What question did this study set out to answer?

The study aims to investigate the combined effect of inhibiting SLC6A14 and autophagy/macropinocytosis on pancreatic ductal adenocarcinoma growth.

April 5, 2026

Abstract 7317: Dual targeting of SLC6A14 and autophagy/macropinocytosis enhances therapeutic efficacy in pancreatic ductal adenocarcinoma

Key Points

The study aims to investigate the combined effect of inhibiting SLC6A14 and autophagy/macropinocytosis on pancreatic ductal adenocarcinoma growth.
Utilized genetic deletion and pharmacological blockade of SLC6A14.
Analyzed in vitro assays using MTT and colony formation to assess cell viability.
Conducted in vivo experiments with subcutaneous xenograft models in athymic nude mice.
Administered dual therapy with α-MLT and HCQ to monitor therapeutic efficacy.
Combination treatment significantly reduced cell viability and clonogenic potential compared to monotherapy.
In vivo results showed superior therapeutic outcomes with the combination regimen.
Induction of nutrient stress by α-MLT, counteracted by HCQ, resulted in enhanced tumor attenuation.

Abstract

Abstract PDAC is highly desmoplastic and undergoes metabolic reprogramming to sustain their growth and proliferation. Our laboratory has identified SLC6A14, an amino acid transporter, as a novel drug target for PDAC. Genetic deletion of SLC6A14 or its pharmacological blockade with α-MLT attenuates PDAC growth by inducing amino acid deprivation. However, nutrient stress, particularly amino acid deprivation, can induce nutrient scavenging mechanisms like autophagy and macropinocytosis, thereby undermining the full anticancer potential of SLC6A14 blockade. To address this, the current work was conducted to test if SLC6A14 blockade induces autophagy and/or macropinocytosis and to further investigate if dual inhibition of SLC6A14 (α-MLT) and autophagy/macropinocytosis (HCQ) would yield a better therapeutic outcome in PDAC as opposed to targeting SLC6A14 alone. In vitro assays (MTT and colony formation) revealed that the combination treatment significantly reduced PDAC cell viability and clonogenic potential as opposed to monotherapy. Treatment model subcutaneous xenograft in athymic nude mice demonstrated a superior therapeutic outcome with the combination regimen. Collectively, our study demonstrates that the afore-described combination therapy creates a metabolic trap wherein α-MLT induces nutrient stress, while HCQ prevents autophagic and macropinocytosis compensation, thus culminating in a more potent tumor attenuation. This dual blockade represents a hitherto unexplored treatment strategy for PDAC. Citation Format: Mosharaf Mahmud Syed, Devaraja Rajasekaran, Souad R. Sennoune, Tanima Sharker, Oscar Sanchez, Mary Katherine Jurek, Longfa Kou, Ruijie Chen, Vadivel Ganapathy, Yangzom D. Bhutia. Dual targeting of SLC6A14 and autophagy/macropinocytosis enhances therapeutic efficacy in pancreatic ductal adenocarcinoma abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 7317.

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