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Rational design of dual ALK inhibitors: scaffolds and strategies to circumvent drug resistance.

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Bioorganic chemistry 2026 Vol.174() p. 109706 Lung Cancer Treatments and Mutations
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PubMed DOI OpenAlex 마지막 보강 2026-04-28
OpenAlex 토픽 · Lung Cancer Treatments and Mutations Melanoma and MAPK Pathways HER2/EGFR in Cancer Research

Yahya TAA, Al-Qadhi MA

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Anaplastic lymphoma kinase (ALK) is a clinically validated oncogenic driver in multiple malignancies; however, the long-term efficacy of ALK tyrosine kinase inhibitors is frequently compromised by tum

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APA Tawfeek A.A. Yahya, Mustafa A. Al-Qadhi (2026). Rational design of dual ALK inhibitors: scaffolds and strategies to circumvent drug resistance.. Bioorganic chemistry, 174, 109706. https://doi.org/10.1016/j.bioorg.2026.109706
MLA Tawfeek A.A. Yahya, et al.. "Rational design of dual ALK inhibitors: scaffolds and strategies to circumvent drug resistance.." Bioorganic chemistry, vol. 174, 2026, pp. 109706.
PMID 41825145
DOI 10.1016/j.bioorg.2026.109706

Abstract

Anaplastic lymphoma kinase (ALK) is a clinically validated oncogenic driver in multiple malignancies; however, the long-term efficacy of ALK tyrosine kinase inhibitors is frequently compromised by tumor heterogeneity, adaptive signaling, and compensatory pathway activation. Although successive generations of ALK inhibitors have addressed several resistance mutations, achieving durable therapeutic responses remains challenging. In this context, dual-target ALK inhibitors-single molecular entities capable of concurrently inhibiting ALK and complementary oncogenic targets-have emerged as a rational polypharmacological strategy. This review summarizes recent advances (2018-2025) in the rational design of dual ALK inhibitors, highlighting key chemotypes including 2,4-diaminopyrimidines, 2-aminopyridines, and pyrazolo[1,5-a]pyrimidines. Structure-based drug design strategies such as pharmacophore hybridization, scaffold hopping, solvent-front mutation engineering, and macrocyclization are critically analyzed with respect to potency, selectivity, CNS penetration, and resistance coverage. Dual-target combinations involving ALK with TRK, EGFR, ROS1, HDAC, CDK4/6, FAK, and related targets are systematically discussed, supported by SAR trends, crystallographic insights, and molecular modeling. Collectively, this review provides a design-focused framework to guide the development of next-generation dual ALK inhibitors aimed at achieving durable pathway suppression in ALK-driven cancers. Solvent-front mutation engineering.

MeSH Terms

Humans; Anaplastic Lymphoma Kinase; Protein Kinase Inhibitors; Drug Design; Drug Resistance, Neoplasm; Antineoplastic Agents; Molecular Structure; Structure-Activity Relationship; Neoplasms