H. Lee Vahlsing scite author profile

Cholinergic neuron loss is a cardinal feature of Alzheimer disease. Nerve growth factor (NGF) stimulates cholinergic function, improves memory and prevents cholinergic degeneration in animal models of injury, amyloid overexpression and aging. We performed a phase 1 trial of ex vivo NGF gene delivery in eight individuals with mild Alzheimer disease, implanting autologous fibroblasts genetically modified to express human NGF into the forebrain. After mean follow-up of 22 months in six subjects, no long-term adverse effects of NGF occurred. Evaluation of the Mini-Mental Status Examination and Alzheimer Disease Assessment Scale-Cognitive subcomponent suggested improvement in the rate of cognitive decline. Serial PET scans showed significant (P < 0.05) increases in cortical 18-fluorodeoxyglucose after treatment. Brain autopsy from one subject suggested robust growth responses to NGF. Additional clinical trials of NGF for Alzheimer disease are warranted.

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Delayed treatment with nerve growth factor reverses the apparent loss of cholinergic neurons after acute brain damage

Hagg

Manthorpe

Vahlsing

et al. 1988

Experimental Neurology

225

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Long-term effects of spinal cord transection on fast and slow rat skeletal muscle

Lieber

Johansson

Vahlsing

et al. 1986

Experimental Neurology

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H. Lee Vahlsing

A phase 1 clinical trial of nerve growth factor gene therapy for Alzheimer disease

Delayed treatment with nerve growth factor reverses the apparent loss of cholinergic neurons after acute brain damage

Long-term effects of spinal cord transection on fast and slow rat skeletal muscle

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