Your search keyword '"Moon, Yong Wha"' showing total 30 results

1. Targeting PEG10 as a novel therapeutic approach to overcome CDK4/6 inhibitor resistance in breast cancer

Author

Katuwal, Nar Bahadur, Kang, Min Sil, Ghosh, Mithun, Hong, Sa Deok, Jeong, Yeong Gyu, Park, Seong Min, Kim, Seul-Gi, Sohn, Joohyuk, Kim, Tae Hoen, and Moon, Yong Wha

Published

2023

2. First-in-human study of IM156, a novel potent biguanide oxidative phosphorylation (OXPHOS) inhibitor, in patients with advanced solid tumors

Author

Janku, Filip, Beom, Seung-Hoon, Moon, Yong Wha, Kim, Tae Won, Shin, Young G., Yim, Dong-Seok, Kim, Gun Min, Kim, Hyo Song, Kim, Sun Young, Cheong, Jae-Ho, Lee, Young Woo, Geiger, Barb, Yoo, Sanghee, Thurston, Archie, Welsch, Dean, Rudoltz, Marc S., and Rha, Sun Young

Published

2022

3. Trastuzumab-Mediated Antibody-Dependent Cell-Mediated Cytotoxicity (ADCC) Enhances Natural Killer Cell Cytotoxicity in HER2-Overexpressing Ovarian Cancer.

Author

Hong, Sa Deok, Katuwal, Nar Bahadur, Kang, Min Sil, Ghosh, Mithun, Park, Seong Min, Kim, Tae Hoen, Baek, Young Seok, Lee, Seung Ryeol, and Moon, Yong Wha

Subjects

ANTIBODY-dependent cell cytotoxicity, KILLER cells, EPIDERMAL growth factor, OVARIAN cancer, GYNECOLOGIC cancer

Abstract

Ovarian cancer is the deadliest gynecologic cancer. Although human epidermal growth factor receptor-2 (HER2) overexpression, a poor prognostic molecular marker in ovarian cancer, is found in almost 30% of ovarian cancer cases, there are no established therapies for HER2-overexpressing ovarian cancer. In this study, we investigated the efficacy of combined samfenet, a biosimilar compound of trastuzumab, and natural killer (NK) cells in preclinical model of HER2-overexpressing ovarian cancer. Firstly, we screened the HER2 expression in three ovarian cancer cell lines and eight ovarian cancer patient-derived tumor xenograft (PDTX) samples. Then, immunohistochemistry and silver in situ hybridization (SISH) were performed following clinical criteria. HER2-overexpressing cells exhibited the highest sensitivity to samfenet compared with low-HER2-expressing cells. In addition, the combination of samfenet with natural killer (NK) cells resulted in significantly enhanced sensitivity to HER2-overexpressing cells and showed a significant antitumor effect on PDTX mice compared with monotherapy. It is known that anti-HER2-humanized IgG1 monoclonal antibodies, including trastuzumab, induce antibody-dependent cellular cytotoxicity (ADCC). Consequently, the combination of samfenet with NK cells demonstrated NK cell-mediated ADCC, as confirmed using an in vitro NK cytotoxicity assay and in vivo antitumor efficacy. A transferase dUTP nick end labeling (TUNEL) assay using xenografted tumors further supported the ADCC effects based on the increase in the number of apoptotic cells in the combination group. Furthermore, high HER2 expression was associated with shorter progression-free survival and overall survival based on public mRNA expression data. In this study, we demonstrated that the combination of samfenet and NK cell therapy could be a promising treatment strategy for patients with HER2-overexpressing ovarian cancer, through ADCC effects. Therefore, this study supports a rationale for further clinical studies of the combination of samfenet and NK cells as a therapy for patients with HER2-overexpressing ovarian cancer. [ABSTRACT FROM AUTHOR]

Published

2024

4. A randomized, multicenter, open-label, phase III trial comparing anthracyclines followed by taxane versus anthracyclines followed by taxane plus carboplatin as (neo) adjuvant therapy in patients with early triple-negative breast cancer: Korean Cancer...

