Your search keyword '"O'Hearn E"' showing total 6 results

1. Huntington's Disease-like 2 (HDL2) in North America and Japan.

Author

Margolis RL, Holmes SE, Rosenblatt A, Gourley L, O'Hearn E, Ross CA, Seltzer WK, Walker RH, Ashizawa T, Rasmussen A, Hayden M, Almqvist EW, Harris J, Fahn S, MacDonald ME, Mysore J, Shimohata T, Tsuji S, Potter N, Nakaso K, Adachi Y, Nakashima K, Bird T, Krause A, and Greenstein P

Subjects

Adult, Age of Onset, Female, Genotype, Humans, Huntington Disease epidemiology, Japan epidemiology, Male, Membrane Proteins genetics, Middle Aged, North America epidemiology, Pedigree, Repetitive Sequences, Nucleic Acid, Huntington Disease genetics, Trinucleotide Repeat Expansion genetics

Abstract

Huntington's Disease-like 2 (HDL2) is a progressive, autosomal dominant, neurodegenerative disorder with marked clinical and pathological similarities to Huntington's disease (HD). The causal mutation is a CTG/CAG expansion mutation on chromosome 16q24.3, in a variably spliced exon of junctophilin-3. The frequency of HDL2 was determined in nine independent series of patients referred for HD testing or selected for the presence of an HD-like phenotype in North America or Japan. The repeat length, ancestry, and age of onset of all North American HDL2 cases were determined. The results show that HDL2 is very rare, with a frequency of 0 to 15% among patients in the nine case series with an HD-like presentation who do not have the HD mutation. HDL2 is predominantly, and perhaps exclusively, found in individuals of African ancestry. Repeat expansions ranged from 44 to 57 triplets, with length instability in maternal transmission detected in a repeat of r2=0.29, p=0.0098). The results further support the evidence that the repeat expansion at the chromosome 16q24.3 locus is the direct cause of HDL2 and provide preliminary guidelines for the genetic testing of patients with an HD-like phenotype.

Published

2004

2. Clinical signs and symptoms in a large hereditary spastic paraparesis pedigree with a novel spastin mutation.

Author

Nicholas AP, O'Hearn E, Holmes SE, Chen DT, and Margolis RL

Subjects

Adult, DNA Repeat Expansion genetics, Female, Genetic Linkage genetics, Humans, Male, Middle Aged, Pedigree, Polymerase Chain Reaction, Spastin, Videotape Recording, Adenosine Triphosphatases genetics, Calcium-Binding Proteins genetics, Paraparesis, Spastic genetics, Paraparesis, Spastic physiopathology, Point Mutation genetics

Abstract

The most common form of autosomal dominant hereditary spastic paraparesis (HSP), SPG4, is caused by mutations in the spastin gene on chromosome 2p. This disease is characterized by intra- and interfamilial phenotypic variation. To determine the predictive values of clinical signs and symptoms in SPG4, we examined 43 members of a large pedigree with autosomal dominant HSP. We then identified the genetic etiology of the disorder in this family, a novel nonsense mutation in exon 1 of spastin, carried by 24 of the examined family members. The best clinical predictors of positive gene status were the presence of hyperreflexia in the lower extremities, >2 beats of ankle clonus, pes cavus, bladder symptoms and increased tone in the legs. The mean age of onset was 32.2 +/- 7.4 years, but the age of onset was earlier in children from 10 of 12 child-parent gene-positive pairs, with a mean difference of 10.8 +/- 3.3 years. The finding of leg weakness was especially common in older-onset affected family member with leg hyperreflexia. These results suggest that specific clinical signs and symptoms may be of value in differentiating individuals affected with SPG4 from family members with nonspecific neurological findings., (Copyright 2004 Movement Disorder Society)

Published

2004

3. Phenotypic features of Huntington's disease-like 2.

Author

Walker RH, Jankovic J, O'Hearn E, and Margolis RL

Subjects

Adult, Atrophy pathology, Cognition Disorders diagnosis, Female, Humans, Male, Middle Aged, Neuropsychological Tests, Phenotype, Videotape Recording, Brain pathology, Huntington Disease genetics, Trinucleotide Repeat Expansion genetics

