Your search keyword '"Kyi, Chrisann"' showing total 3 results

1. A shared neoantigen vaccine combined with immune checkpoint blockade for advanced metastatic solid tumors: phase 1 trial interim results

Author

Rappaport, Amy R., Kyi, Chrisann, Lane, Monica, Hart, Meghan G., Johnson, Melissa L., Henick, Brian S., Liao, Chih-Yi, Mahipal, Amit, Shergill, Ardaman, Spira, Alexander I., Goldman, Jonathan W., Scallan, Ciaran D., Schenk, Desiree, Palmer, Christine D., Davis, Matthew J., Kounlavouth, Sonia, Kemp, Lindsey, Yang, Aaron, Li, Yaojun John, Likes, Molly, Shen, Annie, Boucher, Gregory R., Egorova, Milana, Veres, Robert L., Espinosa, J. Aaron, Jaroslavsky, Jason R., Kraemer Tardif, Lauren D., Acrebuche, Lindsey, Puccia, Christopher, Sousa, Leiliane, Zhou, Rita, Bae, Kyounghwa, Hecht, J. Randolph, Carbone, David P., Johnson, Benny, Allen, Andrew, Ferguson, Andrew R., and Jooss, Karin

Abstract

Therapeutic vaccines that elicit cytotoxic T cell responses targeting tumor-specific neoantigens hold promise for providing long-term clinical benefit to patients with cancer. Here we evaluated safety and tolerability of a therapeutic vaccine encoding 20 shared neoantigens derived from selected common oncogenic driver mutations as primary endpoints in an ongoing phase 1/2 study in patients with advanced/metastatic solid tumors. Secondary endpoints included immunogenicity, overall response rate, progression-free survival and overall survival. Eligible patients were selected if their tumors expressed one of the human leukocyte antigen-matched tumor mutations included in the vaccine, with the majority of patients (18/19) harboring a mutation in KRAS. The vaccine regimen, consisting of a chimp adenovirus (ChAd68) and self-amplifying mRNA (samRNA) in combination with the immune checkpoint inhibitors ipilimumab and nivolumab, was shown to be well tolerated, with observed treatment-related adverse events consistent with acute inflammation expected with viral vector-based vaccines and immune checkpoint blockade, the majority grade 1/2. Two patients experienced grade 3/4 serious treatment-related adverse events that were also dose-limiting toxicities. The overall response rate was 0%, and median progression-free survival and overall survival were 1.9 months and 7.9 months, respectively. T cell responses were biased toward human leukocyte antigen-matched TP53 neoantigens encoded in the vaccine relative to KRAS neoantigens expressed by the patients’ tumors, indicating a previously unknown hierarchy of neoantigen immunodominance that may impact the therapeutic efficacy of multiepitope shared neoantigen vaccines. These data led to the development of an optimized vaccine exclusively targeting KRAS-derived neoantigens that is being evaluated in a subset of patients in phase 2 of the clinical study. ClinicalTrials.gov registration: NCT03953235.

Published

2024

2. Nivolumab for mismatch-repair-deficient or hypermutated gynecologic cancers: a phase 2 trial with biomarker analyses

Author

Friedman, Claire F., Manning-Geist, Beryl L., Zhou, Qin, Soumerai, Tara, Holland, Aliya, Da Cruz Paula, Arnaud, Green, Hunter, Ozsoy, Melih Arda, Iasonos, Alexia, Hollmann, Travis, Leitao, Mario M., Mueller, Jennifer J., Makker, Vicky, Tew, William P., O’Cearbhaill, Roisin E., Liu, Ying L., Rubinstein, Maria M., Troso-Sandoval, Tiffany, Lichtman, Stuart M., Schram, Alison, Kyi, Chrisann, Grisham, Rachel N., Causa Andrieu, Pamela, Wherry, E. John, Aghajanian, Carol, Weigelt, Britta, Hensley, Martee L., and Zamarin, Dmitriy

Abstract

Programmed death-1 (PD-1) inhibitors are approved for therapy of gynecologic cancers with DNA mismatch repair deficiency (dMMR), although predictors of response remain elusive. We conducted a single-arm phase 2 study of nivolumab in 35 patients with dMMR uterine or ovarian cancers. Co-primary endpoints included objective response rate (ORR) and progression-free survival at 24 weeks (PFS24). Secondary endpoints included overall survival (OS), disease control rate (DCR), duration of response (DOR) and safety. Exploratory endpoints included biomarkers and molecular correlates of response. The ORR was 58.8% (97.5% confidence interval (CI): 40.7–100%), and the PFS24 rate was 64.7% (97.5% one-sided CI: 46.5–100%), meeting the pre-specified endpoints. The DCR was 73.5% (95% CI: 55.6–87.1%). At the median follow-up of 42.1 months (range, 8.9–59.8 months), median OS was not reached. One-year OS rate was 79% (95% CI: 60.9–89.4%). Thirty-two patients (91%) had a treatment-related adverse event (TRAE), including arthralgia (n= 10, 29%), fatigue (n= 10, 29%), pain (n= 10, 29%) and pruritis (n= 10, 29%); most were grade 1 or grade 2. Ten patients (29%) reported a grade 3 or grade 4 TRAE; no grade 5 events occurred. Exploratory analyses show that the presence of dysfunctional (CD8+PD-1+) or terminally dysfunctional (CD8+PD-1+TOX+) T cells and their interaction with programmed death ligand-1 (PD-L1)+cells were independently associated with PFS24. PFS24 was associated with presence of MEGF8or SETD1Bsomatic mutations. This trial met its co-primary endpoints (ORR and PFS24) early, and our findings highlight several genetic and tumor microenvironment parameters associated with response to PD-1 blockade in dMMR cancers, generating rationale for their validation in larger cohorts.

Published

2024

3. Mitogen-Activated Protein Kinase (MAPK) Driven Rare Gynecologic Cancers and Evolving Therapeutic Targets

Author

Grisham, Rachel N., Praiss, Aaron, Kyi, Chrisann, and Park, Kay J.

Abstract

The MAPK cascade is a critical pathway involved in cancer cell survival as well as resistance to drug therapy. Phosphorylation of ERK1 and ERK2, the final effectors of the MAPK pathway, results in activation of multiple substrates that are responsible for cellular proliferation, differentiation, survival and migration[1]. Many oncogenic driver mutations have been identified in genes upstream of MAPK/ERK, including mutations in KRASand V600EBRAF,which can lead to overactivation of the MAPK/ERK pathway. This signaling cascade, particularly its intracellular components, RAF and MEK, have been a major focus for drug discovery efforts during the past decade, and small molecule inhibitors of both RAF and MEK have progressed to clinical evaluations and registration in multiple cancers[2].

Published

2023