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[Study of structure-activity relationship in series of Gsb-106 analogues-dipeptide mimetics of brain-derived neurotrophic factor]. [Gsb-106脑源性神经营养因子双肽模拟物系列的构效关系研究]。
Pub Date : 2014-03-01
A V Tarasiuk, T A Gudasheva, N M Sazonova, P I Antipov, D V Kurilov, P Iu Povarnina, I O Logvinov, T A Antipova, S B Seredenin

In previous work we have obtained a dimeric dipeptide mimetic of 4th loop of BDNF - hexamethylenediamide bis-(N-monosuccinil-L-seryl-L-lysine) (GSB-106), having a neuroprotective activity in vitro in a concentration range 10(-5)-10(-8) M and an antidepressant activity in vivo at doses 0.1 and 1 mg/kg i.p. in rats. We have investigated the structural and functional relationships among analogues of GSB-106. Glycine scan was performed and a number of appropriate compounds were synthesized: GT-105 (here lysine is replaced by glycine), GT-107 (here serine is replaced by glycine), GT-106Ac (here monosuccinic radical is replaced by acetyl group). We have studied the dependence of activity of following compounds from the configuration of amino acid residues: GT-107D (D-enantiomer of the GT-107), GT-106DL (L-serine was replaced by D-serine), GT-106LD (L-lysine was replaced by D-lysine). The investigation of these compounds using the HT22 cell culture in conditions of oxidative stress has approved only two analogues of GSB-106 to have a neuroprotective effect: in the case of replacement of serine to glycine and of replacment of succinic radical to acetic group. A disappearance of this effect was observed in event of the replacement of lysine residue to glycine in GT-105, L-lysine residue to D-lysine and also by conversion of serine configuration. These results show that lysine residue is crucial for the neuroprotective activity of GSB-106. L-Configuration of the lysine and serine residues required. Configuration of lysine residue becomes critical in absence of serine side group. Thus, the the following fragment is a minimum pharmacophore of beta-turn of 4 loop of BDNF: HOOC-CH2-CH-CO-NH-(S)-CH(CH2OH)-CO-NH-(S)-CH((CH2)4NHz)-CO-NH-(CH2)3-. Only one (GT-106Ac) out of two analogues of GSB-106 with neuroprotective activity possesses antidepressant activity too. This fact indicates about a necessity of more stringent structural requirements for exposure of antidepressant activity. The results obtained can be useful for designing of new active mimetics of BDNE

在之前的工作中,我们已经获得了BDNF第4环的二聚二肽模拟物-六亚二胺双-(n -单琥珀酸-l -seryl- l-赖氨酸)(GSB-106),在体外浓度范围为10(-5)-10(-8)M时具有神经保护活性,在体内剂量为0.1和1 mg/kg时具有抗抑郁活性。我们研究了GSB-106类似物之间的结构和功能关系。进行甘氨酸扫描,合成了一些合适的化合物:GT-105(这里赖氨酸被甘氨酸取代),GT-107(这里丝氨酸被甘氨酸取代),GT-106Ac(这里单琥珀基被乙酰基取代)。我们研究了GT-107D (GT-107的d对映体)、GT-106DL (l -丝氨酸被d -丝氨酸取代)、GT-106LD (l -赖氨酸被d -赖氨酸取代)等化合物的氨基酸残基构型对活性的依赖性。在氧化应激条件下使用HT22细胞培养对这些化合物进行的研究已批准只有两种GSB-106类似物具有神经保护作用:在将丝氨酸替换为甘氨酸的情况下,以及将琥珀酸自由基替换为乙酸基的情况下。在GT-105中将赖氨酸残基替换为甘氨酸,将l -赖氨酸残基替换为d -赖氨酸以及将丝氨酸构型转化时,这种效应消失。这些结果表明,赖氨酸残基对GSB-106的神经保护活性至关重要。所需赖氨酸和丝氨酸残基的构型。赖氨酸残基的构型在没有丝氨酸侧基的情况下变得至关重要。因此,以下片段是BDNF 4环β匝最小药效团:HOOC-CH2-CH-CO-NH-(S)- ch (CH2OH)- co - nh -(S)- ch ((CH2)4NHz)- co - nh -(CH2)3-。GSB-106的两种类似物中只有一种(GT-106Ac)具有神经保护活性,也具有抗抑郁活性。这一事实表明,有必要对抗抑郁药物活性暴露进行更严格的结构要求。所得结果可为新型BDNE主动模拟物的设计提供参考
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引用次数: 0
Synthesis, insecticidal, and fungicidal screening of some new synthetic quinoline derivatives. 一些新的合成喹啉衍生物的合成及杀虫、杀真菌筛选。
Pub Date : 2014-03-01
M R E Aly, M M Ibrahim, A M Okael, Y A M H Gherbawy

