Overview
Abemaciclib is an antitumor agent and dual inhibitor of cyclin-dependent kinases 4 (CDK4) and 6 (CDK6) that are involved in the cell cycle and promotion of cancer cell growth in case of unregulated activity. On September 28, 2017, FDA granted approval of abemaciclib treatment under the market name Verzenio for the treatment of HR-positive and HER2-negative advanced or metastatic breast cancer that has progressed after unsuccessful endocrine therapy. It is either given alone in patients who has undergone endocrine therapy and chemotherapy after the metastasis of cancer, or in combination with Fulvestrant. Following oral treatment in patients with HR-positive, HER2-negative breast cancer, abemaciclib demonstrated increased progression-free survival rates and objective response rates. Abemaciclib has been used in trials studying the treatment of melanoma, lymphoma, neoplasm, solid tumor, and glioblastoma.
Indication
适应症为:⑴单药治疗接受过内分泌疗法和化疗后疾病进展的 ER+/HER2-晚期或转移性乳腺癌;⑵或联合氟维司群,二线治疗接受过内分泌疗法后疾病进展的 ER+/HER2-晚期或转移性乳腺癌;⑶联合芳香酶抑制剂作为 ER+/HER2-绝经后女性晚期或转移性乳腺癌的初始内分泌疗法。
Associated Conditions
- HR+, HER2-, Advanced Breast Cancer
- Early Hormone Receptor Positive, HER2/Neu Negative Node Positive Breast Cancer
- Metastatic HR + HER2 - breast cancer
Research Report
Abemaciclib: A Comprehensive Review of its Pharmacology, Clinical Efficacy, and Regulatory Status in Cancer Therapy
1. Introduction to Abemaciclib
1.1. Overview, Chemical Properties, and DrugBank Identification
Abemaciclib, an orally administered small molecule, is a significant therapeutic agent in oncology, primarily for specific types of breast cancer [User query]. Its unique chemical and pharmacological properties underpin its clinical utility.
Key identifiers and properties include:
- Drug Name: Abemaciclib [User query]
- DrugBank ID: DB12001 [User query]
- Drug Type: Small Molecule [User query]
- CAS Number: 1231929-97-7 [User query]
- Molecular Formula: C27H32F2N8 [1]
- Molecular Weight: 506.61 g/mol [1]
These identifiers are crucial for its consistent recognition in scientific literature, clinical trials, and regulatory documentation. The chemical structure, characterized by the presence of fluorine atoms and multiple nitrogen-containing rings, contributes to its binding affinity and pharmacokinetic profile.
1.2. Background and Rationale for Development
Abemaciclib was developed as an antitumor agent specifically targeting cyclin-dependent kinases 4 (CDK4) and 6 (CDK6).[3] These kinases are pivotal in regulating the cell cycle, and their dysregulation, often observed in various cancers, leads to uncontrolled cell proliferation and tumor growth.[3] The therapeutic rationale for developing CDK4/6 inhibitors like abemaciclib stems from the understanding that aberrant CDK4/6 activity, frequently driven by cyclin D overexpression or loss of endogenous inhibitors (e.g., p16INK4a), is a key driver in many hormone receptor-positive (HR+) breast cancers. By inhibiting these kinases, abemaciclib aims to restore cell cycle control and suppress cancer progression.
Clinical Trials
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Title | Posted | Study ID | Phase | Status | Sponsor |
---|---|---|---|---|---|
2019/09/17 | Phase 1 | Recruiting | |||
2019/08/30 | Early Phase 1 | Active, not recruiting | |||
2019/08/28 | Phase 1 | Completed | |||
2019/08/08 | Early Phase 1 | UNKNOWN | |||
2019/07/31 | Phase 2 | Recruiting | |||
2019/07/24 | Phase 4 | Terminated | |||
2019/07/01 | Phase 2 | Terminated | |||
2019/06/25 | Phase 2 | Terminated | Nataliya Uboha | ||
2019/06/21 | Phase 2 | Recruiting | |||
2019/06/17 | Phase 4 | Withdrawn |
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