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利用吸光性微粒和纳米颗粒进行细胞选择性靶向

Selective cell targeting with light-absorbing microparticles and nanoparticles.

作者信息

Pitsillides Costas M, Joe Edwin K, Wei Xunbin, Anderson R Rox, Lin Charles P

机构信息

Wellman Laboratories of Photomedicine, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02114, USA.

出版信息

Biophys J. 2003 Jun;84(6):4023-32. doi: 10.1016/S0006-3495(03)75128-5.

Abstract

We describe a new method for selective cell targeting based on the use of light-absorbing microparticles and nanoparticles that are heated by short laser pulses to create highly localized cell damage. The method is closely related to chromophore-assisted laser inactivation and photodynamic therapy, but is driven solely by light absorption, without the need for photochemical intermediates (particularly singlet oxygen). The mechanism of light-particle interaction was investigated by nanosecond time-resolved microscopy and by thermal modeling. The extent of light-induced damage was investigated by cell lethality, by cell membrane permeability, and by protein inactivation. Strong particle size dependence was found for these interactions. A technique based on light to target endogenous particles is already being exploited to treat pigmented cells in dermatology and ophthalmology. With exogenous particles, phamacokinetics and biodistribution studies are needed before the method can be evaluated against photodynamic therapy for cancer treatment. However, particles are unique, unlike photosensitizers, in that they can remain stable and inert in cells for extended periods. Thus they may be particularly useful for prelabeling cells in engineered tissue before implantation. Subsequent irradiation with laser pulses will allow control of the implanted cells (inactivation or modulation) in a noninvasive manner.

摘要

我们描述了一种基于使用光吸收性微粒和纳米颗粒的选择性细胞靶向新方法,这些微粒和纳米颗粒通过短激光脉冲加热以造成高度局部化的细胞损伤。该方法与发色团辅助激光失活和光动力疗法密切相关,但仅由光吸收驱动,无需光化学中间体(特别是单线态氧)。通过纳秒时间分辨显微镜和热模型研究了光与粒子的相互作用机制。通过细胞存活率、细胞膜通透性和蛋白质失活研究了光诱导损伤的程度。发现这些相互作用对颗粒大小有很强的依赖性。一种基于光靶向内源性颗粒的技术已被用于皮肤科和眼科治疗色素细胞。对于外源性颗粒,在该方法与光动力疗法用于癌症治疗进行评估之前,需要进行药代动力学和生物分布研究。然而,与光敏剂不同,颗粒的独特之处在于它们可以在细胞中长期保持稳定和惰性。因此,它们对于在植入前对工程组织中的细胞进行预标记可能特别有用。随后用激光脉冲照射将允许以非侵入性方式控制植入的细胞(失活或调节)。

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