去氧鬼臼毒素mPEG-PDLLA聚合物胶束的制备及其性质的研究

目的合成聚乙二醇单甲醚-聚乳酸(mPEG-PDLLA)嵌段共聚物,制备去氧鬼臼毒素mPEG-PDLLA嵌段共聚物(DPT-PM),提高去氧鬼臼毒素在水中的溶解度。方法以开环聚合反应合成mPEG-PDLLA,并通过IR、1H-HMR确证其结构,芘荧光探针法测定其临界胶束浓度(CMC);采用溶剂蒸发法制备DPT-PM溶液,并将其冷冻干燥;分别采用动态光散射法(DLS)、透射电子显微镜(TEM)、差示扫描量热法(DSC)、高效液相色谱法(HPLC)等手段对胶束形态、粒径与分布、载药量、包封率等进行表征,并采用透析法考察DPT-PM体外释放,并对释放机制进行探讨。结果制备了去氧鬼臼毒素共聚物胶束,透射电镜下观察为近球形,平均粒径为22.0±8.9nm,载药量为20.67%,包封率为99.63%。结论 m PEG-PDLLA聚合物胶束可作为疏水性药物去氧鬼臼毒素的载体,具有较高的载药性能,能一定程度提高去氧鬼臼毒素在水中的溶解度。

Box-Behnken效应面法优化mPEG-PDLLA多烯紫杉醇/白藜芦醇载药胶束处方

目的通过优化手段筛选处方,制备同时包载多烯紫杉醇/白藜芦醇的单甲氧基聚乙二醇-聚丙交酯嵌段共聚物(poly(ethylene glycol)methoxy-poly(D,L-lactide)mPEG-PDLLA)胶束。方法采用薄膜分散法制备mPEG-PDLLA载药胶束,分别以成膜温度(X1)﹑水化温度(X2)、投药量(X3)为考察指标,以多烯他赛(docetaxel,DTX)的包封率(Y1,EE%)及载药质量分数(Y2,wLC%)、白藜芦醇(resveratrol,RES)的包封率(Y3,EE%)及载药质量分数(Y4,wLC%)为评价指标;采用3因素3水平Box-Behnken效应面设计法筛选载药胶束处方;并测定载药胶束的粒径和zeta电位。结果共聚物对2种药物的胶束包封率均大于98%,载药质量分数均大于16%。载药胶束的平均粒径为(17±3.2)nm;zeta电位为-18.0mV。结论采用Box-Behnken实验设计法优化处方所得到的数学模型预测性良好,可以用于多烯紫杉醇∕白藜芦醇载药胶束的处方优化。

PDLLA length on anti-breast cancer efficacy of acid-responsive self-assembling mPEG-PDLLA–docetaxel conjugates

Engineering small-molecule drugs into nanoparticulate formulations provides an unprecedented opportunity to improve the performance of traditional chemo drugs,but suffers from poor compatibility between drugs and nanocarriers.Stimuli-responsive mPEG-PDLLA–drug conjugate-based nanomedicines can facilitate the exploitation of beneficial properties of the carrier and enable the practical fabrication of highly efficacious self-assembled nanomedicines.However,the influence of hydrophobic length on the performance of this type of nanomedicine is little known.Here we synthesized two acid-sensitive ketal-linked mPEG-PDLLA–docetaxel prodrugs with different lengths of PDLLA,and engineered them into self-assembled sub-20 nm micellar nanomedicines for breast cancer chemotherapy.We found that the nanomedicine consisting of a mPEG-PDLLA–docetaxel prodrug with the shorter length of PDLLA stood out due to its potent cytotoxicity,deep penetration into multicellular spheroids,and improved in vivo anticancer performance.Additionally,our prodrug-based nanomedicines outperformed the generic formulation of commercial Nanoxel in terms of safety profile,tolerated doses,and tumor suppression.Our findings indicate that the hydrophobic content of a polymeric prodrug nanomedicine plays an important role in the performance of the nanomedicine,and should be instructive for developing polymeric prodrug-based nanomedicines with clinical translational potential.

An injectable mPEG-PDLLA microsphere/PDLLA-PEG-PDLLA hydrogel composite for soft tissue augmentation

Injectable filling material is a simple and efficient method for soft tissues reconstruction and is extremely popular in not only plastic surgery but also cosmetic industry.However,there is a lack of soft tissue fillers with perfect performance on the market currently.Here,we constructed a new microsphere/hydrogel composite and evaluated its potential as a candidate for soft tissue augmentation.mPEG-PDLLA micro-spheres were prepared by utilizing a SPG membrane emulsifier which endowed microspheres with good sphericity and particle size uniformity.PDLLA-PEG-PDLLA hydrogel which shared the same component with the mPEG-PDLLA copolymer acted as a carrier and fixed the microspheres at the injected sites.The mPEG-PDLLA microsphere/PDLLA-PEG-PDLLA hydrogel composite was flowable in room temperature and transformed into gel after being heated to body temperature.This feature is convenient for subcutaneous filling.In vivo assessment on mice showed good safety profile of the composite.Moreover,the density of collagen fibers increased over 13 weeks.Overall,this biocompatible microsphere/hydrogel composite involves simple component and no extra crosslinking agents,and has the ability to stimulate collagen production,thus,may be a candidate for soft tissue augmentation.

