交联聚苯乙烯固载聚乙二醇树脂（PEG）含量与活性的依赖关系研究

将具有不同ＰＥＧ含量的交联聚苯乙烯固载聚乙二醇树脂用于催化环已稀的二氯卡宾加成和乙酰苯胺的Ｎ－丁基化反应，发现树脂ＰＥＧ含量与催化剂活性之间存在的依赖关系。通过测定不同ＰＥＧ含量的树脂分别在水和甲苯中的溶胀系数，用树脂亲油－亲水性的变化规律，解释树脂活性与ＰＥＧ含量之间的依赖关系。     

含偶氮苯生色团的聚醚的合成与热致液晶性质

β－氯乙基缩水甘油醚（ＧＣＥ）和ＧＣＥ／羟丁基乙烯基醚（ＨＢＶＥ）分别通过阳离子聚合、光引发共聚合,获得两种聚醚,然后再分别与４－硝基－４’－羟基偶氦苯（ＮＨＡ）反应,制备了两种侧链含偶氦苯生色团的液晶聚合物（ＰＡＥＧ、ＰＡＶ）。用ＦＴＩＲ、＾１Ｈ－ＮＭＲ和ＥＡ对其化学结构及生色团含量进行了表征,以ＰＯＭ,ＤＳＣ、ＴＧＡ和ＷＡＸＤ对聚合物介晶相转变温度、织构、热稳定性及相行为进行了研究。结果表明,     

三羟甲基十一烷的合成与表征

三羟甲基烷烃是用于醇酸树脂、聚氨酯树脂、表面活性剂、合成润滑油等的原料[1-3].三羟甲基十一烷(化学结构见图1)作为三羟甲基烷烃中直碳链最长的一员,不仅具有亲水性(分子中含三个亲水基),而且具有疏水性(含一个长直碳链亲油基),因此可用作表面活性剂.不仅如此,与同样用作乳化剂的一般高级脂肪醇(如十六烷醇)相比,可以在化妆品用的乳液中加入三羟甲基十一烷作乳化剂,以降低乳液的黏度,防止乳液中由于大量加入高级脂肪醇而导致产品黏度过高以至不能在皮肤上被充分涂抹开的状况发生[4].为制备智能芳香缓释型聚氨酯微胶囊壳材[5],需要设计聚氨酯的分子结构中含有能与相变石腊和油溶性香料有良好相容性的疏水链(三羟甲基十一烷与六亚甲基二异氰酸酯的加成物).因此,本文合成并表征了三羟甲基十一烷.     

选择性接聚乙二醇枝聚醚聚酯的合成及其血液相容性

水解α－甲基－ω（２，３－环氧）丙基聚乙二醇（Ⅱ）得到接有聚乙二醇（ＰＥＧ）枝的丙二醇（Ⅲ），用其与对苯二甲酰氯及聚丁二醇反应制得在硬链段接有ＰＥＧ枝的聚醚聚酯（Ｈ－ＰＥＥｓ），以四氢呋喃与Ⅱ进行正离子开环共聚合制得每他链接有１．２５个ＰＥＧ枝的聚丁二醇（ＩＶ），用Ⅳ合成了在软链上接ＰＥＧ枝的聚醚聚酯（Ｓ－ＰＥＥｓ），不同位置接权的ＰＥＥｓ亲水性均较母体明显改进，抗凝血性则以Ｈ－ＰＥＥｓ改进显著。     