Abstract

Huntington's disease-like 2 is an autosomal dominantly inherited disorder due to an expansion of trinucleotide repeats. It resembles classic Huntington's disease in clinical phenotype, inheritance pattern, and neuropathological features. We highlight the clinical features of this disorder, including chorea, dystonia, parkinsonism, and cognitive deficits., (Copyright 2003 Movement Disorder Society)

Published

2003

4. A disorder similar to Huntington's disease is associated with a novel CAG repeat expansion.

Author

Margolis RL, O'Hearn E, Rosenblatt A, Willour V, Holmes SE, Franz ML, Callahan C, Hwang HS, Troncoso JC, and Ross CA

Subjects

Adult, Atrophy, Brain pathology, Chorea genetics, Chorea pathology, Chorea psychology, Female, Genotype, Heredodegenerative Disorders, Nervous System pathology, Heredodegenerative Disorders, Nervous System psychology, Humans, Huntington Disease pathology, Huntington Disease psychology, Magnetic Resonance Imaging, Male, Middle Aged, Pedigree, Phenotype, Heredodegenerative Disorders, Nervous System genetics, Huntington Disease genetics, Mutation genetics, Trinucleotide Repeat Expansion genetics

Abstract

Huntington's disease (HD) is an autosomal dominant disorder characterized by abnormalities of movement, cognition, and emotion and selective atrophy of the striatum and cerebral cortex. While the etiology of HD is known to be a CAG trinucleotide repeat expansion, the pathways by which this mutation causes HD pathology remain unclear. We now report a large pedigree with an autosomal dominant disorder that is clinically similar to HD and that arises from a different CAG expansion mutation. The disorder is characterized by onset in the fourth decade, involuntary movements and abnormalities of voluntary movement, psychiatric symptoms, weight loss, dementia, and a relentless course with death about 20 years after disease onset. Brain magnetic resonance imaging scans and an autopsy revealed marked striatal atrophy and moderate cortical atrophy, with striatal neurodegeneration in a dorsal to ventral gradient and occasional intranuclear inclusions. All tested affected individuals, and no tested unaffecteds, have a CAG trinucleotide repeat expansion of 50 to 60 triplets, as determined by the repeat expansion detection assay. Tests for the HD expansion, for all other known CAG expansion mutations, and for linkage to chromosomes 20p and 4p were negative, indicating that this mutation is novel. Cloning the causative CAG expansion mutation for this new disease, which we have termed Huntington's disease-like 2, may yield valuable insight into the pathogenesis of HD and related disorders.

Published

2001

5. A disorder similar to Huntington's disease is associated with a novel CAG repeat expansion.

Author

Margolis RL, O'Hearn E, Rosenblatt A, Willour V, Holmes SE, Franz ML, Callahan C, Hwang HS, Troncoso JC, and Ross CA

Subjects

Adult, Atrophy, Chorea genetics, Chorea pathology, Chorea psychology, Female, Genotype, Heredodegenerative Disorders, Nervous System pathology, Heredodegenerative Disorders, Nervous System psychology, Humans, Huntington Disease pathology, Huntington Disease psychology, Magnetic Resonance Imaging, Male, Middle Aged, Pedigree, Phenotype, Heredodegenerative Disorders, Nervous System genetics, Huntington Disease genetics, Mutation genetics, Trinucleotide Repeat Expansion genetics

Abstract

Huntington's disease (HD) is an autosomal dominant disorder characterized by abnormalities of movement, cognition, and emotion and selective atrophy of the striatum and cerebral cortex. While the etiology of HD is known to be a CAG trinucleotide repeat expansion, the pathways by which this mutation causes HD pathology remain unclear. We now report a large pedigree with an autosomal dominant disorder that is clinically similar to HD and that arises from a different CAG expansion mutation. The disorder is characterized by onset in the fourth decade, involuntary movements and abnormalities of voluntary movement, psychiatric symptoms, weight loss, dementia, and a relentless course with death about 20 years after disease onset. Brain magnetic resonance imaging scans and an autopsy revealed marked striatal atrophy and moderate cortical atrophy, with striatal neurodegeneration in a dorsal to ventral gradient and occasional intranuclear inclusions. All tested affected individuals, and no tested unaffecteds, have a CAG trinucleotide repeat expansion of 50 to 60 triplets, as determined by the repeat expansion detection assay. Tests for the HD expansion, for all other known CAG expansion mutations, and for linkage to chromosomes 20p and 4p were negative, indicating that this mutation is novel. Cloning the causative CAG expansion mutation for this new disease, which we have termed Huntington's disease-like 2, may yield valuable insight into the pathogenesis of HD and related disorders.

