CDR1as expression in PBMCs strongly discriminated vulnerable carotid plaques, correlating with plaque inflammation and outperforming other circRNAs as a noninvasive biomarker.
Do circulating circRNAs in PBMCs identify carotid atherosclerotic plaque vulnerability preoperatively in patients undergoing carotid endarterectomy?
Circulating circRNAs, particularly CDR1as, show promise as noninvasive biomarkers for preoperative risk stratification of carotid plaque vulnerability.
Tasa de eventos absoluta: 0% vs 0%
Vulnerable carotid atherosclerotic plaques are prone to cap rupture and thrombosis, yet definitive assessment still relies on postoperative histology. We investigated whether circulating circular RNAs (circRNAs) in peripheral blood mononuclear cells (PBMCs) can identify plaque vulnerability preoperatively. In patients undergoing carotid endarterectomy, plaques were classified as vulnerable or stable, and PBMC expression of candidate circRNAs (circVIRMA, circGRN, circANRIL and CDR1as) and paired linear transcripts was quantified by RT-qPCR. A composite in-plaqueSCORE (IL-1β, IL-6, IL-10, PPARγ mRNAs) characterized intraplaque inflammation. We derived two PBMC metrics: circRNASCORE (mean expression of deregulated circRNAs) and circ/linear mRNASCORE (mean of circ/linear mRNA expression ratios) and evaluated diagnostic performance by Receiver Operating Characteristic curve (ROC) analysis and logistic regression. circVIRMA and circGRN were modestly increased in PBMCs from patients with vulnerable plaques, whereas linear host genes were unchanged. CDR1as was markedly upregulated and showed the strongest discrimination among the other circRNAs, similarly to the circRNAₐnd circRNA/linear mRNA ratioSCOREs. Indeed, circRNASCORE correlated positively with the intraplaque inflammatory in-plaqueSCORE, linking systemic signatures to local plaque biology. In plaque tissue, CDR1 mRNA was reduced while CDR1as was relatively preserved, yielding a higher CDR1as/CDR1 mRNA ratio in vulnerable lesions. PBMC circRNAs—particularly CDR1as —show promise as noninvasive biomarkers of carotid plaque vulnerability and reflect plaque inflammatory status. Validation in independent cohorts and integration with imaging could enable improved preoperative risk stratification. • circVIRMA, circGRN and CDR1as increased in PBMCs of vulnerable plaque patients; linear transcripts unchanged. • CDR1as (1) was strongly upregulated, and its level and ratio to linear CDR1 best predicted disease among circRNAs tested. • CDR1as (1) showed discrimination comparable to circRNA and circRNA/mRNA ratio scores, supporting its biomarker potential. • circRNASCORE positively correlated with in-plaque inflammatory score, linking systemic and local plaque biology.
Greco et al. (Wed,) reported a other. CDR1as expression in PBMCs strongly discriminated vulnerable carotid plaques, correlating with plaque inflammation and outperforming other circRNAs as a noninvasive biomarker.