Nicotinic receptor abnormalities in the cerebellar cortex in autism

doi:10.1093/brain/awf160

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Brain, Vol. 125, No. 7, 1483-1495, July 2002
© 2002 Guarantors of Brain

Nicotinic receptor abnormalities in the cerebellar cortex in autism

M. Lee¹, C. Martin-Ruiz¹, A. Graham¹, J. Court¹, E. Jaros², R. Perry², P. Iversen³, M. Bauman⁴ and E. Perry¹

¹ MRC/University of Newcastle Upon Tyne Development in Clinical Brain Ageing and ² Department of Neuropathology, Newcastle General Hospital, Newcastle upon Tyne, UK, ³ Cure Autism Now, Los Angeles, CA and ⁴ Children’s Neurology Service, Harvard Medical School, Massachusetts’s General Hospital, Boston, MA, USA

Correspondence to: E. K. Perry, MRC Building, Newcastle General Hospital, Westgate Road, Newcastle upon Tyne NE4 6BE, UK E-mail: e.k.perry{at}ncl.ac.uk

Autism is a common developmental disorder associated with structuraland inferred neurochemical abnormalities of the brain. Cerebellarabnormalities frequently have been identified, based on neuroimagingor neuropathology. Recently, the cholinergic neurotransmittersystem has been implicated on the basis of nicotinic receptorloss in the cerebral cortex. Cerebellar cholinergic activitieswere therefore investigated in autopsy tissue from a seriesof autistic individuals. The presynaptic cholinergic enzyme,choline acetyltransferase, together with nicotinic and muscarinicreceptor subtypes were compared in the cerebellum from age-matchedmentally retarded autistic (eight), normal control (10) andnon-autistic mentally retarded individuals (11). The nicotinicreceptor binding the agonist epibatidine (the high affinityreceptor subtype, consisting primarily of ${alpha}$ 3 and ${alpha}$ 4, togetherwith ß2 receptor subunits) was significantly reducedby 40–50% in the granule cell, Purkinje and molecularlayers in the autistic compared with the normal group (P < 0.05).There was an opposite increase (3-fold) in the nicotinic receptorbinding ${alpha}$ -bungarotoxin (to the ${alpha}$ 7 subunit) which reached significancein the granule cell layer (P < 0.05). These receptorchanges were paralleled by a significant reduction (P < 0.05)and non-significant increase, respectively, of ${alpha}$ 4 and ${alpha}$ 7 receptorsubunit immunoreactivity measured using western blotting. Immunohistochemicallyloss of ${alpha}$ ₄reactivity was apparent from Purkinje and the othercell layers, with increased ${alpha}$ 7 reactivity in the granule celllayer. There were no significant changes in choline acetyltransferaseactivity, or in muscarinic M1 and M2 receptor subtypes in autism.In the non-autistic mentally retarded group, the only significantabnormality was a reduction in epibatidine binding in the granulecell and Purkinje layers. In two autistic cases examined histologically,Purkinje cell loss was observed in multiple lobules throughoutthe vermis and hemispheres. This was more severe in one casewith epilepsy, which also showed vermis folial malformation.The case with less severe Purkinje cell loss also showed cerebellarwhite matter thinning and demyelination. These findings indicatea loss of the cerebellar nicotinic ${alpha}$ 4 receptor subunit in autismwhich may relate to the loss of Purkinje cells, and a compensatoryincrease in the ${alpha}$ 7 subunit. It remains to be determined how thesereceptor abnormalities are involved in neurodevelopment in autismand what is the relationship to mental function. Since nicotinicreceptor agonists enhance attentional function and also inducean elevation in the high affinity receptor, nicotinic therapyin autism may be worth considering.

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