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相关概念视频

Antidotes01:17

Antidotes

Antidotes are medicinal substances used to counteract the harmful effects of toxins or drugs in the body. They function in various ways, each uniquely designed to combat specific toxic compounds.
Specific antidotes operate by inhibiting the enzymes that control biochemical pathways, reducing the production of harmful metabolites.
An example of an antidote is atropine, which counteracts the detrimental effects of cholinesterase inhibitors. It achieves this by deactivating muscarinic receptors,...
Anticholinesterase Agents: Poisoning and Treatment01:26

Anticholinesterase Agents: Poisoning and Treatment

Anticholinesterases, also known as cholinesterase inhibitors, work by blocking the breakdown of acetylcholine, leading to its accumulation in the synaptic cleft. This accumulation indirectly enhances both muscarinic and nicotinic actions. These agents are classified as reversible or irreversible based on their mechanism of action.     
Irreversible agents form a strong bond with the cholinesterase enzyme, making it inactive. The breakdown of the phosphorylated enzyme is slower than the...
Phase II Reactions: Sulfation and Conjugation with α-Amino Acids01:19

Phase II Reactions: Sulfation and Conjugation with α-Amino Acids

Sulfation and α-amino acid conjugation are two critical biotransformation reactions in drug metabolism. Sulfation, a phase II biotransformation reaction, involves adding a polar sulfate group to a drug, enhancing its water solubility and promoting excretion. This process can either co-occur with or occur independently of glucuronidation. Nonmicrosomal sulfotransferase enzymes catalyze the process. The reaction involves 3'-phosphoadenosine-5'-phosphosulfate or PAPS coenzyme activation, sulfur...
Phase II Reactions: Glutathione Conjugation and Mercapturic Acid Formation01:22

Phase II Reactions: Glutathione Conjugation and Mercapturic Acid Formation

Glutathione, a tripeptide made up of glutamate, cysteine, and glycine, is a critical player in the detoxification of drugs and xenobiotics via a process known as glutathione conjugation or mercapturic acid formation. This phase II biotransformation reaction involves the covalent binding of glutathione to a drug or its metabolite, enhancing the compound's water solubility and enabling its excretion.
Several distinctive characteristics distinguish glutathione conjugation from other phase II...
Phase II Reactions: Acetylation Reactions01:24

Phase II Reactions: Acetylation Reactions

Acetylation, a phase II biotransformation reaction, introduces an acetyl group to drugs or their metabolites. Acetyltransferase enzymes facilitate this reaction, which resembles α-amino acid conjugation due to the addition of a functional group to the drug molecule.
The substrates for acetylation are typically drugs or their metabolites with an amino, sulfonamide, or hydrazine functional group. Acetylation can occur at several points in the drug molecule, including primary, secondary, and...
Sulfur Assimilation01:20

Sulfur Assimilation

Sulfur is an essential element in biological systems, contributing to synthesizing key biomolecules, including amino acids such as cysteine and methionine, and cofactors such as coenzyme A and biotin. Microorganisms primarily assimilate sulfur as sulfate (SO₄²⁻) from the environment, which must undergo a series of biochemical transformations before it can be incorporated into cellular components. As sulfate is highly oxidized, it must undergo assimilatory sulfate reduction to become...

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相关实验视频

Updated: Jun 9, 2026

A Strategy for Sensitive, Large Scale Quantitative Metabolomics
14:18

A Strategy for Sensitive, Large Scale Quantitative Metabolomics

Published on: May 27, 2014

另一个纠结#82:N-乙半氨酸.

Sandeep Yerraguntla1, Bhavya Bakshi1, Keshav Chandran2

  • 1Medical College of GA at Augusta University, Augusta, GA, USA.

Amyotrophic lateral sclerosis & frontotemporal degeneration
|March 4, 2026
PubMed
概括
此摘要是机器生成的。

通过向氧化应激和炎症,N-乙半氨酸 (NAC) 显示出对肌缩侧面硬化症 (ALS) 的理论前景. 然而,来自临床前研究和临床试验的现有证据不支持其在减缓ALS进展方面的有效性.

关键词:
肌缩性侧面硬化症 (AMLS) 是一种疾病.这是一种N-乙囊氨酸.抗氧化剂是一种抗氧化剂.氧化应激是一种氧化应激.

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An In Vitro Batch-culture Model to Estimate the Effects of Interventional Regimens on Human Fecal Microbiota
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An In Vitro Batch-culture Model to Estimate the Effects of Interventional Regimens on Human Fecal Microbiota

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Resin-Assisted Capture Coupled with Isobaric Tandem Mass Tag Labeling for Multiplexed Quantification of Protein Thiol Oxidation
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Resin-Assisted Capture Coupled with Isobaric Tandem Mass Tag Labeling for Multiplexed Quantification of Protein Thiol Oxidation

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相关实验视频

Last Updated: Jun 9, 2026

A Strategy for Sensitive, Large Scale Quantitative Metabolomics
14:18

A Strategy for Sensitive, Large Scale Quantitative Metabolomics

Published on: May 27, 2014

An In Vitro Batch-culture Model to Estimate the Effects of Interventional Regimens on Human Fecal Microbiota
07:15

An In Vitro Batch-culture Model to Estimate the Effects of Interventional Regimens on Human Fecal Microbiota

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Resin-Assisted Capture Coupled with Isobaric Tandem Mass Tag Labeling for Multiplexed Quantification of Protein Thiol Oxidation
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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.

背景情况:

  • N-乙半氨酸 (NAC) 是一种具有潜在神经保护机制的谷氨前体,与肌缩侧面硬化症 (ALS) 有关.
  • 建议的机制包括减少氧化应激,神经炎症和ALS中的线粒体功能障碍.
  • 关于NAC在ALS小鼠模型中的疗效的临床前数据是矛盾的.

研究的目的:

  • 评估N-乙半氨酸在减缓肌缩侧面硬化症 (ALS) 的进展方面的治疗潜力.

主要方法:

  • 在ALS小鼠模型中进行的临床前研究的审查.
  • 分析涉及ALS患者口服或皮下NAC给药的案例研究.
  • 从已完成的临床试验中检查ALS治疗NAC的数据的检查.

主要成果:

  • 临床前研究在ALS小鼠模型中的运动损伤和生存率方面产生了不一致的结果.
  • 案例研究和临床试验并没有证明NAC在减缓ALS进展方面具有令人信服的益处或有效性.
  • 根据现有证据,ALSUntangled目前不建议NAC减缓ALS进展.

结论:

  • 由于其抗氧化和抗炎性质,N-乙半氨酸在理论上显示出对ALS治疗的前景.
  • 尽管理论上有希望,但目前的临床证据并不支持使用N-乙半氨酸来减缓ALS的进展.
  • 需要进一步的研究来确定N-乙半氨酸在治疗ALS中的治疗作用,如果有的话.