Design, synthesis and biological evaluation of fluorescent ligands for MT1 and/or MT2 melatonin receptors

G. Viault; S. Poupart; S. Mourlevat; C. Lagaraine; S. Devavry; F. Lefoulon; V. Bozon; L. Dufourny; P. Delagrange; G. Guillaumet; F. Suzenet

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Design, synthesis and biological evaluation of fluorescent ligands for MT1 and/or MT2 melatonin receptors

机译：MT1和/或MT2褪黑素受体荧光配体的设计，合成和生物学评价

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Fluorescent melatoninergic ligands have been designed by associating the 4-azamelatonin ligands with different fluorophores. The ligands show good affinities for MT _(1) and/or MT _(2) receptors and substitution of the fluorophore at positions 2 or 5 of the azamelatonin core had a direct impact on the MT receptors selectivity while grafting the fluorophores on position N1 produced fluorescent ligands with good affinities for both MT _(1) /MT _(2) receptors. The optimal position N-1, C-2 or C-5 on the 4-azamelatonin ligand appeared strongly dependent upon the nature of the fluorophore itself.

机译：通过将4-二胺蛋白配体与不同的荧光团相关联设计了荧光褪黑素能配体。配体对Mt _（1）和/或Mt _（2）的受体显示出良好的亲和力，并且在阿凡蛋白酶核的位置2或5处取代荧光团的荧光团对Mt受体的选择性直接影响，同时嫁接荧光团在位置N1上的荧光团产生具有良好亲和力的荧光配体，适用于MT _（1）/ mT _（2）受体。在4-αzamelonin配体上的最佳位置N-1，C-2或C-5非常依赖于荧光团本身的性质。

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《RSC Advances》 |2016年第67期|共14页
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G. Viault; S. Poupart; S. Mourlevat; C. Lagaraine; S. Devavry; F. Lefoulon; V. Bozon; L. Dufourny; P. Delagrange; G. Guillaumet; F. Suzenet;
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1. Design, synthesis and biological evaluation of fluorescent ligands for MT1 and/or MT2 melatonin receptors [J] . Viault G., Poupart S., Mourlevat S., RSC Advances . 2016,第67期

机译：MT1和/或MT2褪黑激素受体的荧光配体的设计，合成和生物学评估
2. Synthesis and pharmacological evaluation of dual ligands for melatonin (MT1/MT2) and serotonin 5-HT2C receptor subtypes (II) [J] . Ettaoussi Mohamed, Peres Basile, Errazani Aicha, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2015,第Null期

机译：褪黑素（MT1 / MT2）和5-羟色胺5-HT2C受体亚型的双重配体的合成和药理评估（II）
3. Preferential formation of MT1/MT2 melatonin receptor heterodimers with distinct ligand interaction properties compared with MT2 homodimers. [J] . Ayoub MA, Levoye A, Delagrange P, Molecular pharmacology. . 2004,第2期

机译：与MT2同型二聚体相比，具有独特的配体相互作用特性的MT1 / MT2褪黑激素受体异二聚体的优先形成。
4. Design, Synthesis and Biological Evaluation of Multivalent Ligands with μ/δ Opioid Agonist (μ-preferring) /NK-1 Antagonist Activities [C] . Aswini Kumar Giri, Qiong Xie, Christopher R. Apostol American Peptide Symposium . 2013

机译：多价配体的设计，合成和生物学评价，具有μ/δOpiOd激动剂（μ-opmoldring）/ NK-1拮抗剂活性
5. Design and synthesis of molecular probes to modulate cell membrane permeation: I. Design, synthesis, and biological evaluation of novel chicoric acid analogues as inhibitors of HIV-1 integrase. II. Design, synthesis, and biological evaluation of novel estradiol analogues targeting the membrane estrogen receptor. [D] . Charvat, Trevor Thomas. 2004

机译：设计和合成的分子探针，可调节细胞膜的渗透性：I.设计，合成和生物评价作为抗HIV-1整合酶抑制剂的新型菊苣酸类似物。二。针对膜雌激素受体的新型雌二醇类似物的设计，合成和生物学评估。
6. Design Synthesis and Biological evaluation of Multifunctional Ligands Targeting Opioid and Bradykinin 2 Receptors [O] . Srinivas Deekonda, David Rankin, Peg Davis, -1

机译：靶向阿片样物质和缓激肽2受体的多功能配体的设计合成和生物学评估
7. Synthesis, Biological Evaluation, and Utility of Fluorescent Ligands Targeting the μ-Opioid Receptor [O] . Luke S. Schembri, Leigh A. Stoddart, Stephen J. Briddon, 2015

机译：靶向μ-ApiOID受体的荧光配体的合成，生物学评价和效用

Design, synthesis and biological evaluation of fluorescent ligands for MT1 and/or MT2 melatonin receptors

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