Frataxin deficiency increases cyclooxygenase 2 and prostaglandins in cell and animal models of Friedreich's ataxia

Al-Mahdawi; Al-Mahdawi; Block; Campuzano; Campuzano; Capdevila; Capdevila; Castaldo; Chantrel-Groussard; Chen; Cossee; Dewitt; Durr; Durr; Feng; Genki Hayashi; Gino Cortopassi; Harding; John W. Newman; Kang; Koeppen; Li; Liang; Lin; Lu; Mark Pook; Masi; Michael; Miranda; Node; O'Flaherty; Paupe; Piemonte; Piro; Praticò; Qin; Ristow; Rojo; Samuelsson; Sanchez-Mejia; Schulz; Shan; Shi; Shin; Small; Smith; Strokin; Tan; Teismann; Theresa L. Pedersen; Tian; Wardlaw; Wong; Wong; Xi; Yan; Yan Shen; Zhang

research

Frataxin deficiency increases cyclooxygenase 2 and prostaglandins in cell and animal models of Friedreich's ataxia

Authors: Al-Mahdawi
Al-Mahdawi
Block
Campuzano
Campuzano
Capdevila
Capdevila
Castaldo
Chantrel-Groussard
Chen
Cossee
Dewitt
Durr
Durr
Feng
Genki Hayashi
Gino Cortopassi
Harding
John W. Newman
Kang
Koeppen
Li
Liang
Lin
Lu
Mark Pook
Masi
Michael
Miranda
Node
O'Flaherty
Paupe
Piemonte
Piro
Praticò
Qin
Ristow
Rojo
Samuelsson
Sanchez-Mejia
Schulz
Shan
Shi
Shin
Small
Smith
Strokin
Tan
Teismann
Theresa L. Pedersen
Tian
Wardlaw
Wong
Wong
Xi
Yan
Yan Shen
Zhang
Publication date: 7 August 2014
Publisher: 'Oxford University Press (OUP)'
Doi

Abstract

© The Author 2014. Published by Oxford University Press This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.An inherited deficiency of the mitochondrial protein frataxin causes Friedreich's ataxia (FRDA); the mechanism by which this deficiency triggers neuro- and cardio-degeneration is unclear. Microarrays of neural tissue of animal models of the disease showed decreases in antioxidant genes, and increases in inflammatory genes. Cyclooxygenase (COX)-derived oxylipins are important mediators of inflammation. We measured oxylipin levels using tandem mass spectrometry and ELISAs in multiple cell and animal models of FRDA. Mass spectrometry revealed increases in concentrations of prostaglandins, thromboxane B2, 15-HETE and 11-HETE in cerebellar samples of knockin knockout mice. One possible explanation for the elevated oxylipins is that frataxin deficiency results in increased COX activity. While constitutive COX1 was unchanged, inducible COX2 expression was elevated over 1.35-fold (P < 0.05) in two Friedreich's mouse models and Friedreich's lymphocytes. Consistent with higher COX2 expression, its activity was also increased by 58% over controls. COX2 expression is driven by multiple transcription factors, including activator protein 1 and cAMP response element-binding protein, both of which were elevated over 1.52-fold in cerebella. Taken together, the results support the hypothesis that reduced expression of frataxin leads to elevation of COX2-mediated oxylipin synthesis stimulated by increases in transcription factors that respond to increased reactive oxygen species. These findings support a neuroinflammatory mechanism in FRDA, which has both pathomechanistic and therapeutic implications.The study was supported by NIH grants NS077777, EY012245 and AG025532 to G.A.C., and USDA-ARS Intramural Projects 5306-51530-019-00D and 1 U24 DK097154-01 to J.W.N. Funding to pay the Open Access publication charges for this article was provided by the NIH