Author

Sohn, Joohyuk, Kim, Gun Min, Jung, Kyung Hae, Jeung, Hei-Cheul, Lee, Jieun, Lee, Keun Seok, Im, Seock-Ah, Kang, Seok Yun, Kim, Se Hyun, Kim, Han Jo, Park, Kyong Hwa, Chae, Yee Soo, Koh, Su-Jin, Cho, Eun Kyung, Park, Keon Uk, Lee, Sung Sook, Kim, Ji-Yeon, Choi, In Sil, Baek, Sun Kyung, and Moon, Yong Wha

Published

2024

5. Combined PI3K Inhibitor and Eribulin Enhances Anti-Tumor Activity in Preclinical Models of Paclitaxel-Resistant, PIK3CA-Mutated Endometrial Cancer

Author

Jeong, Yeong Gyu, primary, Katuwal, Nar Bahadur, additional, Kang, Min Sil, additional, Ghosh, Mithun, additional, Hong, Sa Deok, additional, Park, Seong Min, additional, Kim, Seul-Gi, additional, Kim, Tae Hoen, additional, and Moon, Yong Wha, additional

Published

2023

6. PSPC1 Inhibition Synergizes with Poly(ADP-ribose) Polymerase Inhibitors in a Preclinical Model of BRCA-Mutated Breast/Ovarian Cancer.

Author

Ghosh, Mithun, Kang, Min Sil, Katuwal, Nar Bahadur, Hong, Sa Deok, Jeong, Yeong Gyu, Park, Seong Min, Kim, Seul-Gi, and Moon, Yong Wha

Subjects

POLY ADP ribose, BREAST, DNA repair, OVARIAN cancer, ANIMAL models in research, DOUBLE-strand DNA breaks, SMALL interfering RNA

Abstract

Poly (ADP-ribose) polymerase (PARP) inhibitors are effective against BRCA1/2-mutated cancers through synthetic lethality. Unfortunately, most cases ultimately develop acquired resistance. Therefore, enhancing PARP inhibitor sensitivity and preventing resistance in those cells are an unmet clinical need. Here, we investigated the ability of paraspeckle component 1 (PSPC1), as an additional synthetic lethal partner with BRCA1/2, to enhance olaparib sensitivity in preclinical models of BRCA1/2-mutated breast and ovarian cancers. In vitro, the combined olaparib and PSPC1 small interfering RNA (siRNA) exhibited synergistic anti-proliferative activity in BRCA1/2-mutated breast and ovarian cancer cells. The combination therapy also demonstrated synergistic tumor inhibition in a xenograft mouse model. Mechanistically, olaparib monotherapy increased the expressions of p-ATM and DNA-PKcs, suggesting the activation of a DNA repair pathway, whereas combining PSPC1 siRNA with olaparib decreased the expressions of p-ATM and DNA-PKcs again. As such, the combination increased the formation of γH2AX foci, indicating stronger DNA double-strand breaks. Subsequently, these DNA-damaged cells escaped G2/M checkpoint activation, as indicated by the suppression of p-cdc25C (Ser216) and p-cdc2 (Tyr15) after combination treatment. Finally, these cells entered mitosis, which induced increased apoptosis. Thus, this proves that PSPC1 inhibition enhances olaparib sensitivity by targeting DNA damage response in our preclinical model. The combination of olaparib and PSPC1 inhibition merits further clinical investigation to enhance PARP inhibitor efficacy. [ABSTRACT FROM AUTHOR]

Published

2023

7. Abstract 4485: JPI-547, a novel dual inhibitor of PARP 1/2 and tankyrase 1/2 overcomes olaparib resistance in BRCA 1/2 mutant ovary and breast cancer preclinical model

Author

Kang, Min Sil, primary, Katuwal, Nar, additional, Ghosh, Mithun, additional, Jeong, Young kyu, additional, deok Hong, Sa, additional, Park, Sung Min, additional, Kim, John, additional, Cha, Hyunju, additional, Cheon, Banyoon, additional, Kim, Seul-Gi, additional, and Moon, Yong Wha, additional

Published

2023

8. Supplementary Figure 3A from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

9. Supplementary Figure S3. Treatment of EGFR ligands in BRAF V600E mutnat A375 melanoma cell line. from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

10. Supplementary Table 1 from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

11. Supplementary Figure 2 from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

12. Data from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

13. Supplementary Table 2 from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

14. Supplementary Figure S1. Combination of GSK2118436 and a c-MET inhibitor, SU11274, did not restore sensitivity to GSK2118436. from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

15. Supplementary Figure S2. Autocrine HB-EGF-EGFR signaling mediates resistance to GSK2118436 in MV522 and HCC364 cells. from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

16. Supplementary Figure S4. Overexpression of RIP2 wild type or RIP2 (S176E) induces the resistance to GSK2118436 in MV522 cells. from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

17. Supplementary Figure 1 from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

18. Supplementary Table from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

19. Supplementary Figure S5. HB-EGF was selectively decreased in GSR (pool) cells with RIP2 siRNA. from EGFR-Mediated Reactivation of MAPK Signaling Induces Acquired Resistance to GSK2118436 in BRAF V600E–Mutant NSCLC Cell Lines

