Your search keyword '"Peer, Cody"' showing total 15 results

1. PARP inhibitors: A review of the pharmacology, pharmacokinetics, and pharmacogenetics

Author

Zeng, Yi, Arisa, Oluwatobi, Peer, Cody J., Fojo, Antonio, and Figg, William D.

Published

2024

2. Colesevelam for Lenalidomide Associated Diarrhea in Patients with Multiple Myeloma

Author

Hultcrantz, Malin, primary, Hassoun, Hani, additional, Korde, Neha, additional, Maclachlan, Kylee, additional, Mailankody, Sham, additional, Patel, Dhwani, additional, Shah, Urvi, additional, Tan, Carlyn Rose, additional, Chung, David, additional, Landau, Heather, additional, Scordo, Michael, additional, Shah, Gunjan, additional, Giralt, Sergio, additional, Lahoud, Oscar, additional, Pianko, Matthew, additional, Burge, Mirande, additional, Barnett, Kelly, additional, Shekarkhand, Tala, additional, Caple, Julia, additional, Blaslov, Jenna, additional, Tran, Linh, additional, Salcedo, Meghan, additional, Hamid, Selena, additional, Nemirovsky, David, additional, Derkach, Andriy, additional, Arisa, Oluwatobi, additional, Peer, Cody, additional, Figg, William, additional, Usmani, Saad, additional, Landgren, Ola, additional, and Lesokhin, Alexander, additional

Published

2024

3. Pharmacokinetics (PK) and pharmacogenomics (PGx) of ribociclib (ribo) in Black patients with metastatic breast cancer (mBC): The LEANORA study.

Author

Smith, Donald, primary, Schlam, Ilana, additional, Peer, Cody, additional, Sissung, Tristan, additional, Schmidt, Keith Thomas, additional, Tan, Ming Tony, additional, Chitalia, Ami, additional, Bishopric, Nanette H., additional, Steinberg, Seth M., additional, Choo-Wosoba, Hyoyoung, additional, Gallagher, Christopher, additional, Ashai, Nadia, additional, Whitaker, Kristen Danielle, additional, Mainor, Candace Bavette, additional, Tiwari, Shruti Rakesh, additional, Swanson, Nicole, additional, Malloy, Stacy K, additional, Isaacs, Claudine, additional, Figg, William Douglas, additional, and Swain, Sandra M., additional

Published

2024

4. Treatment with novel topoisomerase inhibitors in Ewing sarcoma models reveals heterogeneity of tumor response.

Author

Lee, Unsun, Szabova, Ludmila, Collins, Victor J., Gordon, Melanie, Johnson, Kristine, Householder, Deborah, Jorgensen, Stephanie, Lu, Lucy, Bassel, Laura, Elloumi, Fathi, Peer, Cody J., Nelson, Ariana E., Varriano, Sophia, Varma, Sudhir, Roberts, Ryan D., Ohler, Zoe Weaver, Figg, William D., Sharan, Shyam K., Pommier, Yves, and Heske, Christine M.

Subjects

EWING'S sarcoma, WHOLE genome sequencing, DNA topoisomerase I, INHIBITION of cellular proliferation, RNA sequencing

Abstract

Introduction: The topoisomerase 1 (TOP1) inhibitor irinotecan is a standard-of-care agent for relapsed Ewing sarcoma (EWS), but its efficacy is limited by chemical instability, rapid clearance and reversibility, and dose-limiting toxicities, such as diarrhea. Indenoisoquinolines (IIQs) represent a new class of clinical TOP1 inhibitors designed to address these limitations. Methods: In this study, we evaluated the preclinical efficacy of three IIQs (LMP400, LMP744, and LMP776) in relevant models of EWS. We characterized the pharmacokinetics of IIQs in orthotopic xenograft models of EWS, optimized the dosing regimen through tolerability studies, and tested the efficacy of IIQs in a panel of six molecularly heterogeneous EWS patient-derived xenograft (PDX) models. For each PDX, we conducted whole genome and RNA sequencing, and methylation analysis. Results: We show that IIQs potently inhibit the proliferation of EWS cells in vitro, inducing complete cell growth inhibition at nanomolar concentrations via induction of DNA damage and apoptotic cell death. LMP400 treatment induced ≥30% tumor regression in two of six PDX models, with more durable regression compared to irinotecan treatment in one of these models. RNA sequencing of PDX models identified a candidate predictive biomarker gene signature for LMP400 response. These data, along with pharmacogenomic data on IIQs in sarcoma cell lines, are available at a new interactive public website: https://discover.nci.nih.gov/rsconnect/EwingSarcomaMinerCDB/. Discussion: Our findings suggest that IIQs may be promising new agents for a subset of EWS patients. [ABSTRACT FROM AUTHOR]

Published

2024

5. Pharmacokinetics and pharmacogenomics of ribociclib in black patients with metastatic breast cancer the LEANORA study.

