Complete pathological response in patients with bladder cancer: predictors and outcomes

Pathologic complete response (pCR) in bladder cancer, most often defined as pT0N0 at radical cystectomy (RC) following transurethral resection of the bladder tumor with/without neoadjuvant therapy, has emerged as a powerful prognostic marker. Predicting pCR before RC and understanding its prognostic nuances are increasingly important as perioperative chemotherapy and immunotherapy evolve. In this study, we reviewed the contemporary evidence regarding definitions and clinical contexts of pCR in bladder cancer; clinical, pathological, imaging, molecular, and liquid-biopsy predictors of pCR; and outcomes and recurrence patterns in patients achieving pCR. We found out that pCR rates vary widely according to treatment regimen, patient selection, and underlying tumor biology, ranging from 5%–15% after transurethral resection alone, 25%–35% with cisplatin-based chemotherapy, and up to 40% with combination chemoimmunotherapy. However, regardless of upfront treatment modality, pCR correlates with significantly improved overall survival and recurrence-free survival. A growing body of evidence has identified predictors of pCR spanning clinical and histopathologic features, molecular and genomic alterations, particularly DNA damage response gene mutations, immune biomarkers (e.g., tumor mutational burden and immune gene expression signatures), advanced imaging with multiparametric magnetic resonance imaging and vesical imaging reporting and data system–based assessment, and circulating tumor DNA dynamics. Among these, circulating tumor DNA clearance during neoadjuvant therapy has demonstrated particularly strong predictive and prognostic value. Despite the favorable outcomes associated with pCR, recurrence risk is not negligible, especially among ypT0 patients, highlighting the importance of risk-adapted postoperative surveillance. In parallel, bladder-preserving strategies for carefully selected patients achieving a clinical complete response remain investigational, limited by imperfect concordance between clinical and pathologic response and requiring rigorous multimodal assessment and close follow-up. Collectively, contemporary data indicate that no single biomarker is sufficient to reliably predict pCR; rather, integrated multimodal models offer the greatest potential to refine neoadjuvant treatment selection, inform bladder preservation, and individualize surveillance while maintaining oncologic safety.