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研究了七元瓜环(Q[7])和八元瓜环(Q[8])与盐酸雷尼替丁(RH)的包合作用及包合物的体外药物缓释性能.采用紫外-可见光谱法测定了体系的包合比、包合稳定常数和药物累积释放度;用1H NMR技术考察了体系主-客体的包合作用.结果表明,Q[7]和Q[8]与RH在酸性及中性条件下均能发生1∶1包合作用,包合稳定常数分别为1.21×104和2.06×104 L/mol;在碱性条件下则不发生包合作用.原药RH,Q[7]-RH及Q[8]-RH包合物在人工胃液(pH=1.2)中的60 min累积释放度分别为89.1%,56.6%和38.4%;而在人工肠液(pH=6.8)中三者的60 min累积释放度分别为90.2%,58.7%和38.0%.实验结果表明,Q[7]及Q[8]包合对RH有明显的体外缓释作用. 相似文献
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[structure: see text] Cucurbits come in a variety of sizes, shapes, and colors. We present a building block approach that allows the tailor-made synthesis of CB[5], CB[6], and CB[7] analogues whose sizes, shapes, and colors differ from those of the known CB[n]. 相似文献
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八元瓜环与抗癌药物甲氨蝶呤的超分子相互作用 总被引:1,自引:0,他引:1
利用紫外吸收光谱法考察了八元瓜环(Q[8])与抗癌药物甲氨蝶呤(MTX)的相互作用;同时研究了甲氨蝶呤的不同质子化形式及体系温度对相互作用的影响;计算了相应的稳定常数及热力学参数等.实验结果表明,Q[8]与MTX作用比为1∶1,包结平衡常数为(7.64±1.52)×104 L/mol;龄前热力学参数测定结果表明,上述主... 相似文献
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瓜环的合成及其连续分离 总被引:2,自引:0,他引:2
苷脲和多聚甲醛在盐酸存在下反应,合成了多种聚合度的混合瓜环{Q[n],n=5~8};利用其在盐酸中的溶解性差异,通过连续分离得到了单聚合度的Q[5]~Q[8],其结构经1H NMR表征. 相似文献
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The interaction between cucurbit[8]uril(Q[8]) and oroxin B(ORB) was investigated by UV-visible(UV-Vis) spectroscopy, isothermal titration calorimetry(ITC), mass spectrum(MS) and nuclear magnetic resonance(NMR) spectroscopy. The results showed that ORB formed a 2:1 inclusion complex with Q[8] with a binding constant of 8.266×105 L2·mol-2. ORB had good scavenging ability for 2,2'-azinobis-(3-ethylbenzthiazoline-6-sulphonate)(ABTS) free radicals(IC50=5.74 μmol/L) and the addition of Q[8] did not significantly affect the antioxidant activity of ORB(IC50=5.76 μmol/L). A phase solubility experiment revealed a 1.86-fold increase in the solubility of ORB when c(Q[8])=100 μmol/L. In vitro drug release experiments showed that the release rate for ORB@Q[8] complex was lower than that of ORB in artificial intestinal juice, and higher than that of ORB in artificial gastric juice. 相似文献
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用核磁共振氢谱和紫外-可见光谱滴定法考察了葫[n]环联脲(Cucurbit[n]uril,n=5,6,7,8)与对甲苯重氮氟硼酸盐和4,4′-联苯二重氮氟硼酸盐的配位情况,并用曲线拟合求得形成的包结配合物的稳定常数.结果表明,不同空腔的葫[n]环联脲对不同尺寸的重氮氟硼酸盐具有很显著的选择性包结作用.在相同条件下,与葫[6]环联脲相比,葫[7]环联脲更易于容纳苯环.同时,随着酸性的增强,葫[n]环联脲上的脲羰基质子化程度加大,使得其配位能力有所减弱. 相似文献
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Melamine diamine 1 is able to displace CB[5] from the CB[10].CB[5] complex resulting in CB[10].12 and precipitated CB[5].1. We were able to isolate free CB[10] by treatment of CB[10].1 with acetic anhydride followed by washing with MeOH, DMSO, and water. The spacious cavity of CB[10] is able to complex large guests, including a cationic calix[4]arene derivative in its 1,3-alternate form (CB[10].1,3-alt-3). The addition of adamantane carboxylic acid (4) to CB[10].3 triggers a conformational change during the formation of termolecular complex CB[10].cone-3.4. 相似文献
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Wheate NJ Buck DP Day AI Collins JG 《Dalton transactions (Cambridge, England : 2003)》2006,(3):451-458
