Subcutaneous IGF-1 is not beneficial in 2-year ALS trial

Sorenson, Eric J.; Windbank, A. J.; Mandrekar, J. N.; Bamlet, William R.; Appel, Stanley H.; Armon, C.; Barkhaus, P. E.; Bosch, P.; Boylan, Khrista; David, William S.; Feldman, Eva L.; Glass, Jonathan D.; Gutmann, Laurie; Katz, José; King, Wendy; Luciano, C. A.; McCluskey, Leo; Nash, S.; Newman, D. S.; Pascuzzi, R. M.; Pioro, E.; Sams, L. J.; Scelsa, S.; Simpson, Ericka; Subramony, S. H.; Tiryaki, Ezgi; Thornton, C. A.

doi:10.1212/01.wnl.0000335970.78664.36

Cited by 228 publications

(136 citation statements)

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“…IGF‐1 is known to have a neurotrophic effect on motor neurons 30. To date IGF‐1 ‐based therapies have little beneficial effect upon systemic or intrathecal administration in ALS patients 19, 20, 21. The poor outcomes of these studies may possibly be due to low availability of IGF‐1 as free IGF‐1 is reduced while IGF‐1 R expression is upregulated in both the CNS and muscle of ALS patients 31, 32.…”

Section: Discussionmentioning

confidence: 99%

“…In recent years, many studies have focused on gene delivery of growth factors to the central nervous system (CNS) in order to slow disease progression in animal models of ALS utilizing the intramuscular,10, 11, 12, 13 intracerebral,14, 15 intracerebroventricular16, and intraspinal17, 18 routes of administration. Despite the encouraging results of these studies, subcutaneous delivery of recombinant human insulin‐like growth factor 1 IGF‐1 ( rhIGF‐1) in ALS patients had little effect in 3 clinical trials 19, 20, 21. Each of these approaches has its own limitations which may negate achieving efficacy in ALS patients.…”

Section: Introductionmentioning

confidence: 99%

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αCAR IGF‐1 vector targeting of motor neurons ameliorates disease progression in ALS mice

Eleftheriadou

Manolaras

Irvine

et al. 2016

Ann Clin Transl Neurol

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ObjectiveWe have previously described the generation of coxsackievirus and adenovirus receptor (α CAR)‐targeted vector, and shown that intramuscular delivery in mouse leg muscles resulted in specific retrograde transduction of lumbar‐motor neurons (MNs). Here, we utilized the α CAR‐targeted vector to investigate the in vivo neuroprotective effects of lentivirally expressed IGF‐1 for inducing neuronal survival and ameliorating the neuropathology and behavioral phenotypes of the SOD1G93A mouse model of ALS.MethodsWe produced cell factories of IGF‐1 expressing lentiviral vectors (LVs) bearing α CAR or Vesicular Stomatitis Virus glycoprotein (VSV‐G) on their surface so as to compare neuroprotection from MN transduced versus muscle transduced cells. We performed intramuscular delivery of either α CAR IGF‐1 or VSVG IGF‐1 LVs into key muscles of SOD1G93A mice prior to disease onset at day 28. Motor performance, coordination and gait analysis were assessed weekly.ResultsWe observed substantial therapeutic efficacy only with the α CAR IGF‐1 LV pretreatment with up to 50% extension of survival compared to controls. α CAR IGF‐1 LV‐treated animals retained muscle tone and had better motor performance during their prolonged survival. Histological analysis of spinal cord samples at end‐stage further confirmed that α CAR IGF‐1 LV treatment delays disease onset by increasing MN survival compared with age‐matched controls. Intrastriatal injection of α CAR eGFP LV in rats leads to transduction of neurons and glia locally and neurons in olfactory bulb distally.InterpretationOur data are indicative of the efficacy of the α CAR IGF‐1 LV in this model and support its candidacy for early noninvasive neuroprotective therapy in ALS.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

αCAR IGF‐1 vector targeting of motor neurons ameliorates disease progression in ALS mice

Eleftheriadou

Manolaras

Irvine

et al. 2016

Ann Clin Transl Neurol

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“…Thus, for example, AAV vectors injected into brains to deliver NGF in Alzheimer's disease [248], neurturin or glia cell-derived neurotrophic factor (GDNF) in Parkinson's disease [249,250], and insulin-like growth factor I in ALS [251] have proven safe, but with no demonstrable benefit. This apparent lack of benefit may relate to the late stage of the diseases at the time of treatment, the progressive nature of the diseases and/or the inability to quantitate minor benefit with lack of a robust biomarker [201].…”

Section: Changing the Brain Environmentmentioning

confidence: 99%

Gene Therapy for the Nervous System: Challenges and New Strategies

et al. 2014

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Current clinical treatments for central nervous system (CNS) diseases, such as Parkinson's disease and glioblastoma do not halt disease progression and have significant treatment morbidities. Gene therapy has the potential to "permanently" correct disease by bringing in a normal gene to correct a mutant gene deficiency, knocking down mRNA of mutant alleles, and inducing cell-death in cancer cells using transgenes encoding apoptosis-inducing proteins. Promising results in clinical trials of eye disease (Leber's congenital aumorosis) and Parkinson's disease have shown that genebased neurotherapeutics have great potential. The recent development of genome editing technology, such as zinc finger nucleases, TALENS, and CRISPR, has made the ultimate goal of gene correction a step closer. This review summarizes the challenges faced by gene-based neurotherapeutics and the current and recent strategies designed to overcome these barriers. We have chosen the following challenges to focus on in this review: (1) delivery vehicles (both virus and nonviral), (2) use of promoters for vector-mediated gene expression in CNS, and (3) delivery across the blood-brain barrier. The final section (4) focuses on promising pre-clinical/clinical studies of neurotherapeutics.

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“…There have been several treatment trials using free IGF-1 therapy in amyotrophic lateral sclerosis (ALS) [68][69][70] and one trial of free IGF-1 complexed with IGF-1 binding protein-3 in myotonic dystrophy [71]. ALS trials failed to show a clear beneficial result but demonstrated safety of IGF-1 in these patients.…”

Section: Insulin-like Growth Factormentioning

confidence: 99%