Your search keyword '"Nahor Haddish-Berhane"' showing total 3 results

1. Cardiac Safety Assessment of Lazertinib: Findings From Patients With EGFR Mutation-Positive Advanced NSCLC and Preclinical Studies

Author

Seong Bok Jang, PhD, Kyeong Bae Kim, PhD, Sujin Sim, MS, Byoung Chul Cho, MD, PhD, Myung-Ju Ahn, MD, PhD, Ji-Youn Han, MD, PhD, Sang-We Kim, MD, PhD, Ki Hyeong Lee, MD, PhD, Eun Kyung Cho, MD, PhD, Nahor Haddish-Berhane, PhD, Jaydeep Mehta, PharmD, PhD, and Se-Woong Oh, PhD

Subjects

Non–small cell lung cancer, Tyrosine kinase inhibitor, Lazertinib, Cardiac toxicity, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Introduction: Lazertinib is a potent, irreversible, brain-penetrant, mutant-selective, and wild-type–sparing third-generation EGFR tyrosine kinase inhibitor (TKI), creating a wide therapeutic index. Cardiovascular adverse events (AEs), including QT prolongation, decreased left ventricular ejection fraction (LVEF), and heart failure, have emerged as potential AEs with certain EGFR TKI therapies. Methods: Cardiac safety of lazertinib was evaluated in TKI-tolerant adults with EGFR mutation-positive locally advanced or metastatic NSCLC receiving lazertinib (20–320 mg/d). QT intervals corrected with Fridericia’s formula (QTcF) prolongation, time-matched concentration-QTcF relationship, change of LVEF, and cardiac failure-associated AEs were evaluated. The clinical findings were supplemented by the following three preclinical studies: an in vitro hERG inhibition assay, an ex vivo isolated perfused rabbit heart study, and an in vivo telemetry-instrumented beagle dog study. Results: Preclinical evaluation revealed little to no physiological effect on the basis of electrocardiogram, electrophysiological, proarrhythmic, and hemodynamic parameters. Clinical evaluation of 181 patients revealed no clinically relevant QTcF prolongation by centralized electrocardiogram in any patient and at any dose level. The predicted magnitude of QTcF value increase at maximum steady-state plasma concentration for the therapeutic dose of lazertinib (240 mg/d) was 2.2 msec (upper bound of the two-sided 90% confidence interval: 3.6 msec). No patient had clinically relevant LVEF decrease (i.e., minimum postbaseline LVEF value of

Published

2021

2. Contributors

Author

Nilanjan Adhikari, Gouri Ahir, Hanan A. Al-Dossary, Meneerah Abdurhman Aljafary, Khulood Mohammed Al-Khater, Ebtesam Abdullah Al-Suhaimi, Sk. Abdul Amin, Ghulam Md Ashraf, Reem A. Assuhaimi, Himani Balutia, Anwar L. Bilgrami, Diana Campos-Iglesias, Sapana Sameer Chaudhary, Sameer Choudhary, V. Cicaloni, Rohit Dutt, Sayan Dutta Gupta, Abdelhamid Elaissari, I. Fotopoulos, José M.P. Freije, Ankit Ganeshpurkar, Vandana Garg, Rishitha Gundala, Satya P. Gupta, Nahor Haddish-Berhane, D. Hadjipavlou-Litina, B.S. Harish, Srabanti Jana, Tarun Jha, Deepak Kumar, Devendra Kumar, Sanjay Kumar, R. Lavanya, Carlos López-Otín, A.K. Madan, Ayesha Mahmood, Subhajit Makar, Tanima Mandal, Ashima Nagpal, Dolly A. Parasrampuria, A. Peperidou, F. Pettini, Nitesh Kumar Poddar, E. Pontiki, Pankaj Kumar Rai, Vijaya Ravinayagam, Sakshi Rawat, Kuldeep K. Roy, Priyanka Saha, Adeeb Shehzad, Devendra Shukla, Sushil Kumar Singh, O. Spiga, Amit Kumar Srivastava, Mohamad Tarhini, Rajiv Kumar Tonk, A. Trezza, Kiran Babu Uppuluri, Ravichandiran Velayutham, Saroj Verma, Alex Yu, and Nadiah Zafar

Published

2020

3. KRAS: Structure, function, and development of anticancer drugs

Author

Dolly A. Parasrampuria, Alex Yu, and Nahor Haddish-Berhane

Subjects

Mutation, Cell signaling, Tumor suppressor gene, Effector, Mutant, Guanosine triphosphate, Biology, medicine.disease_cause, Cell biology, chemistry.chemical_compound, chemistry, Guanosine diphosphate, medicine, KRAS

Abstract

The Ras family of genes are highly conserved across species and play an integral role in cell signaling. KRAS belongs to this family of genes that function as switches cycling between guanosine diphosphate (GDP)-bound OFF state or guanosine triphosphate (GTP)-bound ON state. When the homeostasis between the GDP- or GTP-bound states is disrupted, cell proliferation and signaling proceeds unchecked. Wild-type KRAS appears to function as a tumor suppressor gene, but mutated KRAS imparts an especially recalcitrant and a highly lethal cancer phenotype. Despite almost four decades of intense research, no therapies have been successful in targeting mutant KRAS. In part this is due to the small structure of the protein, which does not present scaffolds that can be readily targeted to render the molecule in an inactive conformation. The manifold interactions of KRAS with effector proteins and a host of posttranslational modifications appear to magnify the impact on cell signaling and allow for redundant pathways that can overcome attempts to silence the effects of the mutation. It is thought that KRAS mutations are not sufficient to activate a cancer; typically, another trigger is needed. This trigger might differ between different organs and is not fully understood. An understanding of the structure, function, signaling, and mutations can help advance the quest for a therapy for this elusive target.

Published

2020