Animal models and human tissue compared to better understand and treat the epilepsies

Author:

Milior Giampaolo1,Morin‐Brureau Mélanie2,Pallud Johan345,Miles Richard1,Huberfeld Gilles16ORCID

Affiliation:

1. Center for Interdisciplinary Research in Biology, College de France, CNRS, INSERM Université PSL Paris France

2. INSERM, Sorbonne University, UMRS 938 Saint‐Antoine Research Center, Immune System and Neuroinflammation Laboratory Hôpital Saint‐Antoine Paris France

3. Department of Neurosurgery GHU Paris—Hôpital Sainte‐Anne Paris France

4. Université Paris Cité Paris France

5. INSERM, U1266, IMA‐Brain Institut de Psychiatrie et Neurosciences de Paris Paris France

6. Neurology Department Hôpital Fondation Adolphe de Rothschild Paris France

Abstract

AbstractAnimal models of human brain disorders permit researchers to explore disease mechanisms and to test potential therapies. However, therapeutic molecules derived from animal models often translate poorly to the clinic. Although human data may be more relevant, experiments on patients are constrained, and living tissue is unavailable for many disorders. Here, we compare work on animal models and on human tissue for three epileptic syndromes where human tissue is excised therapeutically: (1) acquired temporal lobe epilepsies, (2) inherited epilepsies associated with cortical malformations, and (3) peritumoral epilepsies. Animal models rest on assumed equivalencies between human brains and brains of mice, the most frequently used model animal. We ask how differences between mouse and human brains could influence models. General principles and compromises in model construction and validation are examined for a range of neurological diseases. Models may be judged on how well they predict novel therapeutic molecules or new mechanisms. The efficacy and safety of new molecules are evaluated in clinical trials. We judge new mechanisms by comparing data from work on animal models with data from work on patient tissue. In conclusion, we stress the need to cross‐verify findings from animal models and from living human tissue to avoid the assumption that mechanisms are identical.

Funder

H2020 European Research Council

Publisher

Wiley

Subject

Neurology (clinical),Neurology

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