Published

2001

6. Dual serotoninergic projections to forebrain in the rat: morphologically distinct 5-HT axon terminals exhibit differential vulnerability to neurotoxic amphetamine derivatives.

Author

Mamounas LA, Mullen CA, O'Hearn E, and Molliver ME

Subjects

Animals, Axons drug effects, Cerebral Cortex anatomy & histology, Cerebral Cortex drug effects, Dose-Response Relationship, Drug, Hippocampus anatomy & histology, Hippocampus drug effects, Immunohistochemistry, Male, Organ Specificity, Prosencephalon drug effects, Rats, Rats, Inbred Strains, Reference Values, Serotonin metabolism, 3,4-Methylenedioxyamphetamine toxicity, Axons ultrastructure, Cerebral Cortex pathology, Hippocampus pathology, Neurotoxins toxicity, Prosencephalon anatomy & histology, Prosencephalon pathology, Serotonin analysis, p-Chloroamphetamine toxicity

Abstract

The cerebral cortex of the rat and other mammals is innervated by two morphologically distinct classes of serotoninergic (5-HT) axon terminals: fine axons with minute varicosities and beaded axons characterized by large, spherical varicosities. Fine and beaded 5-HT axons exhibit different regional and laminar distributions in forebrain and arise from separate brainstem nuclei, the dorsal and median raphe nuclei, respectively. The present neuroanatomic study, based on immunocytochemical methods to visualize 5-HT axons, demonstrates that the two axon types differ markedly in their vulnerability to the neurotoxic amphetamine derivatives, methylenedioxyamphetamine (MDA), and p-chloroamphetamine (PCA). While both drugs cause extensive degeneration of fine 5-HT axons throughout forebrain, beaded 5-HT axons are consistently spared. Fine 5-HT axons, which richly innervate most regions of dorsal forebrain in control rats, are rarely seen 2 weeks after treatment with MDA or PCA; this loss of fine axons reflects a marked denervation that persists for months after drug administration. The serotoninergic axon terminals remaining after MDA or PCA administration are almost entirely of the beaded type and appear to be unaffected by both drugs. Over a wide range of doses (2.5-40 mg/kg PCA) and survival times (2 weeks to 2 months), these spared 5-HT axons with large, spherical varicosities cannot be distinguished from the normal, beaded 5-HT axons in control rats by morphologic criteria. Moreover, beaded 5-HT axons exhibit a highly characteristic regional distribution which is the same in control as in MDA- and PCA-treated rats: these axons innervate specific zones or layers within parietal and occipital cortex, hippocampus, cingulate cortex, entorhinal cortex, and the olfactory bulb, among other forebrain areas, and they form a dense plexus lining the ventricular system. Taken together, the results of this study demonstrate that fine 5-HT axons are highly vulnerable to the neurotoxic effects of the amphetamine derivatives MDA and PCA, while beaded 5-HT axons are markedly resistant. These findings are consistent with the hypothesis that there are two anatomically and functionally distinct sets of serotoninergic neurons projecting to forebrain. While both of these neuronal systems utilize 5-HT as a neurotransmitter, they differ in several features: 1) origin from separate nuclei in the brainstem (the dorsal and median raphe), 2) two types of morphologically distinct axon terminals, 3) markedly different distribution and innervation patterns in forebrain, and 4) dissimilar pharmacological properties. The results further suggest that psychotropic amphetamine derivatives have a selective action upon fine serotoninergic axons that arise from the dorsal raphe nucleus.

Published

1991