The encapsulation of cisplatin by cucurbit[7]uril (Q[7]) and multinuclear platinum complexes linked via a 4,4'-dipyrazolylmethane (dpzm) ligand by Q[7] and cucurbit[8]uril (Q[8]) has been studied by NMR spectroscopy and molecular modelling. The NMR studies suggest that some cisplatin binds in the cucurbituril cavity, while cis-[PtCl(NH3)2(H2O)]+ only binds at the portals. Alternatively, the dpzm-linked multinuclear platinum complexes are quantitatively encapsulated within the cavities of both Q[7] and Q[8]. Upon encapsulation, the non-exchangeable proton resonances of the multinuclear platinum complexes show significant upfield shifts in 1H NMR spectra. The H3/H3* resonances shift upfield by 0.08 to 0.55 ppm, the H5/H5* shift by 0.9 to 1.6 ppm, while the methylene resonances shift by 0.74 to 0.88 ppm. The size of the resonance shift is dependent on the cavity size of the encapsulating cucurbituril, with Q[7] encapsulation producing larger shifts than Q[8]. The upfield shifts of the dpzm resonances observed upon cucurbituril encapsulation indicate that the Q[7] or Q[8] is positioned directly over the dpzm linking ligand. The terminal platinum groups of trans-[{PtCl(NH3)2}2 mu-dpzm]2+ (di-Pt) and trans-[trans-{PtCl(NH3)2}2-trans-{Pt(dpzm)2(NH3)2}]4+ (tri-Pt) provide a barrier to the on and off movement of cucurbituril, resulting in binding kinetics that are slow on the NMR timescale for the metal complex. Although the dpzm ligand has relatively few rotamers, encapsulation by the larger Q[8] resulted in a more compact di-Pt conformation with each platinum centre retracted further into each Q[8] portal. Encapsulation of the hydrolysed forms of di-Pt and tri-Pt is considerably slower than for the corresponding Cl forms, presumably due to the high-energy cost of passing the +2 platinum centres through the cucurbituril portals. The results of this study suggest that cucurbiturils could be suitable hosts for the pharmacological delivery of multinuclear platinum complexes. 相似文献
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《Angewandte Chemie (Weinheim an der Bergstrasse, Germany)》2017,129(41):12788-12792
Stimuli‐responsive molecular containers are of great importance for controlled drug delivery and other biomedical applications. A new type of acid labile acyclic cucurbit[n ]uril (CB[n ]) molecular containers is presented that can degrade and release the encapsulated cargo at accelerated rates under mildly acidic conditions (pH 5.5–6.5). These containers retain the excellent recognition properties of CB[n ]‐type hosts. A cell culture study demonstrated that the cellular uptake of cargos could be fine‐tuned by complexation with different containers. The release and cell uptake of cargo dye was promoted by acidic pH. 相似文献
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In contrast to the high yield formation of cucurbit[n]uril (CB[n]) from a 1:2 ratio of glycoluril to formaldehyde, the condensation of glycoluril with less than 2 equiv of formaldehyde delivers a reaction mixture that contains glycoluril oligomers (2-6) and CB[n] compounds that lack one or more methylene bridges known as nor-seco-cucurbit[n]urils (ns-CB[n]). In this paper we report the chromatographic purification of C-shaped glycoluril oligomers (dimer-hexamer), their characterization in solution, and their X-ray crystal structures. Quite interestingly, despite being acyclic glycoluril pentamer 5 and hexamer 6 retain the ability to bind to guests typical of CB[6] but are also able to expand their cavity to accommodate larger guests like cationic adamantane derivatives. We performed product resubmission experiments with glycoluril oligomers 2-6 and found preferences for the formation of specific ring sizes during CB[n] formation. A comprehensive mechanistic scheme is proposed that accounts for the observed formation of 2-6 and ns-CB[n]. Overall, the experiments establish that a step-growth cyclo-oligomerization process operates during CB[n] formation. 相似文献
