Abstract
Evasion of apoptosis is a hallmark of cancer, which is frequently mediated by upregulation of the antiapoptotic BCL-2 family proteins. In colorectal cancer (CRC), previous work has highlighted differential antiapoptotic protein dependencies determined by the stage of the disease. While intestinal stem cells (ISCs) require BCL-2 for adenoma outgrowth and survival during transformation, ISC-specific MCL1 deletion results in disturbed intestinal homeostasis, eventually contributing to tumorigenesis. Colon cancer stem cells (CSCs), however, no longer require BCL-2 and depend mainly on BCL-XL for their survival. We therefore hypothesized that a shift in antiapoptotic protein reliance occurs in ISCs as the disease progresses from normal to adenoma to carcinoma. By targeting antiapoptotic proteins with specific BH3 mimetics in organoid models of CRC progression, we found that BCL-2 is essential only during ISC transformation while MCL1 inhibition did not affect adenoma outgrowth. BCL-XL, on the other hand, was crucial for stem cell survival throughout the adenoma-to-carcinoma sequence. Furthermore, we identified that the limited window of BCL-2 reliance is a result of its downregulation by miR-17-5p, a microRNA that is upregulated upon APC-mutation driven transformation. Here we show that BCL-XL inhibition effectively impairs adenoma outgrowth in vivo and enhances the efficacy of chemotherapy. In line with this dependency, expression of BCL-XL, but not BCL-2 or MCL1, directly correlated to the outcome of chemotherapy-treated CRC patients. Our results provide insights to enable the rational use of BH3 mimetics in CRC management, particularly underlining the therapeutic potential of BCL-XL targeting mimetics in both early and late-stage disease.
Highlights
Intestinal homeostasis is tightly regulated by a balance between proliferation and apoptosis, with intestinal stem cells (ISCs) at the bottom of the crypt driving regeneration [1]
By employing these powerful tools, we show that while B-cell lymphoma-2 (BCL-2) is only essential during ISC transformation, BCL-XL is critical for ISC survival throughout colorectal cancer (CRC) progression
We find that AZD5991 treatment does not impair ISC transformation in our models, even though MCL1 deletion was shown to severely disrupt intestinal homeostasis [18]
Summary
Intestinal homeostasis is tightly regulated by a balance between proliferation and apoptosis, with intestinal stem cells (ISCs) at the bottom of the crypt driving regeneration [1]. Disruption of this balance is an integral step in colorectal cancer (CRC) initiation and progression. Tumor cells frequently deregulate BCL-2 family proteins as a mechanism of survival and resistance [5,6,7]. While BCL-2 is required for apoptosis resistance in several hematological malignancies, amplification of MCL-1 and BCL-XL by chromosomal gain is a frequent alteration especially in solid tumors, making them promising targets for therapy [7]. Inhibiting antiapoptotic proteins with so-called BH3 mimetics holds great promise for anticancer therapy, heralded by the remarkable results obtained with FDA-approved BCL-2 inhibitor Venetoclax (ABT-199), in blood cancers [8]
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