This paper describes the synthesis of a series of quinolines graphted with hydrazones, pyrazoles, pyridazine, phthalazine, triazepinone, semicarbazide, and thiomorpholide moieties and four metal complexes. These derivatives were screened against Fusarium oxysporum and the red palm weevil (RPW) Rhynchophorus ferrugineus Oliver (coleopteran: Curculionidae) as palm pathogens. Only chlorinated quinolines were active against these organisms with hydrazones being good fungicides, while those modified with pyrazoles and pyrazines showed moderate insecticidal activity. A unique trihydroxylated hydrazone was active against both organisms, while another hydrazone, the most potent fungicide in this series, exhibited insecticidal activity only upon com- plexation with Zn2+ ions.

本文介绍了一系列以腙、吡唑、吡啶、酞嗪、三氮平酮、氨基脲、硫代烷和四种金属配合物为基体的喹啉类化合物的合成。这些衍生物对尖孢镰刀菌(Fusarium oxysporum)和红棕榈象(Rhynchophorus ferrugineus Oliver)作为棕榈病原体进行了筛选。只有氯代喹啉类对这些微生物有活性,腙类是较好的杀真菌剂,而吡唑类和吡嗪类修饰的杀虫剂具有中等的杀虫活性。一个独特的三羟基化腙对这两种生物都有活性,而另一个腙是该系列中最有效的杀菌剂,只有在与Zn2+离子复合时才表现出杀虫活性。
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引用次数: 0
[Development of methods for rapid test of staphylococcal enterotoxin A in food]. [食品中葡萄球菌肠毒素A快速检测方法的研究]。
Pub Date : 2014-03-01
I A Liubavina, F A Brovko, T I Valiakina, Iu V Vertiev, E V Grishin

Noninstrumental methods of qualitative rapid test for detection of staphylococcal enterotoxin A (SEA) in milk foods sample and brothof using immunochromatography (IC) and dot-assay has been developed. Monoclonal antibodies to SEA with colloidal gold forimmunochromatography; monoclonal antibodies to SEA with colloidal gold or biotinylated monoclonal antibodies and streptavidin-peroxidase conjugate for dot-assay were used to visualize the results. The detection limits, ng/mL: 10 (IC), 20 (dot-assay with antibody-colloidal gold), 10 (dot-assay with STR-HRP), 4 (ELISA). Time of assay, min: 25 (IC), 60 (dot-assay with antibody-colloidal gold), 70 (dot-assay with STR-HRPO, 150 (ELISA).

建立了乳食品样品和肉汤中葡萄球菌肠毒素A (SEA)的免疫层析和斑点法非仪器定性快速检测方法。SEA单克隆抗体胶体金免疫层析;用带胶体金的SEA单克隆抗体或生物素化单克隆抗体和链亲和素过氧化物酶偶联物进行点测定,将结果可视化。检测限分别为:10 (IC)、20(抗体胶体金斑点法)、10 (STR-HRP斑点法)、4 (ELISA法)。检测时间,min: 25 (IC), 60(抗体胶体金斑点法),70 (STR-HRPO斑点法),150 (ELISA)。
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引用次数: 0
Molecular cloning of a dehydration-responsive protein gene (MRD22) from mulberry, and determination of abiotic stress patterns of MRD22 gene expression. 桑树脱水反应蛋白基因MRD22的克隆及非生物胁迫下MRD22基因表达模式的测定。
Pub Date : 2014-03-01
Heng Wang, Zhaoyue Liu, Feng Li, Yuhua Wang, Rongjun Fang, Weiguo Zhao, Long Li

A full-length cDNA sequence coding for Dehydration-responsive protein gene of mulberry tree, which we designated was MRD22 (GenBank accession number: JQ804833) was cloned based on mulberry expressed sequence tags (ESTs). MRD22 is 1503 bp long, contains a 334 bp 5'-UTR (untranslated region) and a 563 bp 3'-UTR, encodes 201 amino acids with a predicted molecular weight of 54.28 kDa and an isoelectric point of 9.35. Phylogenetic analysis based on MRD22 sequences from different species showed that mulberry has close relationship with Populus trichocarpa, Ricinus communis, Camellia sinensis, Gossypium hirsutum, Gossypium barbadense and so on. The expression level of the MRD22 gene under conditions of drought, low temperature and salt stresses was quantified by qRT-PCR. The results show that the expression level changed significantly under the stress conditions compared to the normal growth environment. It helps us to get a better understanding of the molecular basis for signal transduction mechanisms underlying the stress response in mulberry.

