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载多西紫杉醇的疏水衍生超支化聚甘油的组织摄取及其对膀胱尿路上皮形态的影响。

Tissue uptake of docetaxel loaded hydrophobically derivatized hyperbranched polyglycerols and their effects on the morphology of the bladder urothelium.

机构信息

University of British Columbia, Vancouver, BC V6T 1Z3, Canada.

出版信息

Biomaterials. 2012 Jan;33(2):692-703. doi: 10.1016/j.biomaterials.2011.09.081. Epub 2011 Oct 19.

DOI:10.1016/j.biomaterials.2011.09.081
PMID:22014457
Abstract

Recently, we have reported that docetaxel (DTX) loaded, amine terminated hyperbranched polyglycerol (HPG-C(8/10)-MePEG-NH(2)) nanoparticles significantly increased drug uptake in mouse bladder tissues and was the most effective formulation to significantly inhibit tumor growth in an orthotopic model of bladder cancer. The objective of this study was to investigate the effects of HPG-C(8/10)-MePEG-NH(2) nanoparticles on bladder urothelial morphology and integrity, DTX uptake and permeability in bladder tissue and the extent of bladder urothelial recovery following exposure to, and then washout of, HPG-C(8/10)-MePEG-NH(2) nanoparticles. HPG-C(8/10)-MePEG-NH(2) nanoparticles significantly increased the uptake of DTX in both isolated pig bladder as well as in live mouse bladder tissues. Furthermore, HPG-C(8/10)-MePEG-NH(2) nanoparticles were demonstrated to increase the permeability of the urinary bladder wall by causing changes to the urothelial barrier function and morphology through opening of tight junctions and exfoliation of the superficial umbrella cells. These data suggest that exfoliation may be triggered by an apoptosis mechanism, which was followed by a rapid recovery of the urothelium within 24 h post-instillation of HPG-C(8/10)-MePEG-NH(2) nanoparticles. HPG-C(8/10)-MePEG-NH(2) nanoparticles cause significant but rapidly recoverable changes in the bladder urothelial morphology, which we believe may make them suitable for increasing drug permeability of bladder tissue and intravesical drug delivery.

摘要

最近,我们报道了多西紫杉醇(DTX)负载的胺封端超支化聚甘油(HPG-C(8/10)-MePEG-NH(2))纳米粒显著增加了小鼠膀胱组织中的药物摄取,并且是最有效的制剂,可以显著抑制膀胱癌的原位模型中的肿瘤生长。本研究的目的是研究 HPG-C(8/10)-MePEG-NH(2)纳米粒对膀胱尿路上皮形态和完整性、膀胱组织中 DTX 摄取和通透性以及暴露于 HPG-C(8/10)-MePEG-NH(2)纳米粒后膀胱尿路上皮恢复程度的影响),然后冲洗。HPG-C(8/10)-MePEG-NH(2)纳米粒显著增加了分离的猪膀胱和活小鼠膀胱组织中 DTX 的摄取。此外,HPG-C(8/10)-MePEG-NH(2)纳米粒通过打开紧密连接和脱落表面伞状细胞来改变尿路上皮屏障功能和形态,从而被证明可以增加膀胱壁的通透性。这些数据表明,脱落可能是由细胞凋亡机制触发的,随后在 HPG-C(8/10)-MePEG-NH(2)纳米粒灌注后 24 小时内,尿路上皮迅速恢复。HPG-C(8/10)-MePEG-NH(2)纳米粒导致膀胱尿路上皮形态发生显著但可迅速恢复的变化,我们认为这可能使它们适合增加膀胱组织的药物渗透性和膀胱内药物递送。

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