Author

Schlam, Ilana, Smith, D. Max, Peer, Cody, Sissung, Tristan, Schmidt, Keith T., Tan, Ming, Chitalia, Ami, Bishopric, Nanette H., Steinberg, Seth, Choo-Wosoba, Hyoyoung, Napoli, Giulia, Gallagher, Christopher, Ashai, Nadia, Whitaker, Kristen, Mainor, Candace, Tiwari, Shruti, Swanson, Nicole, Malloy, Stacy, Isaacs, Claudine, and Figg, William Douglas

Published

2024

6. Distinct uptake and elimination profiles for trastuzumab, human IgG, and biocytin-TMR in experimental HER2+ brain metastases of breast cancer.

Author

Silvestri, Vanesa L, Tran, Andy D, Chung, Monika, Chung, Natalie, Gril, Brunilde, Robinson, Christina, Difilippantonio, Simone, Wei, Debbie, Kruhlak, Michael J, Peer, Cody J, Figg, W Douglas, Khan, Imran, and Steeg, Patricia S

Published

2024

7. Pharmacogenomic Variation May Impact Cyclophosphamide Metabolism and Graft Status after HCT for Sickle Cell Disease

Author

Zeng, Yi, primary, Arisa, Oluwatobi, additional, Peer, Cody J., additional, Sissung, Tristan, additional, Figg, William Douglas, additional, Fitzhugh, Courtney D., additional, and Limerick, Emily, additional

Published

2024

8. Tofacitinib to prevent anti-drug antibody formation against LMB-100 immunotoxin in patients with advanced mesothelin-expressing cancers.

Author

Skorupan, Nebojsa, Peer, Cody J., Xianyu Zhang, Hyoyoung Choo-Wosoba, Ahmad, Mehwish I., Min-Jung Lee, Shraddha Rastogi, Nahoko Sato, Yunkai Yu, Pegna, Guillaume Joe, Steinberg, Seth M., Kalsi, Shelley S., Liang Cao, Figg, William D., Trepel, Jane B., Pastan, Ira, FitzGerald, David, and Alewine, Christine

Subjects

CANCER patients, ANTIBODY formation, PANCREATIC intraepithelial neoplasia, T cells, EXOTOXIN

Abstract

Background: LMB-100 is a mesothelin (MSLN)-targeting recombinant immunotoxin (iTox) carrying a Pseudomonas exotoxin A payload that has shown promise against solid tumors, however, efficacy is limited by the development of neutralizing anti-drug antibodies (ADAs). Tofacitinib is an oral Janus Kinase (JAK) inhibitor that prevented ADA formation against iTox in preclinical studies. Methods: A phase 1 trial testing LMB-100 and tofacitinib in patients with MSLNexpressing cancers (pancreatic adenocarcinoma, n=13; cholangiocarcinoma, n=1; appendiceal carcinoma, n=1; cystadenocarcinoma, n=1) was performed to assess safety and to determine if tofacitinib impacted ADA formation. Participants were treated for up to 3 cycles with LMB-100 as a 30-minute infusion on days 4, 6, and 8 at two dose levels (100 and 140 µg/kg) while oral tofacitinib was administered for the first 10 days of the cycle (10 mg BID). Peripheral blood was collected for analysis of ADA levels, serum cytokines and circulating immune subsets. Results: The study was closed early due to occurrence of drug-induced pericarditis in 2 patients. Pericarditis with the combination was not reproducible in a transgenic murine model containing human MSLN. Two of 4 patients receiving all 3 cycles of treatment maintained effective LMB-100 levels, an unusual occurrence. Sustained increases in systemic IL-10 and TNF-α were seen, a phenomenon not observed in prior LMB-100 studies. A decrease in activated T cell subsets and an increase in circulating immunosuppressive myeloid populations occurred. No radiologic decreases in tumor volume were observed. Discussion: Further testing of tofacitinib to prevent ADA formation is recommended in applicable non-malignant disease settings. [ABSTRACT FROM AUTHOR]