利用桑树表达序列标签(ESTs)克隆了桑树脱水反应蛋白基因的全长cDNA序列,编号为MRD22 (GenBank登录号:JQ804833)。MRD22全长1503 bp,包含一个334 bp的5'-UTR(非翻译区)和一个563 bp的3'-UTR,编码201个氨基酸,预测分子量为54.28 kDa,等电点为9.35。基于不同种MRD22序列的系统发育分析表明,桑树与毛杨(Populus trichocarpa)、蓖麻(Ricinus communis)、山茶(Camellia sinensis)、绵棉(Gossypium hirsutum)、巴氏绵棉(Gossypium barbadense)等亲缘关系较近。采用qRT-PCR方法定量分析干旱、低温和盐胁迫下MRD22基因的表达水平。结果表明,与正常生长环境相比,胁迫条件下的表达量发生了显著变化。这有助于我们更好地了解桑树胁迫反应的信号转导机制的分子基础。
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引用次数: 0
[A new fluorescent analogue for the investigation of anandamide transport in cell cultures]. [一种新的荧光模拟物,用于研究细胞培养中anandamide运输]。
Pub Date : 2014-03-01
N M Gretskaia, M G Akimov, V V Bezuglov

For the first time a new fluorescent analogue of anadamide incorporating BODIPY®-FL-fluorophore, attached to arachidonic acid via 2,2'-(ethylenedioxy)-bis(ethylenediamine), was prepared. Using rat glioma C6 cells it was demonstrated that the fluorescent analogue is a substrate of the cellular anandamide uptake system (Km 4.5 ± 0.9 µM, Vmax 20 ± 1 amol/(min x cell)).

首次制备了一种新的含BODIPY®- fl -荧光基团的阿纳达胺荧光类似物,通过2,2'-(乙二氧基)-二(乙二胺)连接到花生四烯酸。在大鼠胶质瘤C6细胞中,荧光类似物被证明是细胞anandamide摄取系统的底物(Km 4.5±0.9µM, Vmax 20±1 amol/(min x细胞))。
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引用次数: 0
[Synthesis of a fluorescent analog of methotrexate lipophilic prodrug]. [甲氨蝶呤亲脂前药荧光模拟物的合成]。
Pub Date : 2014-01-01
Yu V Ylasenko, A S Alekseeva, E L Vodovozova

A fluorescent analog of the lipophilic prodrug of antitumor agent methotrexate has been synthesized. The conjugate consists of a residue of rac-1-[13-(Me4-BODIPY-8)tridecanoyl]-2-oleoylglycerol connected to methotrexate by ester bond via β-Ala-N-carbonylmethylene linker (Me4-BODIPY-8,4,4-difluoro-1,3,5,7-tetramethyl-4-bora-3a,4a-diaza-s-indacen-8-yl). The probe is designed for incorporation in the membrane of liposomal vehicle to study a mechanism of interaction with tumor cells and an intracellular traffic.

合成了抗肿瘤药物甲氨蝶呤亲脂前药的荧光类似物。该缀合物由rac-1-[13-(Me4-BODIPY-8)三烷醇]-2-油基甘油残基通过β- ala - n-羰基亚甲基连接物(me4 - bodipy -8,4,4-二氟-1,3,5,7-四甲基-4-bora-3a,4 -diaza-s-indacen-8-基)与甲氨蝶呤通过酯键连接而成。该探针被设计用于整合到脂质体载体的膜中,以研究与肿瘤细胞相互作用和细胞内运输的机制。
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引用次数: 0
Disordered binding regions of Ewing's sarcoma fusion proteins. 尤文氏肉瘤融合蛋白的无序结合区。
Pub Date : 2014-01-01
R Todorova