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利用高效液相色谱法考察七、八元瓜环对苯丁酸氮芥稳定性的影响. 结果表明在37 ℃, pH 2.0盐酸溶液中, 七元瓜环的浓度为2.0×10-4 mol•L-1时可使苯丁酸氮芥的稳定性提高近4倍, 而八元瓜环浓度为8.0×10-5 mol•L-1时可使苯丁酸氮芥的稳定性提高近15倍|相溶解度法的研究则证实在苯丁酸氮芥分解速度最低的条件下(3 ℃, pH 2.0盐酸溶液中), 1.0×10-3 mol•L-1浓度七元瓜环的存在可使苯丁酸氮芥的溶解度增加36倍, 八元瓜环浓度为1.0×10-4 mol• L-1时可增加6倍|通过紫外吸收光谱法考察了在不同pH条件下, 七、八元瓜环与苯丁酸氮芥的相互作用, 计算了瓜环与苯丁酸氮芥相互作用的稳定常数和作用比例, 并与动力学的结果进行了比较, 同时用核磁进一步验证了瓜环与苯丁酸氮芥的相互作用, 给出了可能的相互作用模式. 相似文献
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[reaction: see text] The synthesis of cucurbit[n]uril analogues (18, 19, (+/-)-20, 33, 34, 35, 36, and 37) is presented. These CB[5], CB[6], and CB[7] analogues all contain bis(phthalhydrazide) walls that are incorporated into the macrocycle. The tailor-made synthesis of these CB[n] analogues proceeds by the condensation of the appropriate bis(electrophile) (4, 7, or 9) with bis(phthalhydrazide) (17), which delivers the CB[6] and CB[7] analogues in good yield, whereas the CB[5] analogue is formed in low yield. To improve the solubility characteristics of the CB[n] analogues for recognition studies in water or organic solution, the CO2Et groups were transformed to CO2H and CO2(CH2)9CH3 groups. On the basis of the results of product resubmission experiments, we conclude that these macrocycles are kinetic products. To help rationalize the good yields obtained in the CB[6] and CB[7] analogue macrocyclization reactions, we performed mechanistic studies of model methylene bridged glycoluril dimers, which suggest an intramolecular isomerization during CB[n] analogue formation. 相似文献
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Simin Liu Xiaojun Wu Zixiang Huang Junhua Yao Feng Liang Chengtai Wu 《Journal of inclusion phenomena and macrocyclic chemistry》2004,50(3-4):203-207
1H-NMR spectroscopic analysis indicates that cucurbit[7]uril can form a stable inclusion complex with 1,6-hexanediamine, while cucurbit[5]uril cannot form pseudorotaxane with 1,6-hexanediamine under our experimental conditions. This was confirmed by the crystal structure of the complex. The cavity of cucurbit[8]uril seems to be large for binding 1,6-hexanediamine efficiently. And a simple, mild, high-yield (>80%) method has been described for the synthesis of rotaxanes through the self-assembly of pseudorotaxanes of cucurbit[n]uril (n=6, 7)/1, 6-hexanediamine and sodium tetraphenylborate. The obtained rotaxanes are held intact solely by noncovalent interactions, and are characterized by elemental analysis, 1H-NMR, ESI-MS and MALDI-TOF MS. 相似文献
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Dr. Ji Liu Dr. Cindy Soo Yun Tan Prof. Oren A. Scherman 《Angewandte Chemie (International ed. in English)》2018,57(29):8854-8858
Supramolecular building blocks, such as cucurbit[n]uril (CB[n])‐based host–guest complexes, have been extensively studied at the nano‐ and microscale as adhesion promoters. Herein, we exploit a new class of CB[n]‐threaded highly branched polyrotaxanes (HBP‐CB[n]) as aqueous adhesives to macroscopically bond two wet surfaces, including biological tissue, through the formation of CB[8] heteroternary complexes. The dynamic nature of these complexes gives rise to adhesion with remarkable toughness, displaying recovery and reversible adhesion upon mechanical failure at the interface. Incorporation of functional guests, such as azobenzene moieties, allows for stimuli‐activated on‐demand adhesion/de‐adhesion. Macroscopic interfacial adhesion through dynamic host–guest molecular recognition represents an innovative strategy for designing the next generation of functional interfaces, biomedical devices, tissue adhesives, and wound dressings. 相似文献
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