Tehran University of Medical Sciences

Science Communicator Platform

Stay connected! Follow us on X network (Twitter):
Share By
Identifying the Potential Mediators of Pathological Complete Response to Neoadjuvant Chemotherapy Among Tacr1 Gene Polymorphisms: A Study on Breast Cancer Patients Publisher Pubmed



Ghorbani M1 ; Namazi S2 ; Dehghani M3 ; Razi F4 ; Khalvati B5, 6 ; Dehshahri A1
Authors

Source: Breast Cancer Research and Treatment Published:2025


Abstract

Purpose: Recent studies have shown that the truncated isoform of the neurokinin-1 receptor (NK-1R) and its ligand, substance P (SP), are overexpressed in tumor cells playing a crucial role in chemoresistance, leading to proliferation, angiogenesis, and metastasis. Hence, this study aims to assess if the polymorphisms of the NK-1R-encoding gene influence the truncated NK-1R level, chemoresistance, and pathological complete response (pCR) achievement in breast cancer patients. Methods: The real-time PCR-HRMA was performed to genotype TACR1 eighteen tag SNPs in 153 neoadjuvant chemotherapy-receiving breast cancer patients. Univariate analysis was performed to assess the association of baseline and tumor characteristics with pCR achievement. The association of each variant and pCR achievement was assessed by executing logistic regression while adjusting for covariates and correcting for multiple tests using permutation. Results: The probability of pCR to neoadjuvant chemotherapy is higher for patients with tumor grade-III as well as stage-I. Assuming the additive, dominant, or recessive models, rs17010664, rs6715729, and rs3771869 were significantly associated with pCR achievement. Conclusion: Positioned close to the truncation-occurring region, belonging to an exon-splicing enhancer motif, the rs17010664 C allele seems to play a crucial role in enhancing the TACR1 last exon splicing leading to increased truncated NK-1R production, chemoresistance, and decreased pCR achievement. Accordingly, The SP/truncated NK-1R axis blockade by NK-1R antagonists seems to be a therapeutic approach to overcoming chemoresistance and achieving pCR in the rs17010664 risk-allele-bearing patients. Hence, conducting further studies to determine the required dose of NK-1R antagonists, repurposed as an antitumor agent, is favored. © The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature 2025.
Related Docs
View other Related Docs
1. Gene Polymorphisms of Tacr1 Serve As the Potential Pharmacogenetic Predictors of Response to the Neurokinin-1 Receptor Antagonist-Based Antiemetic Regimens: A Candidate-Gene Association Study in Breast Cancer Patients, Cancer Chemotherapy and Pharmacology (2024)
2. Inhibition of Tachykinin Nk1receptor Using Aprepitant Induces Apoptotic Cell Death and G1 Arrest Through Akt/P53 Axis in Pre-B Acute Lymphoblastic Leukemia Cells, European Journal of Pharmacology (2016)
3. Evaluation of Pathologic Complete Response (Pcr) to Neoadjuvant Chemotherapy in Iranian Breast Cancer Patients With Estrogen Receptor Positive and Her2 Negative and Impact of Predicting Variables on Pcr, European Journal of Breast Health (2020)
Experts (# of related papers)
View all Related Experts
Massoud Amanlou (3)
Seyed Hamidollah Ghaffari (2)
Other Related Docs
4. Neurokinin-1 Receptor (Nk1r) Inhibition Sensitizes Apl Cells to Anti-Tumor Effect of Arsenic Trioxide Via Restriction of Nf-Κb Axis: Shedding New Light on Resistance to Aprepitant, International Journal of Biochemistry and Cell Biology (2018)
5. Neuropilin-I Expression Is Associated With Lymph Node Metastasis in Breast Cancer Tissues, Cancer Management and Research (2018)
6. Factors Impacting Pathologic Complete Response After Neoadjuvant Chemotherapy in Breast Cancer: A Single-Center Study, International Journal of Cancer Management (2018)
7. Treatment Outcomes and Clinicopathologic Characteristics of Triple-Negative Breast Cancer: A Report From Cancer Institute of Iran, International Journal of Hematology-Oncology and Stem Cell Research (2017)
8. Deletion of Loop Fragment Adjacent to Active Site Diminishes the Stability and Activity of Exo-Inulinase, International Journal of Biological Macromolecules (2016)
9. Introducing a New Model of Sweet Taste Receptor, a Class C G-Protein Coupled Receptor (C Gpcr), Cell Biochemistry and Biophysics (2019)
10. Androgen Receptor Expression on Breast Cancer Cells: A Clinicopathologic and Survival Study, Tehran University Medical Journal (2015)
11. In Silico Analysis of Novel Mutations in Maple Syrup Urine Disease Patients From Iran, Metabolic Brain Disease (2017)
12. Association of Dna Repair Gene Variants With Colorectal Cancer: Risk, Toxicity, and Survival, BMC Cancer (2020)
13. Fut2: Filling the Gap Between Genes and Environment in Behcet's Disease?, Annals of the Rheumatic Diseases (2015)
14. A Novel Mutation in the Pax3 Gene Causes Waardenburg Syndrome Type I in an Iranian Family, International Journal of Pediatric Otorhinolaryngology (2015)
15. Role of Tumor Subtypes in Response to Neoadjuvant Chemotherapy in Non-Metastatic Breast Cancer, Archives of Iranian Medicine (2021)
16. Azoridactase Enzyme Engineering to Induce Structural Changes in the Active Site and Improve Its Affinity for Azo Dyes, Journal of Knowledge and Health in Basic Medical Sciences (2024)
17. Display of B. Pumilus Chitinase on the Surface of B. Subtilis Spore As a Potential Biopesticide, Pesticide Biochemistry and Physiology (2017)
18. The Importance of the Non-Active Site and Non-Periodical Structure Located Histidine Residue Respect to the Structure and Function of Exo-Inulinase, International Journal of Biological Macromolecules (2017)
19. Novel Genetic Structures Associated With Adverse Response to Chemotherapy in Breast Cancer, Journal of Oncology Pharmacy Practice (2024)
20. Virtual Screening Reveals Aprepitant to Be a Potent Inhibitor of Neutral Sphingomyelinase 2: Implications in Blockade of Exosome Release in Cancer Therapy, Journal of Cancer Research and Clinical Oncology (2023)