转铁蛋白修饰脂质体的制备及其肝癌靶向性研究

目的：肿瘤的靶向治疗是当前研究的热点,肝肿瘤细胞表面有大量的转铁蛋白受体表达,而正常组织较少,因此本研究制备转铁蛋白（TF）修饰的脂质体（TFLPs）,并对其肝肿瘤靶向性进行研究。方法：采用薄膜分散法制备普通脂质体,考察其形态,粒径,电位。通过体外血清稳定性模拟脂质体进入体内后的稳定性。通过HepG2肿瘤细胞对TFLPs的摄取实验考查脂质体与肝癌细胞的亲和力。构建荷瘤裸鼠模型,考查TFLPs在荷瘤裸鼠体内的分布。结果：所制备的TFLPs平均粒径为108．8±9．5nm,Zeta电位为．1．80±0．73mV。学期稳定性试验结果显示,TFLPs在24h内具有良好的血清稳定性。体外细胞摄取实验表明,HepG2细胞对TFLPs的摄取效率是普通长循环脂质体（LPs）的3．4倍。荷瘤裸鼠肝组织和肿瘤组织切片结果显示,TFLPs比LPs具有更好的肿瘤靶向性。结论：该脂质体制备方法简单,与LPs相比,经转铁蛋白修饰可显著提高肿瘤细胞对脂质体的摄取,TFLPs是一种潜在高效的肝癌靶向给药系统。     

抗肿瘤靶向脂质体的研究进展

近年来,随着肿瘤靶向治疗在临床的不断推广,抗肿瘤靶向脂质体的研究也备受关注。抗肿瘤靶向脂质体可分为物理靶向脂质体和分子靶向脂质体,前者包括pH敏感脂质体、光敏感脂质体、磁性脂质体和热敏感脂质体;后者包括抗体靶向脂质体、叶酸修饰脂质体、转铁蛋白修饰脂质体、多肽修饰脂质体及糖基修饰脂质体等。现介绍抗肿瘤靶向脂质体的研究进展,为靶向脂质体的研究和应用提供参考。     

脂质体包裹阿霉素的体外抗肿瘤作用

 我们用超声法制备了内部包裹阿霉素,表面有抗人胃癌细胞M85的单克隆抗体3Hll或非相关抗体IgG的阿霉素靶向脂质体和阿霉素非靶向脂质体,研究了这些脂质体和游离阿霉素抑制靶细胞M85和非靶细胞HeLa细胞生长的能力。结果表明,一方面,与游离阿霉素或阿霉素非靶向脂质体相比,阿霉素靶向脂质体抑制M85细胞生长的能力提高了2—4倍,而在抑制非靶细胞HeLa细胞的生长方面,阿霉素靶向脂质体的效力还不如游离阿霉素或阿霉素非靶向脂质体。过量的游离单克隆抗体3Hll可以有效地抑制阿霉素靶向脂质体对M85细胞的细胞毒作用,而另一种单克隆抗体3G9则不能。空靶向和空非靶向脂质体对M85细胞生长均无影响。因此,靶向脂质体可以把包裹的抗癌药物专一地送给胃癌细胞,井杀伤它们。     

转铁蛋白导向脂质体核磁造影剂纳米粒子(TfNTR-LipNBD-Magnevist)——一种肿瘤靶向磁共振造影剂

造影剂辅助的核磁共振成像是目前肿瘤诊断的最好方法之一.但是由于核磁共振成像内在的低灵敏性以及造影剂的非特异性,导致肿瘤早期诊断较为困难.文章将一种新的肿瘤靶向核磁造影剂纳米粒子应用于早期肿瘤的影像诊断.这种新的肿瘤靶向核磁造影剂纳米粒子由配体转铁蛋白(Tf)、纳米水平的正电脂质体(Lip)载体和临床常用的造影剂Magnevist(TfNIR-LipNBD-Magnevist)三部分构成.另外转铁蛋白和脂质体粒子上,亦标记了荧光物质用于确定转铁蛋白-脂质体-造影剂纳米粒子的靶向性,以及肿瘤的光学影像诊断.在体外实验中,利用激光共聚焦显微镜和光学影像证明了靶向纳米粒子介导的细胞内吞和特异性结合.在裸鼠肿瘤模型中,造影剂纳米粒子TfNIR-LipNBD-Magnevist经尾静脉注入后,显著增强了肿瘤内信号与周围组织的对比度.由造影剂纳米粒子介导的肿瘤内信号显著强于单独Magnevist辅助的肿瘤内信号.同时,利用光学影像方法,在肿瘤内检测到特异的荧光信号.其结果进一步支持了转铁蛋白-脂质体-造影剂(TfNIR-LipNBD-Magnevist)纳米粒子的靶向性和肿瘤影像诊断的有效性.     