选择性接聚乙烯醇枝聚醚氨酯的合成及其血液相容性

合成了α－甲基，ω－（２，３－环氧丙基）－聚乙二醇醚（Ⅱ）．经水解得到悬挂聚乙二醇（ＰＥＧ）枝的丙二醇－２，３（Ⅲ）．用二元醇（Ⅲ）为扩链剂制得了在硬链段上接有ＰＥＧ枝的聚醚氨酯（Ｈ－ＰＥＵ）．以四氢呋喃与少量大分子单体（Ⅱ）进行正离子开环共聚合制得每个链接有约１．３个ＰＥＧ枝的聚丁二醇（Ⅳ），用以合成了在软链段上接有ＰＥＧ枝的聚醚氨酯（Ｓ－ＰＥＵ）．ＥＳＣＡ及抗凝血性研究结果表明，不同位置接枝的ＰＥＵ，其表面都有明显的聚醚链段富集．Ｓ－ＰＥＵ抗凝血复钙时间只比未接枝者增长约２０％，而Ｈ－ＰＥＵ则增约一倍，比Ｓ－ＰＥＵ增约６０％．随ＰＥＧ最增大，复钙时间增长．     

聚丙交酯/聚乙二醇多嵌段共聚物的合成及其性能

聚丙交酯 (ＰＬＬＡ)由于具有良好的生物降解性和生物相容性 ,在医学领域已经得到了广泛的临床应用 ,近来又被制备成细胞支架大量应用于组织工程中[1,2 ] ,但由于其疏水性而造成细胞亲和性不好 .聚乙二醇 (ＰＥＧ)具有良好的亲水性 ,良好的生物相容性 ,但是ＰＥＧ是非降解性的 ,只有低分子量的ＰＥＧ可以被吞噬细胞所吞噬或透过肾滤膜而排出体外 ,因此 ,低分子量的ＰＥＧ常被用来与丙交酯 (Ｌ ＬＡ)共聚以改善ＰＬＬＡ支架的亲水性 .聚丙交酯 聚乙二醇共聚物 (ＰＬＥ)的三嵌段及两嵌段共聚物的合成及其性能的研究已被广泛报道[3～ 5] .研究…     

离子交换树脂负载Ni—B无定形合金催化剂的制备与性能

制备了一种新型离子交换树脂负载的Ｎｉ－Ｂ无定形合金催化剂．用３种树脂作为催化剂载体，即弱酸型阳离子树脂Ｄ１５２，强酸型阳离子树脂Ｄ７２及强碱型阴离子树脂Ｄ２６１．用ＸＰＳ、ＴＥＭ和ＩＣＰ等技术对催化剂进行了表征．结果表明，催化剂上镍与带有功能基的载体树脂之间有着很强的相互作用，但其强度与所带的功能基有关．３种催化剂Ｎｉ２ｐ３／２的ＸＰＳ谱图上，ＮｉＢ／Ｄ１５２催化剂的氧化态峰最小，而ＮｉＢ／Ｄ２６１的氧化态峰最大．异丙醇脱氢反应活性实验证实了这一结果．     

停流光谱分析PEG甲苯体系中辣根过氧化物酶与过氧化氢复合物的形成

比较研究了在ＰＥＧ水相和ＰＥＧ甲苯有机相中辣根过氧化物酶（ＨＲＰ）的ＵＶ－Ｖｉｓ光谱,研究表明,ＰＥＧ甲苯体系破坏了酶的结构并导致血红素辅基脱落,利用停流光谱仪对ＨＲＰ与过氧化氢复合物的形成进行研究,结果发现,ＰＥＧ甲苯体系中复合物Ⅱ的形成比ＰＥＧ水溶液中复合物Ⅱ形成慢４倍左右,并且在ＰＥＧ甲苯体系中,复合物Ⅱ很不稳定,导致了酶失活。     

可生物降解的聚乳酸弹性体的合成与表征

本文将丙交酯（ＤＬ－ＬＡ）与聚乙二醇（ＰＥＧ）的预聚体用甲苯－二异氰酸酯８０（ＴＤＩ）扩链，得到了一系列的聚乳酸（聚醚）型聚氨酯（ＰＥＧ－ＰＬＡ／ＰＵ）弹性体。对预聚体和弹性体分别进行了ＩＲ、ＨＮＭＲ和ＤＭＡ表征，并测定了弹性体的力学性能。结果表明，ＬＡ与ＰＥＧ生成的预聚体是一种三嵌段结构：ＨＯ－ＰＬＡ－ＰＥＧ－ＰＬＡ－ＯＨ。随着ＰＥＧ含量的增加，弹性体的玻璃化温度下降；ＰＥＧ分子量增大时，弹性体     

