D-Leucine (BioDeep_00000014649)

 

Secondary id: BioDeep_00001868196

human metabolite PANOMIX_OTCML-2023 Endogenous blood metabolite


代谢物信息卡片


(2R)-2-amino-4-methylpentanoic acid

化学式: C6H13NO2 (131.0946238)
中文名称: D-亮氨酸
谱图信息: 最多检出来源 Homo sapiens(blood) 5.88%

分子结构信息

SMILES: CC(C)CC(C(=O)O)N
InChI: InChI=1S/C6H13NO2/c1-4(2)3-5(7)6(8)9/h4-5H,3,7H2,1-2H3,(H,8,9)/t5-/m1/s1

描述信息

An essential branched-chain amino acid important for hemoglobin formation. [PubChem]; Branched chain amino acids (BCAA) are essential amino acids whose carbon structure is marked by a branch point. These three amino acids are critical to human life and are particularly involved in stress, energy and muscle metabolism. BCAA supplementation as therapy, both oral and intravenous, in human health and disease holds great promise. BCAA denotes valine, isoleucine and leucine which are branched chain essential amino acids. Despite their structural similarities, the branched amino acids have different metabolic routes, with valine going solely to carbohydrates, leucine solely to fats and isoleucine to both. The different metabolism accounts for different requirements for these essential amino acids in humans: 12 mg/kg, 14 mg/kg and 16 mg/kg of valine, leucine and isoleucine respectively. Furthermore, these amino acids have different deficiency symptoms. Valine deficiency is marked by neurological defects in the brain, while isoleucine deficiency is marked by muscle tremors. Many types of inborn errors of BCAA metabolism exist, and are marked by various abnormalities. The most common form is the maple syrup urine disease, marked by a characteristic urinary odor. Other abnormalities are associated with a wide range of symptoms, such as mental retardation, ataxia, hypoglycemia, spinal muscle atrophy, rash, vomiting and excessive muscle movement. Most forms of BCAA metabolism errors are corrected by dietary restriction of BCAA and at least one form is correctable by supplementation with 10 mg of biotin daily. BCAA are useful because they are metabolized primarily by muscle. Stress state- e.g surgery, trauma, cirrhosis, infections, fever and starvation--require proportionately more BCAA than other amino acids and probably proportionately more leucine than either valine or isoleucine. BCAA and other amino acids are frequently fed intravenously (TPN) to malnourished surgical patients and in some cases of severe trauma. BCAA, particularly leucine, stimulate protein synthesis, increase reutilization of amino acids in many organs and reduce protein breakdown. Furthermore, leucine can be an important source of calories, and is superior as fuel to the ubiquitous intravenous glucose (dextrose). Leucine also stimulates insulin release, which in turn stimulates protein synthesis and inhibits protein breakdown. These effects are particularly useful in athletic training. BCAA should also replace the use of steroids as commonly used by weightlifters. Huntingtons chorea and anorexic disorders both are characterized by low serum BCAA. These diseases, as well as forms of Parkinsons, may respond to BCAA therapy. BCAA, and particularly leucine, are among the amino acids most essential for muscle health. (http://www.dcnutrition.com); Leucine (abbreviated as Leu or L) is a branched-chain amino acid with the chemical formula HO2CCH(NH2)CH2CH(CH3)2. Leucine is classified as a hydrophobic amino acid due to its aliphatic isobutyl side chain. It is encoded by six codons (UUA, UUG, CUU, CUC, CUA, and CUG) and is a major component of the subunits in ferritin, astacin and other buffer proteins. Leucine is an essential amino acid. Leucine is a branched-chain amino acid (BCAA) since it possesses an aliphatic side-chain that is non-linear.
D-Leucine is a more potent anti-seizure agent than L-leucine. D-leucine potently terminates seizures even after the onset of seizure activity. D-leucine, but not L-leucine, reduces long-term potentiation but had no effect on basal synaptic transmission in vitro[1].
D-Leucine is a more potent anti-seizure agent than L-leucine. D-leucine potently terminates seizures even after the onset of seizure activity. D-leucine, but not L-leucine, reduces long-term potentiation but had no effect on basal synaptic transmission in vitro[1].

