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Featured researches published by David Stong.


Experimental Neurology | 1993

Insulin-like Growth Factor-I: Potential for Treatment of Motor Neuronal Disorders

Michael E. Lewis; Nicola Neff; Patricia C. Contreras; David Stong; Ronald W. Oppenheim; Peter E. Grebow; Jeffry L. Vaught

Motor neuronal disorders, such as the loss of spinal cord motor neurons in amyotrophic lateral sclerosis or the degeneration of spinal cord motor neuron axons in certain peripheral neuropathies, present a unique opportunity for therapeutic intervention with neurotrophic proteins. Normally, such proteins do not cross the blood-brain barrier, but spinal cord motor neuron axons and nerve terminals lie outside the barrier and thus may be targeted by systemic administration of protein growth factors. Insulin-like growth factor-I (IGF-I) receptors are present in the spinal cord, and, like members of the neurotrophin receptor family, IGF-I receptors mediate signal transduction via a tyrosine kinase domain. IGF-I was found to prevent the loss of choline acetyltransferase activity in embryonic spinal cord cultures, as well as to reduce the programmed cell death of motor neurons in vivo during normal development or following axotomy or spinal transection. Consistent with earlier reports that IGF-I enhances motor neuronal sprouting in vivo, subcutaneous administration of IGF-I increases muscle endplate size in rats. Subcutaneous injections of IGF-I also accelerate functional recovery following sciatic nerve crush in mice, as well as attenuate the peripheral motor neuropathy induced by chronic administration of the cancer chemotherapeutic agent vincristine in mice. Doses of IGF-I that accelerate recovery from sciatic nerve crush in mice result in elevated serum levels of IGF-I which are similar to those obtained following subcutaneous injections of formulated recombinant human IGF-I (Myotrophin) in normal human subjects. Based on these findings, together with evidence of safety in animals and man, clinical trials of recombinant human IGF-I have been initiated in patients with amyotrophic lateral sclerosis and are planned to begin soon in patients with chemotherapy-induced peripheral neuropathies.


Archive | 1994

Acetamide derivative having defined particle size

Peter E. Grebow; Vincent Corvari; David Stong


Annals of the New York Academy of Sciences | 1993

Effects of Multiple Subcutaneous Doses of rhIGF-1 on Total and Free IGF-1 Levels and Blood Glucose in Humans

David Stong; Robert Raskin


Archive | 1995

Modafinil having defined particle size

Peter E. Grebow; Vincent Corvari; David Stong


Archive | 1997

Defineeritud osakeste suurusega modafiniil

Peter E. Grebow; Vincent Corvari; David Stong


Archive | 1997

Hiukkkaskooltaan defined modafinil

Peter E. Grebow; Vincent Corvari; David Stong


Archive | 1997

Hiukkkaskooltaan määritelty modafiniili

Peter E. Grebow; Vincent Corvari; David Stong


Archive | 1995

Modafinilpartikel mit definierter Korngrössenverteilung

Peter E. Grebow; David Stong; Vincent Corvari


Archive | 1995

Modafinilpartikel mit definierter Korngrössenverteilung Modafinil particles with defined particle size distribution

E Grebow; Vincent Corvari; David Stong


Archive | 1995

Mondafinilo particles having a defined granulometry.

Vincent Corvari; Peter E. Grebow; David Stong

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