Published

2024

9. Glycemia and Gluconeogenesis With Metformin and Liraglutide: A Randomized Trial in Youth-onset Type 2 Diabetes

Author

Dietsche, Katrina B, Magge, Sheela N, Dixon, Sydney A, Davis, Faith S, Krenek, Andrea, Chowdhury, Aruba, Mabundo, Lilian, Stagliano, Michael, Courville, Amber B, Yang, Shanna, Turner, Sara, Cai, Hongyi, Kasturi, Kannan, Sherman, Arthur S, Ha, Joon, Shouppe, Eileen, Walter, Mary, Walter, Peter J, Chen, Kong Y, Brychta, Robert J, Peer, Cody, Zeng, Yi, Figg, William, Cogen, Fran, Estrada, D Elizabeth, Chacko, Shaji, and Chung, Stephanie T

Published

2024

10. Phase 1/2a study of PRL-02, a long-acting IM depot injection of abiraterone decanoate, in patients with prostate cancer including those previously treated with enzalutamide.

Author

Avitia, Jose W., Shore, Neal D., Nordquist, Luke T., Malone, Ryan J., Morris, David, Peer, Cody J., Richardson, William, Schmidt, Keith Thomas, Figg, William Douglas, Walling, Jacqueline M., McDougall, Katherine, Eisner, Joel Robert, Moore, William R., and Tutrone, Ronald F.

Published

2024

11. Small-molecule disruption of androgen receptor-dependent chromatin clusters.

Author

Kohrt SE, Novak EJ, Tapadar S, Wu B, Strope J, Asante Y, Kim H, Chang MS, Gurdak D, Khalil A, Rood M, Raftery E, Stavreva D, Nguyen HM, Brown LG, Ramser M, Peer C, Meyers WM, Aboreden N, Chakravortee M, Sallari R, Nelson PS, Kelly KK, Graham TGW, Darzacq X, Figg WD, Oyelere AK, Corey E, Adelaiye-Ogala R, and Gryder BE

Subjects

Humans, Male, Cell Line, Tumor, Animals, Mice, Gene Expression Regulation, Neoplastic drug effects, Promoter Regions, Genetic, Xenograft Model Antitumor Assays, Signal Transduction drug effects, Receptors, Androgen metabolism, Receptors, Androgen genetics, Chromatin metabolism, Prostatic Neoplasms, Castration-Resistant drug therapy, Prostatic Neoplasms, Castration-Resistant metabolism, Prostatic Neoplasms, Castration-Resistant genetics, Prostatic Neoplasms, Castration-Resistant pathology, Androgen Receptor Antagonists pharmacology, Androgen Receptor Antagonists metabolism

Abstract

Sustained androgen receptor (AR) signaling during relapse is a central driver of metastatic castration-resistant prostate cancer (mCRPC). Current AR antagonists, such as enzalutamide, fail to provide long-term benefit for the mCRPC patients who have dramatic increases in AR expression. Here, we report AR antagonists with efficacy in AR-overexpressing models. These molecules bind to the ligand-binding domain of the AR, promote AR localization to the nucleus, yet potently and selectively down-regulate AR-target genes. The molecules BG-15a and the pharmacokinetically optimized BG-15n elicit a decrease in cell and tumor growth in vitro and in vivo in models of mCRPC. BG-15a/n treatment causes the collapse of chromatin loops between enhancers and promoters at key genes in the AR-driven epigenome. AR binding in the promoter, as well as 3D chromatin clustering, is needed for genes to respond. BG-15a/n represent promising agents for treating patients with relapsed AR-driven mCRPC tumors., Competing Interests: Competing interests statement:E.C. received research funding under institutional SRA from Janssen Research and Development, Bayer Pharmaceuticals, KronosBio, Forma Pharmaceutics Foghorn, Gilead, Sanofi, AbbVie, MacrogGenics, Astra Zeneca, GSK, and K36. B.E.G., A.K.O., S.T., W.D.F., and J.S. are co-inventors on a patent covering this technology (WO2021150603A1). P.S.N. receives personal fees from Janssen, Bristol Myers Squibb, Pfizer, and Merck and grants from Janssen. The other authors declare no competing interests.

Published

2024

12. Targeting NAD+ Metabolism Vulnerability in FH-Deficient Hereditary Leiomyomatosis and Renal Cell Carcinoma with the novel NAMPT Inhibitor OT-82.