A relationship was found between the Amino acid (AA) composition, Intrinsic Protein Disorder (IPD) and Protein Binding Regions (PBRs) of the functional regions of Ewing's sarcoma protein (EWS) and oncogenic EWS fusion proteins (EFPs). EWS has high IPD and 64% predicted Disordered Binding Regions (DBRs) by ANCHOR. The native Transcription Factors, fused to EWS Activation Domain (EAD) in EFPs, show high DBRs in N-terminal domain and relatively low in C-terminal domain. EFPs oncogenic function is related to IPD and PBRs probabilities, high around breakpoint and decreased in the fused Transcription Factor. The increased IPD in EAD around (AA 82), and the small RBRs around (AAs (50-60) and 100) are consistent with the reported physical interactions with RNA Polymerase II subunits. The AAs (228-264) of EWS, interacting with ZFM1 (SF1), correspond to two peaks of DBRs by Anchor and high IPD by IUPred. The IQ domain of EAD (AAs 258-280) that is phosphorylated by PKC and interacts with calmodulin, has high IPD and DBRs probability. The Ser266, conserved site of PKC phosphorylation, is situated in DBR and IPD region with about 100% probability. The small PBRs found in the EAD correspond to important physical protein-protein interactions, confirmed by experimental data. Thus regions of EWS and EFPs, included in functional interactions with other partners, are enriched of Protein Binding Regions by ANCHOR. The development of IPD- and PBRs-related, EWS-FLI1-directed specific therapies will help the design of antitumor agents against ESFT because of high patient mortality in cases of meta- static disease.

发现Ewing肉瘤蛋白(EWS)功能区域的氨基酸(AA)组成、内在蛋白紊乱(IPD)和蛋白结合区(PBRs)与致癌性EWS融合蛋白(EFPs)之间存在相关性。EWS的IPD高,锚定预测的DBRs为64%。在EFPs中融合到EWS激活域(EAD)的天然转录因子在n端域表现出较高的dbr,在c端域表现出相对较低的dbr。EFPs的致癌功能与IPD和PBRs概率有关,在断点附近高,在融合转录因子中降低。在EAD (AA 82)附近IPD增加,在AAs(50-60)和100附近rbr小,这与报道的RNA聚合酶II亚基的物理相互作用一致。EWS的AAs(228-264)与ZFM1 (SF1)相互作用,对应Anchor的两个dbr峰和iuppred的高IPD峰。EAD的IQ结构域(AAs 258-280)被PKC磷酸化并与钙调蛋白相互作用,具有较高的IPD和dbr概率。PKC磷酸化的保守位点Ser266位于DBR和IPD区,概率约为100%。实验数据证实,在EAD中发现的小pbr与重要的物理蛋白质-蛋白质相互作用相对应。因此,EWS和EFPs的区域,包括与其他伙伴的功能相互作用,被锚蛋白结合区富集。IPD和pbrs相关、ews - fli1导向的特异性疗法的发展将有助于设计针对ESFT的抗肿瘤药物,因为ESFT在meta- static病例中患者死亡率很高。
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引用次数: 0
Synthesis, insecticidal, and fungicidal screening of some new synthetic quinoline derivatives. 一些新的合成喹啉衍生物的合成及杀虫、杀真菌筛选。
Pub Date : 2014-01-01 DOI: 10.7868/S013234231402002X
M. Aly, M. Ibrahim, A. M. Okael, Y. Gherbawy
This paper describes the synthesis of a series of quinolines graphted with hydrazones, pyrazoles, pyridazine, phthalazine, triazepinone, semicarbazide, and thiomorpholide moieties and four metal complexes. These derivatives were screened against Fusarium oxysporum and the red palm weevil (RPW) Rhynchophorus ferrugineus Oliver (coleopteran: Curculionidae) as palm pathogens. Only chlorinated quinolines were active against these organisms with hydrazones being good fungicides, while those modified with pyrazoles and pyrazines showed moderate insecticidal activity. A unique trihydroxylated hydrazone was active against both organisms, while another hydrazone, the most potent fungicide in this series, exhibited insecticidal activity only upon com- plexation with Zn2+ ions.
本文介绍了一系列以腙、吡唑、吡啶、酞嗪、三氮平酮、氨基脲、硫代烷和四种金属配合物为基体的喹啉类化合物的合成。这些衍生物对尖孢镰刀菌(Fusarium oxysporum)和红棕榈象(Rhynchophorus ferrugineus Oliver)作为棕榈病原体进行了筛选。只有氯代喹啉类对这些微生物有活性,腙类是较好的杀真菌剂,而吡唑类和吡嗪类修饰的杀虫剂具有中等的杀虫活性。一个独特的三羟基化腙对这两种生物都有活性,而另一个腙是该系列中最有效的杀菌剂,只有在与Zn2+离子复合时才表现出杀虫活性。
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引用次数: 1
Site selectivity in reactions of hydrazonoyl halides with heterocycles containing amino and thione groups leading to fused heterocycles of potential antimicrobial activity. 酰腙卤化物与含氨基和硫酮基团的杂环反应的位点选择性导致具有潜在抗菌活性的融合杂环。
Pub Date : 2014-01-01
M E A Khalifa, M A Amin, M A N Mosselhi