转铁蛋白导向脂质体核磁造影剂纳米粒子（TfNIR-LipNBD-Magnevist）——一种肿瘤靶向磁共振造影剂

造影剂辅助的核磁共振成像是目前肿瘤诊断的最吁方法之一。但是由于核磁共振成像内在的低灵敏性以及造影剂的非特异性,导致肿瘤早期诊断较为困难。文章将一种新的肿瘤靶向核磁造影剂纳米粒子应用于早期肿瘤的影像诊断。这种新的肿瘤靶向核磁造影剂纳米粒子由配体转铁蛋白（Tf）、纳米水平的正电脂质体（Lip）载体和临床常用的造影剂Magnevist（Tf^NIR-Lip^NBD-Magnevist）三部分构成。另外转铁蛋白和脂质体粒子上,亦标记了荧光物质用于确定转铁蛋白一脂质体一造影剂纳米粒子的靶向性,以及肿瘤的光学影像诊断。在体外实验中,利用激光共聚焦显微镜和光学影像证明了靶向纳米粒子介导的细胞内吞和特异性结合。在裸鼠肿瘤模型中,造影剂纳米粒子Tf^NIR-Lip^NBD-Magnevist经尾静脉注入后,显著增强了肿瘤内信号与周围组织的对比度。由造影剂纳米粒子介导的肿瘤内信号显著强于单独Magnevist辅助的肿瘤内信号。同时,利用光学影像方法,在肿瘤内检测到特异的荧光信号。其结果进一步支持了转铁蛋白一脂质体一造影利（Tf^NIR-Lip^NBD-Magnevist）纳米粒子的靶向性和肿瘤影像诊断的有效性。     

亚油酸铂靶向脂质体抗肿瘤特性的研究

用超声波制备了内部包裹亚油酸铂,表面有抗人乳腺癌单克隆抗体ＭｃＡｂＧｐ－１Ｄ８的亚油酸铂靶向脂质体和亚油酸铂非靶向脂质体,研究了这些脂质体绎腹部注射到荷瘤裸鼠之后的组织分布和抑瘤效果,实验结果表明,靶向脂质体亚油酸铂在肿瘤组织的含量明显高于游离亚油酸铂组;在肾,肝,肺,脾,心脏等器官中,前者的含量比后者有所降低,分别在接种癌细胞后６天,１２天和２４天,按６ｍｇ／ｋｇ的剂量分别注射ＰＢＳ,游离亚油酸     

转铁蛋白受体——肿瘤的标志物和靶向治疗

转铁蛋白受体不仅介导细胞内铁的摄取和参与细胞生长调节,而且能够在肿瘤细胞表面高度表达,被认为是一种有效的肿瘤标志物,广泛应用于各类恶性肿瘤的靶向治疗。利用转铁蛋白或转铁蛋白受体的单克隆抗体与转铁蛋白受体的特异性结合作用,通过受体介导的内吞机制实现化疗药物、蛋白毒素或治疗性基因等的细胞摄入。随着对转铁蛋白受体的深入研究,靶向转铁蛋白受体的肿瘤药物将在基因治疗和跨血脑屏障运输等多方面得到进一步应用。     

靶向细胞因子CD40的全新多肽配体的筛选与鉴定

CD40是肿瘤坏死因子受体(tumornecrosis factor receptor,TNFR)超家族成员,表达于免疫细胞、造血细胞、血管细胞、内皮细胞及多种类型的癌细胞表面。作者采用计算机虚拟筛选和细胞实验相结合的方法,研究了CD40蛋白的全新多肽配体。首先,通过同源建模构建CD40蛋白的三维结构;然后,用分子对接虚拟筛选出靶向CD40的多肽配体;再通过表面等离子体共振(surface plasmon resonance,SPR)分子结合实验、多肽靶向脂质体的细胞实验,验证并确定被命名为N9的六肽为CD40的全新配体。进一步研究发现,N9修饰的脂质体对其靶向细胞Raji和树突状细胞(dendritic cells,DC)的转染效果明显提高,提示N9有靶向介导转染的功能。     

多肽表面修饰脂质体药物递送系统

本文通过查阅并归纳近几年相关文献,较为系统地概述了靶向活性多肽、细胞穿膜肽和靶向细胞穿膜肽等多肽表面修饰脂质体药物递送系统(drug delivery system, DDS)的研究进展。经不同活性多肽表面修饰,或可增强脂质体DDS的靶向性,或可提高药物的细胞摄取率和生物利用度。总之,多肽表面修饰的脂质体在新型DDS研究及应用中具有良好的前景。     

多肽靶向脂质体的表面配体修饰密度及其体内肿瘤靶向效果的研究

脂质体作为一种药物载体广泛应用于肿瘤药物输送中。配体修饰的靶向脂质体,其靶向配体分子在脂质体表面修饰的构象和密度等参数,对脂质体本身的特性及其体内的靶向效果,有很大的影响。但有关其中的具体相互关系,以及可能的最优条件,国内外文献都尚无定论。据此我们建立了多肽靶向脂质体表面配体修饰的分析方法,并通过影像学手段来研究不同靶向肽含量对脂质体在荷瘤裸鼠中的靶向行为的影响。首先采用孵育插入法将带有多肽的脂质分子插入脂质体表面,用分子筛色谱法分离修饰后的脂质体和未插入的多肽脂质,再用HPLC-ELSD定量各脂质成分,得到多肽靶向脂质体表面的靶向肽密度。而后将修饰有不同密度靶向多肽的荧光脂质体经荷瘤小鼠尾静脉注射,分别在给药前后各时间点对小鼠进行扫描,对扫描得到的图像进行处理并计算AUC、T1/2和MRT等相关药代动力学参数。结果表明,随着脂质体表面多肽密度的增加,即多肽密度大于1.298%的靶向脂质体,其肿瘤部位的荧光AUC、T1/2和MRT都较未修饰的隐形脂质体有所提高,显示其在肿瘤组织中的聚集量增多、停留时间延长,针对肿瘤细胞的特异性作用机制得以彰显。     