Author

Najera SS, Ricketts CJ, Schmidt LS, Medina JI, Saito K, Ileva L, Brender JR, James AM, Peer CJ, Gouker B, Karim BO, Chernova O, Wells C, Wei MH, Yang Y, Zhang X, Klumpp-Thomas C, Travers J, Chen L, Wilson KM, Issaq SH, Figg WD, Difilippantonio S, Kalen JD, Krishna MC, Thomas CJ, Ceribelli M, Heske CM, Crooks DR, and Meier JL

Abstract

Hereditary Leiomyomatosis and Renal Cell Cancer (HLRCC) is an inherited cancer syndrome caused by germline pathogenic variants in the fumarate hydratase (FH) gene. Affected individuals are at risk for developing cutaneous and uterine leiomyomas and aggressive FH-deficient renal cell carcinoma (RCC) with a papillary histology. Due to a disrupted TCA cycle, FH-deficient kidney cancers rely on aerobic glycolysis for energy production, potentially creating compensatory metabolic vulnerabilities. This study conducted a high-throughput drug screen in HLRCC cell lines, which identified a critical dependency on nicotinamide adenine dinucleotide (NAD), a redox cofactor produced by the biosynthetic enzyme nicotinamide phosphoribosyltransferase (NAMPT). Human HLRCC tumors and HLRCC-derived cell lines exhibited elevated NAMPT expression compared to controls. FH-deficient HLRCC cells, but not FH-restored HLRCC or normal kidney cells, were sensitive to NAMPT inhibition. HLRCC cell line viability was significantly decreased in both 2D and 3D in vitro cultures in response to the clinically relevant NAMPT inhibitor OT-82. NAMPT inhibition in vitro significantly decreased the total amount of NAD+, NADH, NADP, NADPH, and PAR levels and the effects of NAMPT inhibition could be rescued by the downstream NAD precursor nicotinamide mononucleotide, confirming the on-target activity of OT-82. Moreover, NAMPT inhibition by OT-82 in two HLRCC xenograft models resulted in severely reduced tumor growth. OT-82 treatment of HLRCC xenograft tumors in vivo inhibited glycolytic flux as demonstrated by reduced lactate/pyruvate ratio in hyperpolarized 13C-pyruvate magnetic resonance spectroscopic imaging experiments. Overall, our data define NAMPT inhibition as a potential therapeutic approach for FH-deficient HLRCC-associated renal cell carcinoma.

Published

2024

13. Colesevelam for lenalidomide associated diarrhea in patients with multiple myeloma.

Author

Hultcrantz M, Hassoun H, Korde N, MacLachlan K, Mailankody S, Patel D, Shah UA, Tan CR, Chung DJ, Lahoud OB, Landau HJ, Scordo M, Shah GL, Giralt SA, Pianko MJ, Burge M, Barnett K, Salcedo M, Caple J, Tran L, Blaslov J, Shekarkhand T, Hamid S, Nemirovsky D, Derkach A, Arisa O, Peer CJ, Figg WD, Usmani SZ, Landgren O, and Lesokhin AM

Subjects

Humans, Male, Female, Aged, Middle Aged, Multiple Myeloma drug therapy, Multiple Myeloma complications, Lenalidomide therapeutic use, Lenalidomide adverse effects, Diarrhea chemically induced

Published

2024

14. Pharmacokinetics and Pharmacogenomics of Ribociclib in Black Patients with Metastatic Breast Cancer: The LEANORA study.

Author

Swain S, Schlam I, Smith DM, Peer C, Sissung T, Schmidt K, Tan M, Chitalia A, Bishopric N, Steinberg S, Choo-Wosoba H, Napoli G, Gallagher C, Ashai N, Whitaker K, Mainor C, Tiwari S, Swanson N, Malloy S, Isaacs C, and Figg W

Abstract

Underrepresented populations' participation in clinical trials remains limited, and the potential impact of genomic variants on drug metabolism remains elusive. This study aimed to assess the pharmacokinetics (PK) and pharmacogenomics (PGx) of ribociclib in self-identified Black women with hormone receptor-positive (HR+)/human epidermal growth factor receptor 2-negative (HER2) advanced breast cancer. LEANORA (NCT04657679) was a prospective, observational, multicenter cohort study involving 14 Black women. PK and PGx were evaluated using tandem mass spectrometry and PharmacoScan™ microarray (including CYP3A5*3 , *6 , and *7 ). CYP3A5 phenotypes varied among participants: 7 poor metabolizers (PM), 6 intermediate metabolizers (IM), and one normal metabolizer (NM). The area-under-the-curve did not significantly differ between PMs (39,230 hr*ng/mL) and IM/NMs (43,546 hr*ng/mL; p = 0.38). The incidence of adverse events (AEs) was also similar. We found no association between CYP3A5 genotype and ribociclib exposure. Continued efforts are needed to include diverse populations in clinical trials to ensure equitable treatment outcomes.