同义名列表

13 个代谢物同义名

(2R)-2-amino-4-methylpentanoic acid; (2R)-2-Amino-4-methylpentanoate; D-2-Amino-4-methylvaleric acid; D-2-Amino-4-methylvalerate; (R)-(−)-leucine; (R)-(-)-Leucine; L-(+)-Leucine; (R)-Leucine; H-D-Leu-OH; D-Leucine; D-Leucin; D-Leuzin; DLE



数据库引用编号

17 个数据库交叉引用编号

分类词条

相关代谢途径

Reactome(0)

BioCyc(0)

PlantCyc(0)

代谢反应

0 个相关的代谢反应过程信息。

Reactome(0)

BioCyc(0)

WikiPathways(0)

Plant Reactome(0)

INOH(0)

PlantCyc(0)

COVID-19 Disease Map(0)

PathBank(0)

PharmGKB(0)

2 个相关的物种来源信息

在这里通过桑基图来展示出与当前的这个代谢物在我们的BioDeep知识库中具有相关联信息的其他代谢物。在这里进行关联的信息来源主要有:

  • PubMed: 来源于PubMed文献库中的文献信息,我们通过自然语言数据挖掘得到的在同一篇文献中被同时提及的相关代谢物列表,这个列表按照代谢物同时出现的文献数量降序排序,取前10个代谢物作为相关研究中关联性很高的代谢物集合展示在桑基图中。
  • NCBI Taxonomy: 通过文献数据挖掘,得到的代谢物物种来源信息关联。这个关联信息同样按照出现的次数降序排序,取前10个代谢物作为高关联度的代谢物集合展示在桑吉图上。
  • Chemical Taxonomy: 在物质分类上处于同一个分类集合中的其他代谢物
  • Chemical Reaction: 在化学反应过程中,存在为当前代谢物相关联的生化反应过程中的反应底物或者反应产物的关联代谢物信息。

点击图上的相关代谢物的名称,可以跳转到相关代谢物的信息页面。



文献列表

  • Nobuhiro Mori, Megumi Yamamoto, Eri Tsukada, Tomoharu Yokooji, Naoko Matsumura, Masanori Sasaki, Teruo Murakami. Comparison of in vivo with in vitro pharmacokinetics of mercury between methylmercury chloride and methylmercury cysteine using rats and Caco2 cells. Archives of environmental contamination and toxicology. 2012 Nov; 63(4):628-36. doi: 10.1007/s00244-012-9800-5. [PMID: 22932937]
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  • Ignacio Cota, Anne Béatrice Blanc-Potard, Josep Casadesús. STM2209-STM2208 (opvAB): a phase variation locus of Salmonella enterica involved in control of O-antigen chain length. PloS one. 2012; 7(5):e36863. doi: 10.1371/journal.pone.0036863. [PMID: 22606300]
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  • David Duguay, Erika Bélanger-Nelson, Valérie Mongrain, Anna Beben, Armen Khatchadourian, Nicolas Cermakian. Dynein light chain Tctex-type 1 modulates orexin signaling through its interaction with orexin 1 receptor. PloS one. 2011; 6(10):e26430. doi: 10.1371/journal.pone.0026430. [PMID: 22028875]
  • Norihiro Ryuman, Nobuo Watanabe, Takao Arai. S-nitrosation of cellular proteins by NO donors in rat embryonic fibroblast 3Y1 cells: factors affecting S-nitrosation. Oxidative medicine and cellular longevity. 2011; 2011(?):450317. doi: 10.1155/2011/450317. [PMID: 21904643]
  • Arjun Sengupta, Angika Basant, Soumita Ghosh, Shobhona Sharma, Haripalsingh M Sonawat. Liver Metabolic Alterations and Changes in Host Intercompartmental Metabolic Correlation during Progression of Malaria. Journal of parasitology research. 2011; 2011(?):901854. doi: 10.1155/2011/901854. [PMID: 21772982]
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  • Mathieu Schue, Agnes Fekete, Philippe Ortet, Catherine Brutesco, Thierry Heulin, Philippe Schmitt-Kopplin, Wafa Achouak, Catherine Santaella. Modulation of metabolism and switching to biofilm prevail over exopolysaccharide production in the response of Rhizobium alamii to cadmium. PloS one. 2011; 6(11):e26771. doi: 10.1371/journal.pone.0026771. [PMID: 22096497]
  • Morten Schiøtt, Adelina Rogowska-Wrzesinska, Peter Roepstorff, Jacobus J Boomsma. Leaf-cutting ant fungi produce cell wall degrading pectinase complexes reminiscent of phytopathogenic fungi. BMC biology. 2010 Dec; 8(?):156. doi: 10.1186/1741-7007-8-156. [PMID: 21194476]
  • Łukasz Samluk, Magdalena Czeredys, Katarzyna A Nałęcz. Regulation of amino acid/carnitine transporter B 0,+ (ATB 0,+) in astrocytes by protein kinase C: independent effects on raft and non-raft transporter subpopulations. Journal of neurochemistry. 2010 Dec; 115(6):1386-97. doi: 10.1111/j.1471-4159.2010.07040.x. [PMID: 20977479]
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