ZNF671 methylation is a potential regression predictor of cervical intraepithelial neoplasia grade 3 in the colposcopy-to-conization interval.

OBJECTIVE

Despite the high risk of cervical intraepithelial neoplasia grade 3 (CIN3) progressing to cervical cancer, approximately 50 percent of CIN3 lesions were overtreated. Furthermore, CIN3 patients who underwent surgery experienced complications and adverse obstetric outcomes. Therefore, exploring reliable biomarkers to differentiate regressing CIN3 lesions from persistent ones is imperative to preserve female fertility.

METHODS

This study evaluated the association between the methylation level of zinc finger protein 671 (ZNF671) and the regression of CIN3 lesions by examining the postoperative pathology of the cones removed by cold knife conization (CKC) or loop electrosurgical excision procedure (LEEP).

RESULTS

In the analysis of 127 cervical scraping cells from CIN3 patients, negative ZNF671 results were significantly associated with downgraded postoperative pathology (OR = 0.225, 95 % CI: 0.084-0.599). Compared to the overall (CKC and LEEP) group, the predictive performance of ZNF671 in the CKC subgroup was improved by 58.7 % (OR = 0.093, 95 % CI: 0.018-0.480). Our results showed that the ZNF671/cytology/HPV16/18 combination (OR = 0.033, 95 % CI: 0.003-0.376) improved the accuracy of detecting cervical intraepithelial neoplasia grade 1 or less (CIN1-) in the CKC subgroup. However, none of the tests could distinguish the postoperative pathology CIN1- from CIN2+ in the LEEP group.

CONCLUSION

These results support that ZNF671 has the potential to predict the regression of CIN3 lesions, and the improved predictive performance of the ZNF671/cytology/HPV16/18 combination may inform individualized treatment of CIN3 patients planning to undergo CKC.