多元醇及其二元混合物固-固相变的IR研究

固固相变储能物质多元醇类以其有适宜的转变温度、较高的转变焓、具有经济和技术潜力而受到人们的重视,已在热力学和动力学等方面对其进行广泛和深入的研究[1-3],并通过红外光谱法研究了几种纯多元醇固固转变的机理[1].本文对几种多元醇及其二元混合物进行变温红外光谱的测定,进一步探讨了变化的规律.1　实　验11　药品:新戊二醇(ＮＰＧ)为保证试剂(日本东京化成株式工业会社),三羟甲基乙烷(ＰＧ)超纯(日本东京化成株式工业会社),季戊四醇(ＰＥ)化学纯(北京化学试剂公司).12　仪器美国ＰＥ公司Ｍ1730型富里叶变换红外光谱仪;日本Ｅ012Ａ号Ｈ…     

Highly-loaded amphiphilic polyimino resin: quench reagent and solid support for peptide synthesis

We demonstrate herein that polyimino resin 4a prepared by condensation of α,α′-dichloro-p-xylene, ethylenediamine and tris-(2-aminoethyl)-amine can be successfully exploited as a quench reagent for acids and electrophiles both in aqueous and organic solutions. Scope and limitations of such a resin as a solid support for peptide synthesis were also investigated.     

Rink Amide树脂结构对多肽合成的影响研究

研究了Rink Amide树脂取代度、溶胀度及肽链的长度不同对肽合成收率的影响,并对影响Rink Amide树脂溶胀度的因素进行了研究,结果表明,合成长肽时低取代度、高溶胀度的Rink Amide树脂能获得较好的肽收率。     

Synthesis of cross-linked polystyrene-supported polyethylene glycol and investigation of its property in peptide synthesis

The polyethylene glycol resin (PEG-Resin) which possesses hydrophilic properties was prepared by grafting the polyethylene glycol onto the chloromethylated copolymer of styrene and divinylbenzene in the presence of concentrated sodium hydroxide solution. The proceeding of the graft reaction was identified by IR spectrum analysis. There factors which affected the grafting reactions were investigated. By using the PEG-Resin polymer support, we compared the reactions for the syntheses of a tetra-peptide and a penta-peptide with the Merrifield solid peptide synthesis. We also measured the reaction kinetics of these reactions. The experimental results showed that by employing the PEG-Resin, the reaction rates and condensation yields of these peptide syntheses were improved.     

胡蜂蜂毒肽的固相合成

采用Fmoc固相合成策略,合成了胡蜂蜂毒肽(COOH-Ile-Asn-Leu-Lys-Ala-Leu-Ala-Ala-Leu-Ala-Lys-Lys-Ile-Leu-NH₂)。以Wang树脂为载体,HBTU-HOBt为缩合剂,按照其氨基酸序列依次缩合,最终用切割试剂将其从树脂上切割下来,得到粗肽,经RP-HPLC纯化得到目标肽,纯度97.6%。经HR-MS（EI）分析,确定产物为胡蜂蜂毒肽。     

Solid-phase synthesis of an isoxazolinopyrrole library

A four-step solid-phase synthesis of isoxazolinopyrroles 8 that employs an acid-labile 2-(4-formyl-3-methoxyphenoxy)ethyl polystyrene HL resin 1 is reported. Resin-bound vinyl sulfone 5 is obtained by DIC coupling with acid 4, which was in turn synthesized in solution phase by a regioselective nitrile oxide 1,3-dipolar cycloaddition. The resin-bound pyrrole 7 was synthesized on solid phase by pyrrole annulation with various isocyano derivatives and potassium t-butoxide in which the sulfone alpha-anion generated by Michael addition gives the desired pyrrole through internal condensation followed by a sigmatropic [1,5]-hydrogen shift. The resulting isoxazolinopyrroles 8 were released from resin 7 by 10% TFA in moderate to excellent overall yields from 2-(4-formyl-3-methoxyphenoxy)ethyl polystyrene HL resin 1.     

