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Heterogenous NECTIN4 expression in urothelial high-risk non-muscle-invasive bladder cancer. | LitMetric

AI Article Synopsis

  • High-grade non-muscle-invasive bladder cancer (HG NMIBC) patients have a high risk of progressing to muscle invasive cancer, and there is a need for new bladder-preserving treatments.
  • Recent approvals of enfortumab vedotin, which targets NECTIN4, show potential for treating advanced bladder cancer, but more research is needed on NECTIN4 in HG NMIBC.
  • A study found that NECTIN4 positivity was high (91% overall) in various HG NMIBC subgroups, with significant differences in expression levels, suggesting that NECTIN4-targeted therapies could be beneficial, particularly for patients with carcinoma in situ (CIS) and pure papillary tumors.

Article Abstract

High-grade non-muscle-invasive bladder cancer (HG NMIBC) patients are at high risk (HR) of progression to muscle-invasion. Bladder-preserving therapies for this patient subgroup are limited, and additional treatments are desirable. Recently, enfortumab vedotin, targeting cancer-associated NECTIN4, has been approved for the treatment of advanced urothelial carcinoma. However, data on the expression of NECTIN4 and its therapeutic potential for HR NMIBC are scarce. Here, NECTIN4 was immunohistochemically analyzed in urothelial HG NMIBC by studying cohorts of carcinoma in situ (CIS)/T1HG (N = 182 samples), HG papillary tumors from mixed-grade lesions (mixed TaHG) (N = 87) and papillary HG tumors without a history of low-grade disease (pure TaHG/T1HG) (N = 98) from overall 225 patients. Moreover, inter-lesional NECTIN4 heterogeneity in multifocal HG NMIBC tumors was determined. A high prevalence of NECTIN4 positivity was noted across HG NMIBC subgroups (91%, N = 367 samples), with 77% of samples showing moderate/strong expression. Heterogenous NECTIN4 levels were observed between HG NMIBC subgroups: non-invasive areas of CIS/T1HG and pure TaHG/T1HG samples showed NECTIN4 positivity in 96% and 99%, with 88% and 83% moderate/strong expressing specimens, respectively, whereas significantly lower NECTIN4 levels were detected in mixed TaHG lesions (72% positivity, 48% of samples with moderate/strong NECTIN4 expression). Moreover, higher NECTIN4 heterogeneity was observed in patients with multifocal mixed TaHG tumors (22% of patients) compared to patients with multifocal CIS/T1HG and pure TaHG/T1HG tumors (9% and 5%). Taken together, NECTIN4-directed antibody-drug conjugates might be promising for the treatment of HR NMIBC patients, especially for those exhibiting CIS/T1HG and pure TaHG/T1HG tumors without a history of low-grade disease.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9226103PMC
http://dx.doi.org/10.1007/s00428-022-03328-1DOI Listing

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