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相关概念视频

Preclinical Development: Overview01:28

Preclinical Development: Overview

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Preclinical development consists of a series of tests that ensure the safety and efficacy of a new therapeutic compound before it is tested in humans. There are four main phases to this process. First, safety pharmacology tests are conducted to ensure the drug does not produce any acutely harmful effects. These tests examine parameters such as bronchoconstriction, cardiac dysrhythmias, blood pressure changes, and ataxia. Next, preliminary toxicological testing is performed to determine the...
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Clinical Trials: Overview01:11

Clinical Trials: Overview

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Clinical development focuses on how the drug will interact with the human body and encompasses four key phases of clinical trials, each serving a specific purpose in assessing the safety and effectiveness of new drugs. These phases overlap and build upon one another. Phase I involves a small group of healthy volunteers (typically 20-80 individuals) or, in cases where significant toxicity is expected, patients with the targeted disease, such as cancer or AIDS. The volunteers are tested for...
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Drug Discovery: Overview01:26

Drug Discovery: Overview

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Drug discovery is a multifaceted process involving extensive screening, testing, and optimization of lead compounds to identify potential new drugs for therapeutic use. It combines several approaches, including screening large numbers of natural products, chemical modification of known active molecules, identification of new drug targets, and rational design based on biological mechanisms and drug-receptor structure. These approaches are carried out in both academic research laboratories and...
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Drug Administration and Therapy Phases: Overview01:26

Drug Administration and Therapy Phases: Overview

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Drugs, the chemical agents used in diagnosing, treating, or preventing diseases, undergo a four-phase process of development: pharmaceutic, pharmacokinetics, pharmacodynamics, and therapeutic.
The pharmaceutical phase focuses on leveraging the physicochemical properties of the drug to design and manufacture an effective product. Variants include orally administered tablets or capsules, topical creams or ointments, and parenteral-delivery solutions or emulsions.
The pharmacokinetic phase...
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In Vitro Drug Release Testing: Overview, Development and Validation01:10

In Vitro Drug Release Testing: Overview, Development and Validation

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In vitro dissolution and drug release tests assess how quickly and how much of a drug is released from its dosage form into an aqueous medium under standardized laboratory conditions. These tests are essential tools in pharmaceutical development and quality assurance, offering insight into the drug's performance before clinical use.During formulation development, dissolution testing identifies incomplete or inconsistent drug release issues. It also supports decisions on selecting the optimal...
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Drug Regulation01:25

Drug Regulation

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Drug regulation encompasses the management of drug usage by evaluating its safety and efficacy through assessments conducted by regulatory authorities. Regrettably, the history of drug regulation is marred by several catastrophic events. One such incident is the Elixir Sulfanilamide tragedy, in which the toxic compound diethyl glycol was included in a sweet-tasting medication, leading to numerous fatalities. This event prompted the enactment of the Food, Drug, and Cosmetic Act in 1938. Under...
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Drug Repurposing Hypothesis Generation Using the "RE:fine Drugs" System
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药物开发 药物开发

Louise Dickson1, Roberto Tolando1, Celina Scholl2

  • 1Cerevance Ltd, Cambridge, Cambridgeshire, United Kingdom.

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PubMed
概括
此摘要是机器生成的。

CVN293,一种新的KCNK13抑制剂,在健康成年人中显示出良好的安全性和大脑透. 这支持其通过减少神经炎症来治疗神经退行性疾病的潜力.

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In Vitro Three-Dimensional Sprouting Assay of Angiogenesis Using Mouse Embryonic Stem Cells for Vascular Disease Modeling and Drug Testing
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科学领域:

  • 神经科学是一个神经科学.
  • 药理学 药理学是指药理学的学科.
  • 免疫学 免疫学 免疫学

背景情况:

  • 微质中的KCNK13通道是NLRP3炎症酶激活的关键.
  • 在NLRP3中介的神经炎症驱动神经退行性疾病.
  • CVN293针对KCNK13抑制微质炎症过程.

研究的目的:

  • 在健康人群中评估口服CVN293的安全性和耐受性.
  • 评估CVN293.3的药理动力学和脑脊液 (CSF) 透率.
  • 支持进一步开发CVN293用于神经退行性疾病.

主要方法:

  • 第1期,随机,双盲,安慰剂对照研究 (SAD/MAD).
  • 每天单剂量高达1000毫克,多剂量高达750毫克.
  • 在禁食和食条件下口服;进行CSF采样.

主要成果:

  • CVN293的耐受性很好,并有轻微的不良事件.
  • 没有观察到严重或剂量限制的不良事件.
  • 剂量相对应的血暴露和CSF透得到证实.

结论:

  • 在健康的成年人中,CVN293表现出良好的安全性.
  • 已证明能够达到CSF的能力支持其潜在的治疗用途.
  • 支持神经炎症驱动的神经退行性疾病的持续发展.