Published

2024

15. Combination Targeted Therapy in Relapsed Diffuse Large B-Cell Lymphoma.

Author

Melani C, Lakhotia R, Pittaluga S, Phelan JD, Huang DW, Wright G, Simard J, Muppidi J, Thomas CJ, Ceribelli M, Tosto FA, Yang Y, Xu W, Davies-Hill T, Pack SD, Peer CJ, Arisa O, Mena E, Lindenberg L, Bergvall E, Portell CA, Farah RJ, Lee ST, Pradhan A, Morrison C, Tadese A, Juanitez AM, Lu C, Jacob A, Simmons H, Figg WD, Steinberg SM, Jaffe ES, Roschewski M, Staudt LM, and Wilson WH

Subjects

Adult, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Adenine analogs & derivatives, Adenine adverse effects, Adenine therapeutic use, Adenine administration & dosage, Bridged Bicyclo Compounds, Heterocyclic adverse effects, Bridged Bicyclo Compounds, Heterocyclic therapeutic use, Bridged Bicyclo Compounds, Heterocyclic administration & dosage, Molecular Targeted Therapy, Prednisone adverse effects, Prednisone administration & dosage, Prednisone therapeutic use, Progression-Free Survival, Pyrazoles adverse effects, Pyrazoles therapeutic use, Pyrazoles administration & dosage, Pyrimidines adverse effects, Pyrimidines therapeutic use, Pyrimidines administration & dosage, Recurrence, Sulfonamides adverse effects, Sulfonamides administration & dosage, Sulfonamides therapeutic use, Antibodies, Monoclonal, Humanized adverse effects, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Antineoplastic Combined Chemotherapy Protocols adverse effects, Lenalidomide adverse effects, Lenalidomide administration & dosage, Lenalidomide therapeutic use, Lymphoma, Large B-Cell, Diffuse drug therapy, Lymphoma, Large B-Cell, Diffuse mortality, Piperidines adverse effects, Piperidines therapeutic use, Piperidines administration & dosage

Abstract

Background: The identification of oncogenic mutations in diffuse large B-cell lymphoma (DLBCL) has led to the development of drugs that target essential survival pathways, but whether targeting multiple survival pathways may be curative in DLBCL is unknown., Methods: We performed a single-center, phase 1b-2 study of a regimen of venetoclax, ibrutinib, prednisone, obinutuzumab, and lenalidomide (ViPOR) in relapsed or refractory DLBCL. In phase 1b, which included patients with DLBCL and indolent lymphomas, four dose levels of venetoclax were evaluated to identify the recommended phase 2 dose, with fixed doses of the other four drugs. A phase 2 expansion in patients with germinal-center B-cell (GCB) and non-GCB DLBCL was performed. ViPOR was administered every 21 days for six cycles., Results: In phase 1b of the study, involving 20 patients (10 with DLBCL), a single dose-limiting toxic effect of grade 3 intracranial hemorrhage occurred, a result that established venetoclax at a dose of 800 mg as the recommended phase 2 dose. Phase 2 included 40 patients with DLBCL. Toxic effects that were observed among all the patients included grade 3 or 4 neutropenia (in 24% of the cycles), thrombocytopenia (in 23%), anemia (in 7%), and febrile neutropenia (in 1%). Objective responses occurred in 54% of 48 evaluable patients with DLBCL, and complete responses occurred in 38%; complete responses were exclusively in patients with non-GCB DLBCL and high-grade B-cell lymphoma with rearrangements of MYC and BCL2 or BCL6 (or both). Circulating tumor DNA was undetectable in 33% of the patients at the end of ViPOR therapy. With a median follow-up of 40 months, 2-year progression-free survival and overall survival were 34% (95% confidence interval [CI], 21 to 47) and 36% (95% CI, 23 to 49), respectively., Conclusions: Treatment with ViPOR was associated with durable remissions in patients with specific molecular DLBCL subtypes and was associated with mainly reversible adverse events. (Funded by the Intramural Research Program of the National Cancer Institute and the National Center for Advancing Translational Sciences of the National Institutes of Health and others; ClinicalTrials.gov number, NCT03223610.)., (Copyright © 2024 Massachusetts Medical Society.)

Published

2024