Targeting chemoresistant colorectal cancer via systemic administration of a BMP7 variant

被引:28
|
作者
Veschi, Veronica [1 ]
Mangiapane, Laura R. [1 ]
Nicotra, Annalisa [1 ]
Di Franco, Simone [1 ]
Scavo, Emanuela [1 ]
Apuzzo, Tiziana [1 ]
Sardina, Davide S. [1 ]
Fiori, Micol [2 ]
Benfante, Antonina [1 ]
Colorito, Maria L. [1 ]
Cocorullo, Gianfranco [1 ]
Giuliante, Felice [3 ,4 ]
Cipolla, Calogero [1 ]
Pistone, Giuseppe [5 ]
Bongiorno, Maria Rita [5 ]
Rizzo, Aroldo [6 ]
Tate, Courtney M. [7 ]
Wu, Xiaohua [7 ]
Rowlinson, Scott [7 ]
Stancato, Louis F. [7 ]
Todaro, Matilde [5 ]
De Maria, Ruggero [3 ,4 ]
Stassi, Giorgio [1 ]
机构
[1] Univ Palermo, Dept Surg Oncol & Stomatol Sci DICHIRONS, I-90127 Palermo, Italy
[2] Ist Super Sanita, Dept Oncol & Mol Med, Rome, Italy
[3] Univ Cattolica Sacro Cuore, Ist Patol Gen, I-00168 Rome, Italy
[4] Fdn Policlin Univ A Gemelli, IRCCS, I-00168 Rome, Italy
[5] Univ Palermo, Dept Hlth Promot Sci Internal Med & Med Specialti, I-90127 Palermo, Italy
[6] Osped Riuniti Villa Sofia Cervello, Pathol Unit, Palermo, Italy
[7] Lilly Corp Ctr, Lilly Res Labs, Indianapolis, IN 46285 USA
关键词
BONE MORPHOGENETIC PROTEIN; EPITHELIAL-MESENCHYMAL TRANSITION; CONSENSUS MOLECULAR SUBTYPES; STEM-CELLS; COLON-CANCER; MICROSATELLITE-INSTABILITY; EXPRESSION PATTERNS; JUVENILE POLYPOSIS; TGF-BETA; DIFFERENTIATION;
D O I
10.1038/s41388-019-1047-4
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Despite intense research and clinical efforts, patients affected by advanced colorectal cancer (CRC) have still a poor prognosis. The discovery of colorectal (CR) cancer stem cell (CSC) as the cell compartment responsible for tumor initiation and propagation may provide new opportunities for the development of new therapeutic strategies. Given the reduced sensitivity of CR-CSCs to chemotherapy and the ability of bone morphogenetic proteins (BMP) to promote colonic stem cell differentiation, we aimed to investigate whether an enhanced variant of BMP7 (BMP7v) could sensitize to chemotherapy-resistant CRC cells and tumors. Thirty-five primary human cultures enriched in CR-CSCs, including four from chemoresistant metastatic lesions, were used for in vitro studies and to generate CR-CSC-based mouse avatars to evaluate tumor growth and progression upon treatment with BMP7v alone or in combination with standard therapy or PI3K inhibitors. BMP7v treatment promotes CR-CSC differentiation and recapitulates the cell differentiation-related gene expression profile by suppressing Wnt pathway activity and reducing mesenchymal traits and survival of CR-CSCs. Moreover, in CR-CSC-based mouse avatars, BMP7v exerts an antiangiogenic effect and sensitizes tumor cells to standard chemotherapy regardless of the mutational, MSI, and CMS profiles. Of note, tumor harboring PIK3CA mutations were affected to a lower extent by the combination of BMP7v and chemotherapy. However, the addition of a PI3K inhibitor to the BMP7v-based combination potentiates PIK3CA-mutant tumor drug response and reduces the metastatic lesion size. These data suggest that BMP7v treatment may represent a useful antiangiogenic and prodifferentiation agent, which renders CSCs sensitive to both standard and targeted therapies.
引用
收藏
页码:987 / 1003
页数:17
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