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Treatment for Pulmonary Arterial Hypertension: Receptor Tyrosine Kinase Inhibitors and Calcium Channel Blockers01:26

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Receptor tyrosine kinase inhibitors (TKIs) and calcium channel blockers (CCBs) are two critical categories of drugs employed in the treatment of pulmonary artery hypertension (PAH). PAH is a disease that causes high blood pressure in the pulmonary arteries, resulting in chest pain, fatigue, and shortness of breath.
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The targeted cancer therapies, also known as “molecular targeted therapies,” take advantage of the molecular and genetic differences between the cancer cells and the normal cells. It needs a thorough understanding of the cancer cells to develop drugs that can target specific molecular aspects that drive the growth, progression, and spread of cancer cells without affecting the growth and survival of other normal cells in the body.
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Post-approval, manufacturers may modify an approved new or generic drug product. Such modifications can encompass alterations in the Active Pharmaceutical Ingredient (API), manufacturing process, formulation, batch size, manufacturing site, and container closure system (FDA Guidance for Industry, April 2004). Often, a drug product may undergo multiple changes.These modifications require careful evaluation to determine their potential impact on the drug product's identity, strength, quality,...
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Neurokinin 1 (NK1) receptors are distributed across the GI tract, vagal afferents, and key CNS regions including the central vomiting center and chemoreceptor trigger zone (CTZ) Chemotherapy agents stimulate enterochromaffin cells in the gastrointestinal (GI) tract to release large amounts of substance P (SP). SP is a neuropeptide released by specific sensory nerves in response to many different stressors, including those in the GI mucosa affected by chemotherapy.  SP binds and activates...
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The orderly progression of the cell cycle depends on the activation of Cdk protein by binding to its cyclin partner. However, the cell cycle must be restricted when undergoing abnormal changes. Most cancers correlate to the deregulated cell cycle, and since Cdks are a central component of the cell cycle, Cdk inhibitors are extensively studied to develop anticancer agents. For instance, cyclin D associates with several Cdks, such as Cdk 4/6, to form an active complex. The cyclin D-Cdk4/6 complex...
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Cancer is the second leading cause of death in the United States. A cancer cell is genetically unstable and hence can mutate faster. They can also modify their microenvironment and escape immune surveillance. The difficulties in treating cancer are further compounded by the emergence of rapid resistance to anticancer drugs. The most common ways to attain resistance in cancer cells include alteration in drug transport and metabolism, modification of drug target, elevated DNA damage response, or...
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相关实验视频

Updated: Feb 27, 2026

Establishment and Characterization of Three Afatinib-resistant Lung Adenocarcinoma PC-9 Cell Lines Developed with Increasing Doses of Afatinib
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随机混合物:第一次批准.

Michael B Brown1

  • 1Springer Nature, Private Bag 65901, Mairangi Bay, Auckland, 0754, New Zealand. dru@adis.com.

Drugs
|February 26, 2026
PubMed
概括
此摘要是机器生成的。

尼兰多米拉斯特是一种新的口服治疗异常性肺纤维化 (IPF) 和渐进性肺纤维化 (PPF) 的治疗方法. 它是一种选择性化酶4B抑制剂,最近在美国和中国获得批准.

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科学领域:

  • 药理学 药理学是指药理学的学科.
  • 肺部病理学 肺部病理学
  • 药物开发 药物开发

背景情况:

  • 异常性肺纤维化 (IPF) 和渐进性肺纤维化 (PPF) 是慢性肺病,治疗选择有限.
  • 二酶4B (PDE4B) 是纤维化肺部疾病的潜在治疗点.
  • 涅兰多米拉斯特是一种口服选择性PDE4B抑制剂,用于治疗肺纤维化.

研究的目的:

  • 总结一下Nerandomilast发展中的关键里程碑.
  • 要突出监管部门对治疗IPF和PPF中的内拉多米拉斯的批准.

主要方法:

  • 发展史和临床试验数据的审查.
  • 对监管提交和批准时间表的分析.

主要成果:

  • 涅兰多米拉斯特于2025年10月7日在美国首次获得批准,用于成人IPF.
  • 随后在中国 (2025年10月22日) 获得IPF,在中国和美国 (2025年12月) 获得PPF的批准.
  • 目前正在进行的全球申请和II/III期试验表明持续发展.

结论:

  • 涅兰多米拉斯特代表了IPF和PPF治疗的重大进步.
  • 该药物的开发里程碑和批准标志着为患有纤维化肺部疾病的患者提供了新的治疗选择.
  • 预计进一步的临床试验和全球申请将扩大对这种新型治疗的获取.