Vasopressin Analog [V4Q5]dDAVP Exerts Cooperative Anticancer Effects in Combination With Low-Dose 5-Fluorouracil on Aggressive Colorectal Cancer Models

Natasha T Sobol; Luisina M Solerno; Candela Llavona; Daniel F Alonso; Juan Garona

doi:10.14740/wjon1715

Vasopressin Analog [V⁴Q⁵]dDAVP Exerts Cooperative Anticancer Effects in Combination With Low-Dose 5-Fluorouracil on Aggressive Colorectal Cancer Models

World J Oncol. 2023 Dec;14(6):540-550. doi: 10.14740/wjon1715. Epub 2023 Nov 18.

Authors

Natasha T Sobol^{1

2

3}, Luisina M Solerno^{1

2

3}, Candela Llavona^{1

2}, Daniel F Alonso^{1

2

4}, Juan Garona^{1

2

4}

Affiliations

¹ Center of Molecular and Translational Oncology (COMTra), Unit of Translational Oncology, Science and Technology Department, National University of Quilmes, Buenos Aires, Argentina.
² Center of Translational Medicine, Unit of Biomedical Cancer Research (IBioCAN), Laboratory N° 6, El Cruce "Nestor Kirchner" Hospital, Buenos Aires, Argentina.
³ These authors contributed equally to the study.
⁴ National Council of Scientific and Technical Research (CONICET), Buenos Aires, Argentina.

Abstract

Background: Colorectal cancer (CRC) is a leading cause of cancer-associated mortality worldwide. Despite being an essential component of systemic chemotherapy for advanced CRC, 5-fluorouracil (5-FU) clinical use has severe limitations, such as high toxicity, low selectivity and drug resistance. [V⁴Q⁵]dDAVP (1-deamino-4-valine-5-glutamine-8-D-arginine vasopressin) is a peptide vasopressin analog and a selective agonist of the arginine vasopressin type 2 membrane receptor (AVPR2), expressed in microvascular and tumor tissue. This synthetic compound has well-proven antitumor and antimetastatic activity in different tumor types, including metastatic CRC. The objective of this work was to assess the potential combinational benefits in preclinical CRC models after [V⁴Q⁵]dDAVP addition to 5-FU.

Methods: Effects on cellular viability, cell cycle progression, apoptosis and molecular mechanisms associated to [V⁴Q⁵]dDAVP treatment in combination with 5-FU were evaluated in murine CT-26 and human COLO-205 cell lines. In vivo, impact of dual therapy was explored on CRC tumor growth and metastatic spread.

Results: In CRC cells, [V⁴Q⁵]dDAVP (1 µM) addition to sub-IC₅₀ 5-FU concentrations resulted in the enhancement of cytostatic effects induced by chemotherapy. Reduction of cell viability after combined treatment was associated with cell cycle arrest in the G₀/G₁ phase, induction of apoptosis and increased gene expression of the cyclin-dependent kinase inhibitor p21 (CDKN1A) and the tumor suppressor p53 (TP53) in malignant cells, as assessed by flow cytometry, terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate (dUTP) nick end labeling (TUNEL), and quantitative reverse transcription polymerase chain reaction (qRT-PCR), respectively. In vivo, intravenous administration of [V⁴Q⁵]dDAVP (0.3 µg/kg) in combination with safe low doses of 5-FU (50 or 80 mg/kg for CT-26 or COLO-205 tumor models, respectively) effectively abrogated CRC growth, reducing aggressiveness of primary lesions and increasing survival of tumor-bearing mice. In addition, concomitant administration of [V⁴Q⁵]dDAVP and 5-FU inhibited pulmonary metastasis formation by CT-26 cells in immunocompetent mice, especially reducing macrometastatic disease.

Conclusions: [V⁴Q⁵]dDAVP seems to enhance the efficacy of 5-FU-based chemotherapy in CRC by modulating tumor progression, as well as metastatic dissemination, suggesting its potential role as a safe and cost-effective co-adjuvant agent for the management of advanced CRC.

Keywords: 5-FU; AVPR2; Antimetastatic; Co-adjuvant therapy; Colorectal cancer; [V4Q5]dDAVP.

Grants and funding

This work was supported by the National Agency for the Promotion of Science and Technology (ANPCYT, Argentina, grants No. PICT2017/2056 to DFA and JG, PICT2021/UCTH0005 to Dr. Alejandro Berra and JG, and PICT2021/AI00113 to Dr. Giselle Ripoll and JG), the National Institute of Cancer (INC, Argentina, grant No. INC2018/2021 to DFA and JG), the National Scientific and Technical Research Council (CONICET, Argentina, grant No. PIP11220210100708CO to DFA), and the National University of Quilmes (UNQ, Argentina, grant No. PUNQ1297/19).