A Unique Protease Cleavage Site Predicted in the Spike Protein of the Novel Pneumonia Coronavirus (2019-nCoV) Potentially Related to Viral Transmissibility

正Dear Editor,In December 2019, a novel human coronavirus caused an epidemic of severe pneumonia(Coronavirus Disease 2019,COVID-19) in Wuhan, Hubei, China(Wu et al. 2020; Zhu et al. 2020). So far, this virus has spread to all areas of China and even to other countries. The epidemic has caused 67,102 confirmed infections with 1526 fatal cases     

Curcuminoids as inhibitors of thioredoxin reductase: A receptor based pharmacophore study with distance mapping of the active site

Curcumin is the yellow pigment of turmeric that interacts irreversibly forming an adduct with thioredoxin reductase (TrxR), an enzyme responsible for redox control of cell and defence against oxidative stress. Docking at both the active sites of TrxR was performed to compare the potency of three naturally occurring curcuminoids, namely curcumin, demethoxy curcumin and bis-demethoxy curcumin. Results show that active sites of TrxR occur at the junction of E and F chains. Volume and area of both cavities is predicted. It has been concluded by distance mapping of the most active conformations that Se atom of catalytic residue SeCYS498, is at a distance of 3.56 from C13 of demethoxy curcumin at the E chain active site, whereas C13 carbon atom forms adduct with Se atom of SeCys 498. We report that at least one methoxy group in curcuminoids is necessary for interation with catalytic residues of thioredoxin. Pharmacophore of both active sites of the TrxR receptor for curcumin and demethoxy curcumin molecules has been drawn and proposed for design and synthesis of most probable potent antiproliferative synthetic drugs.     

The structure, reproduction and taxonomy of Vidalia and Osmundaria (Rhodophyta, Rhodomelaceae)

Comprises species occurring mostly in subtidal habitats in tropical, subtropical and warm-temperate areas of the world. An analysis of the type species, V. spiralis (Sonder) Lamouroux ex J. Agardh, a species from Australia, establishes basic characters for distinguishing species in the genus. These characters are (1) branching patterns of thalli, (2) flat blades that may be spiralled on their axis, (3) width of the blade, (4) primary or secondary derivation of sterile and fertile branchlets and (5) position of sterile and fertile branchlets on the thalli. Application of the latter two characters provides an important basic method for separation of species into three major groups. Osmundaria , a genus known only in southern Australia, was studied in relation to Vidalia , and its separation from the Vidalia assemblage is not accepted. Species of Vidalia therefore are transferred to the older genus name, Osmundaria. Two new species, Osmundaria papenfussii and Osmundaria oliveae are described from Natal. Confusion in the usage of the epithet, Vidalia fimbriala Brown ex Turner has been clarified, and Vidalia gregaria Falkenberg, described as an epiphyte on Osmundaria pro/ifera Lamouroux, is revealed to be young branches of the host, Osmundaria prolifera.     

New or rare chromosome counts in Artemisia L. (Asteraceae, Anthemideae) and related genera from Kazakhstan

Fifteen chromosome counts of six Artemisia taxa and one species of each of the genera Brachanthemum, Hippolytia, Kaschgaria, Lepidolopsis and Turaniphytum are reported from Kazakhstan. Three of them are new reports, two are not consistent with previous counts and the remainder are confirmations of very scarce (one to four) earlier records. All the populations studied have the same basic chromosome number, x = 9, with ploidy levels ranging from 2x to 6x. Some correlations between ploidy level, morphological characters and distribution are noted.     

肝癌中HBV和HCV基因和抗原的分布及意义

采用原位分子杂交方法检测HCV RNA及HBV X基因;采用免疫组织化学方法研究HCV核心抗原,非结构区C33c抗原及HBxAg在肝细胞肝癌中的定位及分布.结果表明(1)HCV RNA、HBV X基因在肝细胞肝癌组织检出率分别为40%(55/136)和82%(112/136).HCV RNA定位于癌细胞的胞浆内,阳性细胞呈散在、灶状及弥漫分布三种形式;HBV X基因在肝癌细胞中的分布呈胞浆型、核型及核浆型,阳性细胞也呈上述三种分布形式;(2)HCV C33c抗原、核心抗原在肝细胞肝癌中的阳性率为81%(133/164)及86%(141/164).C33c抗原定位于癌细胞及肝细胞的胞浆内;核心抗原既定位于癌细胞核中,又可定位于胞浆中.C33c抗原阳性细胞以灶状分布为主;而核心抗原阳性细