摘要
阿尔兹海默症(AD)是一种进行性神经退行性疾病,其特征是记忆力减退、神志不清和各种认知障碍.β-淀粉样蛋白(Aβ)的自组装聚集是阿尔茨海默症患者大脑的主要特征之一,其加剧了AD患者的神经病变和认知障碍,因此抑制Aβ聚集是一种潜在的治疗AD的策略.光动力疗法是抑制Aβ聚集和解聚Aβ聚集体的有效方法.然而,大多数光敏剂为紫外和可见光激发,在生物组织中的渗透深度低,并引起严重的组织损伤,这限制了其在生物医学中的应用.本工作构建了一种近红外光激发的双靶向上转换纳米体系应用于抑制Aβ聚集过程.以核壳结构的上转换纳米颗粒(UCNPs)作为光转换器,通过两亲聚合物二硬脂酰基磷脂酰乙醇胺-聚乙二醇-马来酰亚胺(DSPE-PEG-MAL)的疏水包覆作用负载光敏剂二氢卟吩e6(Ce6),在纳米颗粒表面通过马来酰亚胺与巯基的特异性反应修饰了可跨越血脑屏障的肽链TGN和靶向Aβ42的肽链QSH.实验结果表明在近红外光激发下UCNPs通过发光共振能量转移(LRET)将能量转移至光敏剂Ce6,使其跃迁至激发态后与周围的氧气分子作用产生单线态氧(^(1)O_(2)),不可逆地氧化Aβ,从而有效解聚了Aβ聚集体,降低了Aβ聚集体的神经毒性.此外,该体系不仅具有良好的生物相容性,而且可以有效穿过血脑屏障靶向作用于Aβ42,显示出其在活体水平治疗AD的潜力.
Alzheimer’s disease(AD)is a progressive neurodegenerative disorder characterized by memory loss,confusion,and a variety of cognitive disabilities.The self-assembly and aggregation ofβ-amyloid(Aβ)peptides is a main feature of the brain of Alzheimer’s disease,which can aggravate the nerve damage and cognitive impairment of AD patients.Therefore,inhibition of the aggregation of Aβpeptides is recognized as a potential strategy to alleviate AD.Photodynamic therapy(PDT)is a creative method that has wide applications in suppressing amyloid aggregation or eliminating the amyloid aggregates.However,most photosensitizers are excited by ultraviolet and visible light,have a low penetration depth in biological tissues,and cause serious tissue damage,which limits their application in biomedicine.Herein,we report a dual-targeting upconversion nanoprobe excited by near-infrared light to inhibit the Aβaggregation process.The core-shell structured upconversion nanoparticles NaYF4:Yb,Er,Gd,Tm@Na YF4 are used as light converters,and the photosensitizer chlorin-e6(Ce6)is loaded through the hydrophobic coating of the amphiphilic polymer 1,2-distearoylsn-glycero-3-phosphoethanolamine-N-[maleimide(polyethyleneglycol)-2000](DSPE-PEG-MAL).A blood-brain barrier targeting peptide,TGN,and a Aβtarget peptide,QSH,are simultaneously modified on the surface of nanoparticles via the specific reaction between maleimide and sulfhydryl groups.The results indicate that UCNPs can transfer the excited-state energy to the photosensitizer Ce6 through luminescence resonance energy transfer(LRET)process under the excitation of near-infrared light irradiation.After transition to the excited state,Ce6 further interact with the surrounding oxygen molecules to produce singlet oxygen(1 O2)and irreversibly oxidizeβ-amyloid,thus effectively disassembling Aβaggregates and reducing the cytotoxicity associated with Aβ.In addition,UCNPs-Ce6-TQ not only exhibits good biocompatibility,but also can effectively cross the blood-brain barrier and target Aβ42.This nanoprobe may be a powerful tool to inhibit the accumulation of Aβin the brain and alleviate the neurotoxic damage caused by Aβ.
作者
黄菊
李贞
刘志洪
Ju Huang;Zhen Li;Zhihong Liu(College of Chemistry and Molecular Sciences,Wuhan University,Wuhan 430072,China;College of Chemistry and Chemical Engineering,Hubei University,Wuhan 430062,China)
出处
《化学学报》
SCIE
CAS
CSCD
北大核心
2021年第8期1049-1057,共9页
Acta Chimica Sinica
基金
国家自然科学基金(Nos.21807028,21625503)资助.