Author

Kim, Sung-Moo, primary, Kim, Hwan, primary, Jang, Kang Won, primary, Kim, Min Hwan, primary, Sohn, Jinyoung, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kang, Chan Woo, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Kim, Joo Hang, primary, Paik, Soonmyung, primary, and Cho, Byoung Chul, primary

Published

2023

20. Supplementary Figure 3B and C from Antitumor Activity and Acquired Resistance Mechanism of Dovitinib (TKI258) in RET-Rearranged Lung Adenocarcinoma

Author

Kang, Chan Woo, primary, Jang, Kang Won, primary, Sohn, Jinyoung, primary, Kim, Sung-Moo, primary, Pyo, Kyoung-Ho, primary, Kim, Hwan, primary, Yun, Mi Ran, primary, Kang, Han Na, primary, Kim, Hye Ryun, primary, Lim, Sun Min, primary, Moon, Yong Wha, primary, Paik, Soonmyung, primary, Kim, Dae Joon, primary, Kim, Joo Hang, primary, and Cho, Byoung Chul, primary

Published

2023

21. Abstract P2-26-09: Synergistic activity of PI3K inhibitor in combination with AZD6738, ATR inhibitor in breast cancer preclinical model via DNA damage response pathway

Author

Moon, Yong Wha, primary, Gosh, Mithun, additional, Park, Nahee, additional, Pandey, Kamal, additional, Katwal, Nar Bahadur, additional, and Hong, Sa Deok, additional

Published

2023

22. Abstract P5-14-04: Genomic characterization of hormone receptor-positive advanced breast cancer with high tumor mutational burden: fresh-frozen tissue genomic analysis from MUTATION-1 study (KCSG BR17-04)

Author

Kim, Min Hwan, primary, Yang, Yohan, additional, Kim, Eunyoung, additional, Moon, Yong Wha, additional, Kim, Gun Min, additional, Kim, Seul-Gi, additional, Chae, Yee Soo, additional, Lee, Jieun, additional, Jeong, Jae Ho, additional, Lee, Kyung-Hun, additional, Kim, Han Jo, additional, Jung, Joo Young, additional, Koh, Su-Jin, additional, Lee, Kyoung Eun, additional, Kim, Hee-Jun, additional, Park, Kyong Hwa, additional, Lim, Seungtaek, additional, Park, Yeon Hee, additional, Kim, Sangwoo, additional, and Sohn, Joo Hyuk, additional

Published

2023

23. Eflapegrastim Versus Pegfilgrastim for Chemotherapy-Induced Neutropenia in Korean and Asian Patients with Early Breast Cancer: Results from the Two Phase III ADVANCE and RECOVER Studies

Author

Moon, Yong Wha, primary, Kim, Seung Ki, additional, Lee, Keun Seok, additional, Lee, Moon Hee, additional, Park, Yeon Hee, additional, Park, Kyong Hwa, additional, Kim, Gun Min, additional, Lim, Seungtaek, additional, Lee, Seung Ah, additional, Choi, Jae Duk, additional, Baek, Eunhye, additional, Han, Hyesun, additional, Baek, Seung Jae, additional, and Im, Seock-Ah, additional

Published

2023

24. Preclinical Platform Using a Triple-negative Breast Cancer Syngeneic Murine Model to Evaluate Immune Checkpoint Inhibitors

Author

KATUWAL, NAR BAHADUR, primary, PARK, NAHEE, additional, PANDEY, KAMAL, additional, KANG, MIN SIL, additional, HONG, SA DEOK, additional, GHOSH, MITHUN, additional, KIM, SEUL-GI, additional, CHO, YOUNG BIN, additional, HUR, JIN, additional, KIM, SEUNG KI, additional, and MOON, YONG WHA, additional

Published

2022

25. : A case report of re-challenge of immune checkpoint inhibitors after immune-related neurological adverse events: Review of literature

Author

Moon, Heesung, primary, Kim, Seul-Gi, additional, Kim, Seung Ki, additional, Kim, Jinkwon, additional, Lee, Seung Ryeol, additional, and Moon, Yong Wha, additional

Published

2022

26. Preclinical platform using a triple-negative breast cancer syngeneic murine model to evaluate immune checkpoint inhibitors

Author

Bahadur, Nar Bahadur, primary, Park, Nahee, additional, Pandey, Kamal, additional, Bahadur, Katuwal Nar, additional, Kang, Min Sil, additional, Hong, Sa Deok, additional, Ghosh, Mithun, additional, Kim, Seul-Gi, additional, Cho, Young Bin, additional, Hur, Jin, additional, Kim, Seung Ki, additional, and Moon, Yong Wha, additional

