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      Pathology assessment is necessary to validate translational endpoints in preclinical aging studies

      editorial
      *
      Pathobiology of Aging & Age Related Diseases
      Co-Action Publishing
      geropathology, translational research, anti-aging drugs

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          Abstract

          The Geropathology Research Network has established a plan to identify and use pathology-based surrogate endpoints for aging intervention in preclinical drug studies to provide a predictable and short-term anti-aging drug response in line with clinical trials. The plan involves pathological assessment of tissues and organs from strains of old mice, by independent pathology groups in a concurrent manner in order to characterize the changes in lesion incidence and severity in response to anti-aging drugs at specific time points. This approach allows for connection with translational endpoints of aging, such as serum factors and physiological parameters, between mice and humans. Preclinical drug testing is a critical component of the plan, designed to shorten testing times from lengthy lifespan studies by comparing lesion grades and composite scores in treated and placebo cohorts at cross-sectional time points. In conclusion, a geropathology-based preclinical testing program is a step toward assuring maximum utilization of translational resources and increasing predictability of efficacy of new or repurposed drugs for clinical aging intervention studies.

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          Pathology is a critical aspect of preclinical aging studies

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            Geropathology Research Network Symposium 2015

            Geriatric scientists and pathologists convened in Seattle, WA, on May 7 and 8, 2015, for the first annual symposium of the Geropathology Research Network. The network is a newly formed consortium (Fig. 1) supported by the United States National Institutes of Health (NIH). The mission of the network is to develop ways to translationally enhance the level, scope, and consistency of molecular and anatomic pathology assessment in old animals involved in aging studies using a network of pathologists and scientists with expertise in the pathobiology of aging. Fig. 1 Geropathology Research Network (Executive Core Group). Dr. Felipe Sierra, Director of the Division of Aging Biology at NIH, started the symposium by giving an introductory presentation on the Geroscience Initiative and how the Geropathology Research Network was a key component in plans for helping move the initiative forward. Follow-up presentations were made describing interactive partners including the Geroscience Project by Dr. James Kirkland, Mayo Clinic; the Dog Longevity Project by Dr. Daniel Promislow, University of Washington; and the Intervention Testing Program by Dr. Rich Miller, University of Michigan. These presentations ended with a session devoted to future funding strategies, which included discussions on the advantages of a large initiative approach versus a more focused project-driven approach, and sources of possible funding including NIH, foundations and other private groups, international entities, and commercial corporations. Working groups (Fig. 2) gave presentations describing their goals and objectives and then met in separate sessions to discuss ways of standardizing tissue collection and processing for molecular and anatomic pathology assessments. A translational working group met to discuss ways of using pathology assessment to enhance the value of physiology measurements, with a specific interest in the characterization of frailty in the mouse. The working groups will be publishing follow-up consensus papers in this journal. Fig. 2 The Geropathology Research Network carries out its aims and objectives with four working groups: Molecular Pathology, Translational, Anatomic Pathology, and Bioinformatics. The symposium ended with scientific sessions on 1) Navigating drug development and translation in an academic environment; 2) Aging and health span in consomic mice; 3) Cardiac function, proteomics, and aging interventions; 4) Women's health and clinical aging studies; 5) Preclinical longevity studies in mice; 6) Preclinical anti-aging bioenergetics study in mice; and 7) Clinical anti-aging bioenergetics transition study. The next meeting will be a workshop that will focus on the pathology of frailty in the mouse that will be held in conjunction with the Gerontological Society of America annual meeting in Orlando, FL, on November 18–22, 2015. The next scientific symposium will be in Washington, DC, in March 2016. Warren Ladiges Editor-in-Chief
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              Author and article information

              Journal
              Pathobiol Aging Age Relat Dis
              Pathobiol Aging Age Relat Dis
              PBA
              Pathobiology of Aging & Age Related Diseases
              Co-Action Publishing
              2001-0001
              23 March 2016
              2016
              : 6
              : 10.3402/pba.v6.31478
              Affiliations
              Department of Comparative Medicine, University of Washington, Seattle, WA, USA
              Author notes
              [* ]Correspondence to: Warren Ladiges, Department of Comparative Medicine, University of Washington, Seattle, WA 98195, USA, Email: wladiges@ 123456u.washington.edu
              Article
              31478
              10.3402/pba.v6.31478
              4808080
              27015829
              ae698b43-d256-4850-bcde-a5597419a5c1
              © 2016 Warren Ladiges

              This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial 4.0 International License, permitting all non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

              History
              : 01 March 2016
              : 01 March 2016
              Categories
              Editorial

              Geriatric medicine
              geropathology,translational research,anti-aging drugs
              Geriatric medicine
              geropathology, translational research, anti-aging drugs

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