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Vulnerable plaque features and adverse events in patients with diabetes mellitus: a post hoc analysis of the COMBINE OCT-FFR trial. | LitMetric

AI Article Synopsis

  • Thin-cap fibroatheroma (TCFA) lesions significantly increase the risk of major cardiovascular events, particularly in patients with diabetes mellitus (DM), but the role of other detected vulnerability features (OCT-VFs) is not well understood.
  • * The COMBINE OCT-FFR study analyzed the prognostic impact of various OCT-VFs, including TCFA, reduced minimal lumen area (r-MLA), healed plaque (HP), and complicated plaque (CP), on patients with non-ischaemic lesions over a 5-year period.
  • * Results indicated that the presence of TCFA along with other OCT-VFs greatly elevated the risk of adverse cardiovascular events (LOCE), highlighting the need for further research into these lesion characteristics in

Article Abstract

Background: Thin-cap fibroatheroma (TCFA) lesions are associated with a high risk of future major adverse cardiovascular events. However, the impact of other optical coherence tomography-detected vulnerability features (OCT-VFs) and their interplay with TCFA in predicting adverse events remains unknown.

Aims: We aimed to evaluate the individual as well as the combined prognostic impact of OCT-VFs in predicting the incidence of the lesion-oriented composite endpoint (LOCE) in non-ischaemic lesions in patients with diabetes mellitus (DM).

Methods: COMBINE OCT-FFR (ClinicalTrials.gov: NCT02989740) was a prospective, double-blind, international, natural history study that included DM patients with ≥1 non-culprit lesions with a fractional flow reserve>0.80 undergoing systematic OCT assessment. OCT-VFs included the following: TCFA, reduced minimal lumen area (r-MLA), healed plaque (HP), and complicated plaque (CP). The primary endpoint, LOCE - a composite of cardiac mortality, target vessel myocardial infarction, or clinically driven target lesion revascularisation up to 5 years - was analysed according to the presence of these OCT-VFs, both individually and in combination.

Results: TCFA, r-MLA, HP and CP were identified in 98 (25.3%), 190 (49.0%), 87 (22.4%), and 116 (29.9%) patients, respectively. The primary endpoint rate increased progressively from 6.3% to 55.6% (hazard ratio 15.2, 95% confidence interval: 4.53-51.0; p<0.001) in patients without OCT-VFs as compared to patients with concomitant HP, r-MLA, CP, and TCFA. The coexistence of TCFA with other OCT-VFs resulted in an increased risk of the LOCE at 5 years.

Conclusions: In DM patients with non-ischaemic lesions, TCFA was the strongest predictor of future LOCE events. However, lesions that present additional OCT-VFs are associated with a higher risk of adverse events than OCT-detected TCFA alone. Further randomised studies are warranted to confirm these findings and their potential clinical implications.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11148652PMC
http://dx.doi.org/10.4244/EIJ-D-23-00628DOI Listing

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