What does this research mean for the field?

Isoform switching events in esophageal adenocarcinoma are significantly linked with patient survival and may serve as novel prognostic and therapeutic targets. Novelty: ClaimNovelty.NOVEL_FINDING. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The research aims to explore isoform switching events in esophageal adenocarcinoma to identify prognostic and therapeutic targets.

March 13, 2026Open Access

Identification of isoform switching events linked with esophageal adenocarcinoma patient survival informs novel prognostic and therapeutic targets

Key Points

The research aims to explore isoform switching events in esophageal adenocarcinoma to identify prognostic and therapeutic targets.
Performed RNA-sequencing analysis in esophageal adenocarcinoma and Barrett's Esophagus lesions.
Stratified patients based on histopathology and TP53 mutation status.
Conducted isoform-specific siRNA knockdown of TTLL12 and HM13 to study their effects on EAC cell viability and response to therapies.
TTLL12 and HM13 knockdown significantly reduced viability in EAC cell lines.
Knockdown enhanced sensitivity to chemotherapy agents paclitaxel and carboplatin.
HM13 isoform knockdown improved response to the anti-PD-L1 agent avelumab.

Abstract

Esophageal adenocarcinoma (EAC), the dominant subtype of esophageal cancer in developed countries, is a growing health problem, characterized by poor patient prognosis and dismal survival due to ineffective screening tools and a lack of efficacious options targeting the interception or treatment of EAC. Despite molecular advances, molecular targeting of EAC remains elusive, suggesting the need for identifying alternative targets with improved prognostic and therapeutic value. Herein, we performed RNA-sequencing analysis in EAC and Barrett's Esophagus (BE) precursor lesions to identify isoform switching events significantly linked with all-cause and cancer-specific mortality. Patients were stratified based on histopathology alone or in combination with TP53 mutation status, the most commonly mutated gene in EAC. To gain mechanistic insight, we performed isoform-specific siRNA knockdown of two isoforms, TTLL12 and HM13, both linked to patient survival, and investigated mechanisms associated with isoform dysregulation and whether targeting specific isoforms in EAC acts synergistically to improve therapeutic potential. Isoform-specific knockdown of TTLL12 and HM13 significantly decreased the viability of two EAC cell lines, sensitized EAC cell lines to standard-of-care chemotherapy agents (paclitaxel and carboplatin) with synergy, and inhibited EAC cell migratory potential. Knockdown of the TTLL12 isoform led to activation of chaperone-mediated autophagy, which, in turn, decreased expression of CHK1 and TP53; whereas knockdown of the HM13 isoform activated the unfolded protein response and induced endoplasmic reticulum stress-induced autophagy and apoptosis. In addition, HM13 isoform knockdown increased the response to an anti-PD-L1 agent, avelumab, in EAC cells, suggesting a role for isoform switching in immunosuppression. Taken together, study results suggest that isoform switching may provide novel insight for the identification of prognostic markers and inform new potential therapeutic targets for EAC treatment or prevention.

Mark Helpful

Bookmark

Relay

View Full Paper