Structure-activity relationship of wedelolactone analogues: structural requirements for inhibition of Na+, K+ -ATPase and binding to the central benzodiazepine receptor.

Pocas ES; Lopes DV; da Silva AJ; Pimenta PH; Leitao FB; Netto CD; Buarque CD; Brito FV; Costa PR; Noel F

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Structure-activity relationship of wedelolactone analogues: structural requirements for inhibition of Na+, K+ -ATPase and binding to the central benzodiazepine receptor.

机译：Wedelolactone类似物的结构-活性关系：抑制Na +，K + -ATPase和与中央苯并二氮杂receptor受体结合的结构要求。

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Coumestans 2a-i, bearing different patterns of substitution in A- and D-rings, were synthesized and evaluated as inhibitors of kidney Na+, K+ -ATPase and ligands for the central benzodiazepine (BZP) receptor. The presence of a hydroxyl group in position 2 favours the effect on Na+, K+ -ATPase but decreases the affinity for the BZP receptor, allowing the design of more selective molecules than the natural wedelolactone. On the other hand, the presence of a catechol in ring D is important for the effect on both molecular targets.

机译：合成了在A环和D环上具有不同取代模式的Coumestans 2a-i，并将其作为肾脏Na +，K + -ATPase和中央苯二氮卓（BZP）受体配体的抑制剂进行评估。 2位上羟基的存在有利于对Na +，K + -ATP酶的作用，但降低了对BZP受体的亲和力，从而允许设计比天然韦德尔内酯更具选择性的分子。另一方面，D环中邻苯二酚的存在对于对两个分子靶的影响都很重要。

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《Bioorganic and Medicinal Chemistry》 |2006年第23期|P.7962-7966|共5页
作者
Pocas ES; Lopes DV; da Silva AJ; Pimenta PH; Leitao FB; Netto CD; Buarque CD; Brito FV; Costa PR; Noel F;
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作者单位

Departamento de Farmacologia Basica e Clinica, Instituto de Ciencias Biomedicas, Universidade Federal do Rio de Janeiro, RJ 21941-590, Brazil.;

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原文格式 PDF
正文语种 eng
中图分类基础医学;
关键词
Sodium measurement; Potassium measurement; Adenosinetriphosphatase; wedelolactone; 腺苷三磷酸酶;

机译：Sodium measurement;Potassium measurement;Adenosinetriphosphatase;wedelolactone;腺苷三磷酸酶;

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1. Structure-activity relationship of wedelolactone analogues: structural requirements for inhibition of Na+, K+ -ATPase and binding to the central benzodiazepine receptor. [J] . Pocas ES, Lopes DV, da Silva AJ, Bioorganic and medicinal chemistry . 2006,第23期

机译：Wedelolactone类似物的结构-活性关系：抑制Na +，K + -ATPase并与中央苯并二氮杂receptor受体结合的结构要求。
2. Quantitative structure-activity relationship studies of a series of non-benzodiazepine structural ligands binding to benzodiazepine receptor. [J] . Xia B, Ma W, Zheng B, European Journal of Medicinal Chemistry: Chimie Therapeutique . 2008,第7期

机译：一系列与苯并二氮杂receptor受体结合的非苯并二氮杂structural结构配体的定量构效关系研究。
3. Structure-activity relationship studies of SEN12333 analogues: Determination of the optimal requirements for binding affinities at alpha 7 nAChRs through incorporation of known structural motifs [J] . Beinat Corinne, Reekie Tristan, Banister Samuel D., European Journal of Medicinal Chemistry: Chimie Therapeutique . 2015,第Null期

机译：SEN12333类似物的构效关系研究：通过掺入已知的结构基序，确定对α7nAChRs的结合亲和力的最佳要求
4. Distinct effects of Q925 mutation on intracellular and extracellular Na+ and K+ binding to the Na+ K+-ATPase [O] . Hang N. Nielsen, Kerri Spontarelli, Rikke Holm, -1

机译：Q925突变对细胞内和细胞外Na +和K +与Na +K + -ATPase结合的不同影响
5. Evidence for a Mg2+-Induced Conformational Change at the ATP-Binding Site of (Na+ + K+)-ATPase Demonstrated with a Photoreactive ATP-Analogue [O] . Gerold REMPETERS, Wilhelm SCHONER 1981

机译：用于（Na + + k +） - ATP酶的ATP结合位点的MG2 +-诱导的构象变化的证据 - 用光反应性ATP - 类似物证明

Structure-activity relationship of wedelolactone analogues: structural requirements for inhibition of Na+, K+ -ATPase and binding to the central benzodiazepine receptor.

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