Abstract

Batten's disease is an inherited neurological disorder affecting humans and also has been documented in a variety of animal species including dogs and sheep. Individuals with this disorder are characterized by normal appearance at birth, followed by insidiously progressive neurological deterioration including retarded mental development and/or dementia, blindness, movement disorders, and seizures. Death is the in- evitable outcome as no treatment is currently available. Only recently has research progress begun to clarify the metabolic basis for this disease in that massive storage of a single protein (subunit c of mitochondrial ATP-synthase) has been established. This finding suggests that Batten's disease is a proteolipid proteinosis, but the primary enzyme defect awaits determination. Furthermore, changes in brain structure and function set in motion by the primary metabolic defect and that lead to the devastating neurological symptoms also are poorly understood. Our goal in these studies is to use a well documented animal model of Batten's disease, canine neuronal ceroid lipofuscinosis, to explore mechanisms of pathogenesis. We have proposed two alternative hypotheses to explain onset and progression of neuronal dysfunction. Based on the observation that cortical GABAergic neurons contain more mitochondria than other cortical neurons, coupled with identification of a mitochondrial enzyme as the major storage product in this disease, we propose that GABAergic neurons are inherently more susceptible to the primary metabolic defect (Hypothesis I). According to this view, early GABAergic cell loss would be predicted to precede pyramidal cell loss, but the ensuing loss of inhibitory function would later accelerate pyramidal cell dysfunction. Alternatively, brain dysfunction in Batten's disease may be due to the same mechanisms believed critical in neuronal storage diseases known to be caused by lysosomal hydrolase defects (Hypothesis II). In these cases ectopic dendrites and associated synaptic connections, axonal spheroids in GABAergic neurons, and alterations in second messenger systems are believed linked to specific aspects of brain dysfunction. We propose to use state-of-the-art electrophysiologic and morphologic techniques to explore these hypotheses. A greater understanding of the mechanisms of brain dysfunction in Batten's e anticipated to give insight not only into the primary metabolic defect in brain, but also into possible ways to treat and/or ameliorate clinical symptoms.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS030163-03
Application #
2268232
Study Section
Special Emphasis Panel (ZRG1-NLS-1 (01))
Project Start
1992-09-07
Project End
1996-08-31
Budget Start
1994-09-01
Budget End
1996-08-31
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Neurosciences
Type
Schools of Medicine
DUNS #
009095365
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Jolly, R D; Brown, S; Das, A M et al. (2002) Mitochondrial dysfunction in the neuronal ceroid-lipofuscinoses (Batten disease). Neurochem Int 40:565-71
Jolly, R D; Walkley, S U (1997) Lysosomal storage diseases of animals: an essay in comparative pathology. Vet Pathol 34:527-48
March, P A; Wurzelmann, S; Walkley, S U (1995) Morphological alterations in neocortical and cerebellar GABAergic neurons in a canine model of juvenile Batten disease. Am J Med Genet 57:204-12
Walkley, S U; March, P A; Schroeder, C E et al. (1995) Pathogenesis of brain dysfunction in Batten disease. Am J Med Genet 57:196-203
Walkley, S U (1995) Pyramidal neurons with ectopic dendrites in storage diseases exhibit increased GM2 ganglioside immunoreactivity. Neuroscience 68:1027-35