Preparation of a core-shell type MBHA resin and its application for solid-phase peptide synthesis

MBHA (4-methylbenzhydrylamine) resin has been extensively used as a solid support for the synthesis of peptide amides. Herein, we prepared the core-shell-type MBHA resin by benzotriazole-catalyzed amidoalkylation and partial hydrolysis. The core-shell structure of the MBHA resin was confirmed by two-photon microscopy and its synthetic performance in solid-phase peptide synthesis (SPPS) was evaluated.     

Poly(styrene‐co‐glycerol dimethacrylate): Synthesis,characterization, and application as a resin for gel‐phase peptide synthesis

An efficient cross‐linked polymer support for solid‐phase synthesis was prepared by introducing glycerol dimethacrylate cross‐linker to polystyrene network using free radical aqueous suspension polymerization. The support was characterized by various spectroscopic methods. Morphological feature of the resin was analyzed by microscopy. The polymerization reaction was investigated with respect to the effect of amount of cross‐linking agent, which in turn vary the swelling, loading, and the mechanical stability of the resin. The solvent uptake of the polymer was studied in relation to cross‐linking and compared with Merrifield resin. The stability of the resin was tested in different synthetic conditions used for solid‐phase peptide synthesis. Hydroxy group of the support was derivatized to chloro and then amino groups using different reagents and reaction conditions. Efficiency of the support was tested and compared with TentaGel? resin by following different steps involved in the synthesis of the 65–74 fragment of acyl carrier protein. The results showed that the poly(styrene‐co‐glycerol dimethacrylate) (GDMA‐PS) is equally efficient as TentaGel resin in peptide synthesis. The purity of the peptides was analyzed by HPLC and identities were determined by mass spectroscopy and amino acid analysis. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 4382–4392, 2005     

Solid-phase Synthesis of PNA Monomer by Ugi Four-component Condensation Reaction

Peptide nucleic acids (PNA) oligomers were synthesized in most cases by peptide a peptide synthesis from N-protected monomers. In this work a new method of obtaining PNA monomer by Ugi four-component condensation reaction was tested by solid-phase synthesis. The Fmoc protected PNA monomer was build up with thymin-l-yl acetic acid, 3-methylbutyl aldehyde, Fmoc protected aminoethyl isocyanide and Gly-Wang resin.     

Total chemical synthesis of large CCK isoforms using a thioester segment condensation approach

Silver-ion mediated thioester segment condensation was applied to the chemical synthesis of high molecular weight isoforms of cholecystokinin (CCK). Three building blocks, a C-terminal Tyr(SO₃H)-containing segment and two partially protected thioester segments having a C-terminal Pro residue, were prepared using Fmoc-based chemistry and 2-chlorotrityl chloride (Clt) resin as a solid support. The entire peptide chain was successfully synthesized by two consecutive silver-ion mediated condensation reactions using these building blocks. A brief TFA treatment of the final condensation product gave highly homogeneous CCK-58 in a satisfactory yield. This peptide exhibited glucose-dependent insulinotropic activity at levels comparable to CCK-33. These results demonstrate the usefulness of the silver-ion mediated segment condensation approach in the preparation of large sulfated peptides.     

An Efficient Procedure for Cleavage of T-Butyl Protected Cysteine in Solid Phase Peptide Synthesis

In the Fmoc-strategy of solid phase peptide synthesis, 1M trimethylsilyl bromide-thioanisole/trifluoroacetic acid in the presence of 1,2-ethanedithiol as scavenger was found to be an efficient deprotecting procedure for a full cleavage and side chains deprotection of the peptide resin involving t-butyl protected cysteine. In addition, selective deprotection of the peptide resin containing protected cysteine was also described based on this method.