Published

2022

27. Abstract P1-19-03: Phase II trial of durvalumab and tremelimumab in the hormone receptor-positive metastatic breast cancer with high tumor mutational burden selected by whole exome sequencing: Korean cancer study group trial (KCSG BR17-04)

Author

Moon, Yong Wha, primary, Kim, Eunyoung, additional, Kim, Min Hwan, additional, Kim, Gun Min, additional, Kim, Seul-Gi, additional, Chae, YeeSoo, additional, Lee, Jieun, additional, Jeong, Jae Ho, additional, Lee, Kyung-Hun, additional, Kim, Han Jo, additional, Jung, Joo Young, additional, Koh, Su-Jin, additional, Lee, Kyoung Eun, additional, Kim, Hee-Jun, additional, Park, Kyong Hwa, additional, Lim, Seungtaek, additional, Park, Yeon Hee, additional, Kim, Tae Hoen, additional, Kim, Sewha, additional, Yang, Yohan, additional, Kim, Sangwoo, additional, and Sohn, Joohyuk, additional

Published

2022

28. Combination of Abemaciclib following Eribulin Overcomes Palbociclib-Resistant Breast Cancer by Inhibiting the G2/M Cell Cycle Phase

Author

Pandey, Kamal, primary, Katuwal, Nar Bahadur, additional, Park, Nahee, additional, Hur, Jin, additional, Cho, Young Bin, additional, Kim, Seung Ki, additional, Lee, Seung Ah, additional, Kim, Isaac, additional, Lee, Seung-Ryeol, additional, and Moon, Yong Wha, additional

Published

2022

29. A randomized phase II clinical trial of talazoparib maintenance therapy in patients with triple-negative breast cancer who showed platinum-sensitivity on first- or second-line platinum-based chemotherapy: KCSG BR21-10.

Author

Sohn, Joohyuk, Kim, Min Hwan, Kim, Gun Min, Kim, Jee Hung, Kim, Han Jo, LEE, JIEUN, Moon, Yong Wha, Ahn, Hee Kyung, Kim, Hee Jun, Shin, Seong-Hoon, Lee, Moon Hee, Lee, Kyoung Eun, Won, Hye Sung, Kang, Seok Yun, Lee, Keun Seok, and Park, Kyong Hwa

Published

2023

30. Preclinical Platform Using a Triple-negative Breast Cancer Syngeneic Murine Model to Evaluate Immune Checkpoint Inhibitors.

Author

Katuwal NB, Park N, Pandey K, Kang MS, Hong SD, Ghosh M, Kim SG, Cho YB, Hur J, Kim SK, and Moon YW

Subjects

Humans, Female, Animals, Mice, Disease Models, Animal, Biomarkers, Cytokines therapeutic use, Immune Checkpoint Inhibitors pharmacology, Immune Checkpoint Inhibitors therapeutic use, Triple Negative Breast Neoplasms pathology

Abstract

Background/aim: To evaluate the feasibility of syngeneic mouse models of breast cancer by analyzing the efficacy of immune checkpoint inhibitors (ICIs) and potential predictive biomarkers., Materials and Methods: To establish the murine triple-negative breast cancer (TNBC) models, JC, 4T1, EMT6, and E0771 cells were subcutaneously implanted into female syngeneic mice. When the tumor reached 50-100 mm 3 , each mouse model was divided into a treatment (using a murine PD-1 antibody) and a no-treatment control group. The treatment group was further divided into the responder and non-responder groups. Potential predictive biomarkers were evaluated by analyzing serum cytokines, peripheral blood T cells and tumor infiltrating immune cells., Results: The EMT6 model showed the highest tumor response rate (54%, 6/11) of the syngeneic models: 4T1 (45%, 5/11), JC (40%, 4/10), or E0771 (23%, 3/13). Early changes in tumor size at 7 days post-PD-1 inhibitor treatment predicted the final efficacy of the PD-1 inhibitor. Peripheral blood CD8+ and CD4+ T cells with or without Ki67 expression at 7 days post-PD-1 inhibitor treatment were higher in the finally designated responder group than in the non-responder group. At the time of sacrifice, analyses of tumor infiltrating lymphocytes consistently supported these results. We also demonstrated that retro-orbital blood sampling procedures (baseline, 7 days post-treatment, time of sacrifice) were safe for serum cytokine analyses, suggesting that our preclinical platform may be used for biomarker research using serum cytokines., Conclusion: Our syngeneic mouse model of TNBC is a feasible preclinical platform to evaluate ICI efficacy combined with other drugs and predictive biomarkers in the screening process of immune-oncology drug development., (Copyright © 2023 International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published

2023