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肺肽模拟药物与肽转运的分子机制

Molecular mechanisms of pulmonary peptidomimetic drug and peptide transport.

作者信息

Groneberg David A, Fischer Axel, Chung K Fan, Daniel Hannelore

机构信息

Deptartment of Pediatric Pneumology and Immunology/Medicine, Charité School of Medicine, Humboldt-University; CVK OR-1 R.3.0073, Augustenburger Platz 1, D-13353 Berlin, Germany.

出版信息

Am J Respir Cell Mol Biol. 2004 Mar;30(3):251-60. doi: 10.1165/rcmb.2003-0315TR.

DOI:10.1165/rcmb.2003-0315TR
PMID:14969997
Abstract

The aerosolic administration of peptidomimetic drugs could play a major role in the future treatment of various pulmonary and systemic diseases, because rational drug design offers the potential to specifically generate compounds that are transported efficiently into the epithelium by distinct carrier proteins such as the peptide transporters. From the two presently known peptide transporters, PEPT1 and PEPT2, which have been cloned from human tissues, the high-affinity transporter PEPT2 is expressed in the respiratory tract epithelium. The transporter is an integral membrane protein with 12 membrane-spanning domains and mediates electrogenic uphill peptide and peptidomimetic drug transport by coupling of substrate translocation to a transmembrane electrochemical proton gradient serving as driving force. In human airways, PEPT2 is localized to bronchial epithelium and alveolar type II pneumocytes, and transport studies revealed that both peptides and peptidomimetic drugs such as antibiotic, antiviral, and antineoplastic drugs are carried by the system. PEPT2 is also responsible for the transport of delta-aminolevulinic acid, which is used for photodynamic therapy and the diagnostics of pulmonary neoplasms. Based on the recent progress in understanding the structural requirements for substrate binding and transport, PEPT2 becomes a target for a rational drug design that may lead to a new generation of respiratory drugs and prodrugs that can be delivered to the airways via the peptide transporter.

摘要

拟肽药物的气雾剂给药在未来各种肺部和全身性疾病的治疗中可能发挥重要作用,因为合理的药物设计提供了特异性生成化合物的潜力,这些化合物可通过诸如肽转运体等独特的载体蛋白有效地转运到上皮细胞中。从目前已知的两种已从人体组织中克隆出来的肽转运体PEPT1和PEPT2来看,高亲和力转运体PEPT2在呼吸道上皮中表达。该转运体是一种具有12个跨膜结构域的整合膜蛋白,通过将底物转运与作为驱动力的跨膜电化学质子梯度偶联,介导电生性上坡肽和拟肽药物的转运。在人类气道中,PEPT2定位于支气管上皮和II型肺泡上皮细胞,转运研究表明,该系统可携带肽和拟肽药物,如抗生素、抗病毒和抗肿瘤药物。PEPT2还负责δ-氨基乙酰丙酸的转运,δ-氨基乙酰丙酸用于光动力疗法和肺部肿瘤的诊断。基于在理解底物结合和转运的结构要求方面的最新进展,PEPT2成为合理药物设计的靶点,这可能会导致新一代可通过肽转运体递送至气道的呼吸药物和前体药物。

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