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Nasal tissue dosimetry-issues and approaches for 'Category 1' gases: a report on a meeting held in Research Triangle Park, NC, February 11-12, 1998.

机译:鼻部组织剂量测定法和“第1类”气体的处理方法:1998年2月11日至12日在北卡罗莱纳州研究三角公园举行的会议的报告。

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摘要

Three organizations, the Basic Acrylic Monomer Manufacturers (BAMM), Methacrylate Producers Association (MPA), and Vinyl Acetate Toxicology Group (VATG), have sponsored development of physiologically based pharmacokinetic (PBPK) models for nasal tissue dosimetry with, respectively, acrylic acid (AA), methyl methacrylate (MMA), and vinyl acetate (VA). These compounds cause lesions in nasal epithelial tissues and are classified as "Category 1" gases within the U.S. EPA (1994) classification scheme. The National Center for Environmental Assessment in the U.S. EPA Office of Research and Development also has continuing interests in refining its methods for dosimetry adjustments when data on mode of action are available for Category 1 gases. A round-table discussion was held in Research Triangle Park, NC, on 11-12 February 1998, to develop a broader appreciation of the key processes and parameters required in developing nasal tissue dosimetry models. The discussions at the round table drew on these three case studies and several background presentations to assess the manner in which chemical-specific and mode-of-action data can be incorporated into nasal dosimetry models. The round table had representation from the U.S. EPA, academia, and industry. This article outlines the presentations and topical areas discussed at the round table and notes recommendations made by participants to extend models for nasal dosimetry and to develop improved data for modeling. The contributions of several disciplines-toxicology, engineering, and physiologically based pharmacokinetic (PBPK) modeling-were evident in the discussions. The integration of these disciplines in creating opportunities for dosimetry model applications in risk assessments has several advantages in the breadth of skills upon which to draw in model development. A disadvantage is in the need to provide venues and develop cross-discipline dialogue necessary to ensure the understanding of cultural attitudes, terminology, and methods. The round-table discussions were fruitful in achieving such enhanced understanding and communication. Subsequent elaboration of these models will benefit from the interactions of these groups at the round table. The round-table discussions have already led to model improvements-as noted in several recently published articles. Participants emphasized several generic data needs in relation to nasal vapor uptake studies in human subjects, to broader discussion of tissue diffusion models, and to extensions to other classes of gases. The round-table articles that are published separately in this issue and the discussions, captured in this overview, provide a glimpse of the state of the science in nasal dosimetry modeling and a clear indication of the growth of and continuing opportunities in this important research area.
机译:三个组织,即基本丙烯酸单体制造商(BAMM),甲基丙烯酸酯生产者协会(MPA)和醋酸乙烯酯毒理学小组(VATG),已经赞助开发用于鼻腔剂量的生理学药代动力学(PBPK)模型,分别使用丙烯酸( AA),甲基丙烯酸甲酯(MMA)和乙酸乙烯酯(VA)。这些化合物在鼻上皮组织中引起损伤,并且在美国EPA(1994)分类方案中被分类为“类别1”气体。当可获得有关第1类气体的作用方式的数据时,美国EPA研究与发展办公室的国家环境评估中心也一直对完善其剂量学调整方法感兴趣。 1998年2月11日至12日,在北卡罗莱纳州三角研究园举行了一次圆桌讨论会,以期对开发鼻组织剂量测定模型所需的关键过程和参数有更广泛的了解。圆桌会议上的讨论借鉴了这三个案例研究和一些背景介绍,以评估将化学特异性和作用方式数据纳入鼻部剂量测定模型的方式。圆桌会议由美国EPA,学术界和工业界派代表参加。本文概述了圆桌会议上讨论的演讲和主题领域,并指出了参与者提出的建议,以扩展鼻腔剂量测定模型并开发改进的建模数据。在讨论中,毒理学,工程学和基于生理的药代动力学(PBPK)建模这几个学科的贡献显而易见。这些学科的集成为风险评估中的剂量学模型应用创造了机会,因此在模型开发的技能广度方面具有多个优势。缺点是需要提供场所并开展必要的跨学科对话,以确保对文化态度,术语和方法的理解。圆桌讨论会在增进这种理解和沟通方面取得了丰硕的成果。这些模型的后续阐述将受益于这些小组在圆桌会议上的互动。正如最近发表的几篇文章所指出的那样,圆桌会议的讨论已经导致了模型的改进。与会者强调了与人类受试者的鼻蒸气吸收研究,组织扩散模型的广泛讨论以及对其他气体种类的扩展有关的几种通用数据需求。本期将单独发表的圆桌会议文章和本概述中的讨论,概述了鼻部剂量学建模的科学状况,并清楚地表明了这一重要研究领域的增长和持续机遇。

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