Reaction of hydrazonoyl halides with 6-(benzylidenamino)-2-thioxo-2,3-dihydro-1H-pyrimidin-4-one and 2,3-diaminoquinazolin-4-one site-selectively afforded 3-substituted-7-(benzylidenamino)-1-phenyl-[1,2,4]triazolo[4,3-a]-pyrimidin-5(1H)-ones, [1,2,4,5]tetrazino[6,1-b]quinazolin-6(4H)-one, and 3-methyl-2-(4-substituted-phenylhydrazo)-[1,2,4]triazino[3,2-b]quinazolin-10-ones in good yields. The structures of the newly synthesized compounds were elucidated by chemical evidence and their IR, 1H, 13C NMR, and MS spectra. Furthermore, some of the products were screened against different strains of bacteria and fungi.

腙酰卤化物与6-(苄基氨基)-2-硫氧基-2,3-二氢-1H-嘧啶-4- 1和2,3-二氨基喹唑啉-4- 1位点选择性反应,得到3-取代-7-(苄基氨基)-1-苯基-[1,2,4]三唑啉[4,3-a]-嘧啶-5(1H)- 1,[1,2,4,5]四氮基[6,1-b]喹唑啉-6(4H)- 1和3-甲基-2-(4-取代-苯腙)-[1,2,4]三氮基[3,2-b]喹唑啉-10- 1,收率高。通过化学证据和IR、1H、13C NMR和MS谱对新合成化合物的结构进行了鉴定。此外,还对部分产品进行了抗细菌和真菌的筛选。
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引用次数: 0
Comparison of QSAR models based on combinations of genetic algorithm, stepwise multiple linear regression, and artificial neural network methods to predict Kd of some derivatives of aromatic sulfonamides as carbonic anhydrase II inhibitors. 基于遗传算法、逐步多元线性回归和人工神经网络方法联合预测芳香磺胺类碳酸酐酶II抑制剂衍生物Kd的QSAR模型比较
Pub Date : 2014-01-01
Afshin Maleki, Hiua Daraei, Loghman Alaei, Aram Faraji

Four stepwise multiple linear regressions (SMLR) and a genetic algorithm (GA) based multiple linear regressions (MLR), together with artificial neural network (ANN) models, were applied for quantitative structure-activity relationship (QSAR) modeling of dissociation constants (Kd) of 62 arylsulfonamide (ArSA) derivatives as human carbonic anhydrase II (HCA II) inhibitors. The best subsets of molecular descriptors were selected by SMLR and GA-MLR methods. These selected variables were used to generate MLR and ANN models. The predictability power of models was examined by an external test set and cross validation. In addition, some tests were done to examine other aspects of the models. The results show that for certain purposes GA-MLR is better than SMLR and for others, ANN overcomes MLR models.

采用4种逐步多元线性回归(SMLR)和基于遗传算法(GA)的多元线性回归(MLR),结合人工神经网络(ANN)模型,对62种ArSA衍生物作为人碳酸酐酶II (HCA II)抑制剂的解离常数(Kd)进行定量构效关系(QSAR)建模。采用SMLR和GA-MLR两种方法筛选出最佳的分子描述子子集。这些选定的变量被用来生成MLR和ANN模型。通过外部测试集和交叉验证来检验模型的可预测性。此外,还进行了一些测试来检查模型的其他方面。结果表明,对于某些目的,GA-MLR优于SMLR,而对于其他目的,ANN则优于MLR模型。
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引用次数: 0
期刊
Bioorganicheskaia khimiia
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