(Open access funding provided by Semmelweis University)
Szakterületek:
Urológia
Distinct molecular subtypes of muscle‐invasive bladder cancer (MIBC) may show different
platinum sensitivities. Currently available data were mostly generated at transcriptome
level and have limited comparability to each other. We aimed to determine the platinum
sensitivity of molecular subtypes by using the protein expression‐based Lund Taxonomy.
In addition, we assessed the tumor heterogeneity within the primary tumor and between
the primary and lymph node (LN) metastatic sites. Thirteen immunohistochemical markers
were stained in a tissue microarray with an overall number of 1,508 cores. Statistical
evaluation was performed in 199 patients divided into three chemo‐naïve MIBC cohorts:
(1) pT3/4 and/or LN+ patients who received radical cystectomy without platinum treatment,
(2) patients who received adjuvant chemotherapy (AC), and (3) patients who underwent
palliative platinum treatment for metastatic disease or postoperative progression.
Overall survival (OS) was used as the primary endpoint. Patients with the genomically
unstable (GU) subtype had significantly better OS in the AC group compared to the
radical cystectomy group (HR: 0.395, 95% CI: 0.205–0.795, p = 0.005). In contrast,
no such association was observed for the basal/squamous (Ba/Sq) subtype. Intratumor
heterogeneity was present in 19% of cases, with the lowest level in the Ba/Sq and
GU tumors (14% each) and the highest level of 43% in small‐cell/neuroendocrine‐like
tumors. There was greater subtype heterogeneity between primary tumors and LN metastases.
In conclusion, immunohistochemistry‐based Lund Taxonomy subtypes remain stable within
the same primary tumor, with the GU subtype deriving the greatest OS benefit from
AC. However, high tumor heterogeneity between the primary tumor and metastatic sites
can impact the effectiveness of therapies.