三种注射用新辅料对Beagle犬类过敏及过敏反应研究

目的研究3种注射用新辅料乙交酯-丙交酯共聚物(PLGA)、乙二醇单甲醚-聚乳酸嵌段共聚物(mPEG-PDLLA)和羟丙基-β-环糊精(HP-β-CD)能否引起Beagle犬产生类过敏或过敏反应,为临床研究和应用提供依据。方法使用Beagle犬于1、3、5d致敏共3次,末次致敏后第14d激发。观察给药后反应症状,检测常规血液学指标、血浆中组胺、IgE、IgG和IgM含量。结果上述各项指标在首次给药后和激发日激发后均未见明显异常改变。结论 PLGA、mPEG-PDLLA和HP-β-CD在本实验剂量下不能引起Beagle犬产生类过敏或过敏反应。

替硝唑原位固化缓释凝胶的处方研究

目的:应用Box-Behnken法设计并优化替硝唑原位固化缓释凝胶处方。方法:通过体外释放度的单因素影响试验确定考察因素与水平,以凝胶粘度、遇水固化时间、释放时间为响应变量,应用Box-Behnken法进行处方筛选与优化。结果:优化处方为35.3%(w/w)单甲氧基聚乙二醇-聚乳酸(mPEG-PDLLA10/90),5.9%(w/w)替硝唑和58.8%(w/w)N-甲基-2-吡咯烷酮(NMP)。该凝胶体外释放时间达192 h,无突释现象。结论:通过Box-Behnken法成功实现了替硝唑原位固化缓释凝胶的处方筛选。

Melphalan-loaded methoxy poly(ethylene glycol)-poly(D,L-lactide)copolymer nanomicelles in the treatment of multiple myeloma

Multiple myeloma(MM)is the second most common hematological tumor characterized by the proliferation of monoclonal plasma cells.Melphalan(MEL)is commonly used in the treatment of MM and is especially essential for patients undergoing autologous stem cell transplantation(ASCT).Although many drugs for MM have been developed in recent years,chemotherapy followed by ASCT remains the optimal option.Melphalan,the backbone of the conditioning regimen,brings severe toxicities at a high dose.Nanodrug delivery systems enable drugs to be highly effective and have low toxicity.In this study,methoxy poly(ethylene glycol)-poly(D,L-lactide)copolymer(MPEG-PDLLA)was chosen to encapsulate melphalan,and the characteristics,effectiveness,and safety of MEL/MPEG-PDLLA in vitro and in vivo were investigated.MEL/MPEG-PDLLA showed slow release and was easily engulfed by MM cells despite a result of the antitumor assay comparable to that of free melphalan in vitro.The in vivo results showed that MEL/MPEG-PDLLA could significantly alleviate tumor burden and prolong survival time without increasing the toxicity to vital organs.In addition,MEL/MPEG-PDLLA could significantly reduce the damage to the intestinal mucosa caused by melphalan.In conclusion,MEL/MPEG-PDLLA shows improved antitumor activity and has the potential to alleviate pains of MM patients undergoing ASCT.

不同疏水结构的两亲性聚合物对MDCK-MDR1细胞P-糖蛋白功能的影响

目的研究不同疏水结构的两亲性聚合物单甲醚聚己二醇-聚己内酯聚合物(m PEG-PCL)、单甲醚聚乙二醇-聚D,L-乳酸聚合物(m PEG-PDLLA)、单甲醚聚乙二醇-聚(乳酸-羟基乙酸)聚合物(m PEG-PLGA)对P-糖蛋白(P-glycoprotein,P-gp)外排功能的影响。方法采用薄膜分散法制备聚合物胶束,动态光散射仪测定胶束粒径,芘荧光探针法测定临界胶束浓度(CMC);以P-gp特异性底物罗丹明123(Rhodamine 123,R123)为荧光探针,采用摄取和外排实验评价聚合物及其形成的胶束对MDCK-MDR1细胞P-gp功能的影响。结果m PEG-PCL、m PEG-PDLLA、m PEG-PLGA的粒径分别为(55.9±0.2)、(53.7±1.1)和(61.6±0.6)nm;CMC值分别为2.08、5.42和26.4μg·m L^(-1);摄取实验结果显示,当m PEG-PCL质量浓度在250μg·m L^(-1)、m PEG-PDLLA在1~25μg·m L^(-1)、m PEG-PLGA在1~25μg·m L^(-1)时,可显著增加细胞内R123累积量,表明三者对P-gp外排功能均有抑制作用;外排实验中m PEG-PCL、m PEG-PDLLA、m PEG-PLGA分别在CMC以上、CMC附近及以下、CMC以下时会显著降低R123外排率,与摄取实验结果相对应。结论 m PEG-PCL、m PEG-PDLLA、m PEG-PLGA聚合物对P-gp外排活性均有一定的抑制作用,其作用程度与疏水段结构、聚合物浓度及存在状态有关。