Imperial College London London UK

26. School of Health and Wellbeing, University of Glasgow Glasgow UK

Abstract

AbstractAimsThe randomized, double‐blind, placebo‐controlled HOPE‐HF trial assessed the benefit of atrio‐ventricular (AV) delay optimization delivered using His bundle pacing. It recruited patients with left ventricular ejection fraction ≤40%, PR interval ≥200 ms, and baseline QRS ≤140 ms or right bundle branch block. Overall, there was no significant increase in peak oxygen uptake (VO2max) but there was significant improvement in heart failure specific quality of life. In this pre‐specified secondary analysis, we evaluated the impact of baseline PR interval, echocardiographic E‐A fusion, and the magnitude of acute high‐precision haemodynamic response to pacing, on outcomes.Methods and resultsAll 167 randomized participants underwent measurement of PR interval, acute haemodynamic response at optimized AV delay, and assessment of presence of E‐A fusion. We tested the impact of these baseline parameters using a Bayesian ordinal model on VO2max, quality of life and activity measures. There was strong evidence of a beneficial interaction between the baseline acute haemodynamic response and the blinded benefit of pacing for VO2 (Pr 99.9%), Minnesota Living With Heart Failure (MLWHF) (Pr 99.8%), MLWHF physical limitation score (Pr 98.9%), EQ‐5D visual analogue scale (Pr 99.6%), and exercise time (Pr 99.4%). The baseline PR interval and the presence of baseline E‐A fusion did not have this reliable ability to predict the clinical benefit of pacing over placebo across multiple endpoints.ConclusionsIn the HOPE‐HF trial, the acute haemodynamic response to pacing reliably identified patients who obtained clinical benefit. Patients with a long PR interval (≥200 ms) and left ventricular impairment who obtained acute haemodynamic improvement with AV‐optimized His bundle pacing were likely to obtain clinical benefit, consistent across multiple endpoints. Importantly, this gradation can be reliably tested for before randomization, but does require high‐precision AV‐optimized haemodynamic assessment to be performed.

Funder

British Heart Foundation

Publisher

Wiley

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