Efficacy of rosiglitazone in a genetically defined population with mild-to-moderate Alzheimer's disease

Risner, Marcus E.; Saunders, Ann M.; Altman, Jill F.B.; Ormandy, George C.; Craft, Suzanne; Foley, I.; Zvartau-Hind, Marina; Hosford, David A.; Roses, A D

doi:10.1038/sj.tpj.6500369

Cited by 622 publications

(456 citation statements)

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“…58 This was also observed in the rosglitazone study. 57 In a follow-up study of 31 subjects with mild to moderate probable AD, E4(Ϫ) subjects were found to have significantly lower glucose disposal rates. 55 High-fasting insulin and low-glucose disposal rates both suggest that E4(Ϫ) subjects are insulin resistant, and correcting this insulin resistant state by administration of insulin either systemically, 55 nasally, 54 or by use of the insulin sensitizing agent rosglitazone 57 may explain the beneficial effects seen in these studies.…”

Section: Ketosis and Admentioning

confidence: 99%

“…E4(ϩ) subjects show no difference or got slightly worse. 57 Why would these treatments work preferentially in participants lacking the AD risk factor APOE4? In the rosglitazone study it was proposed that fragments of ApoE4 protein interfered with mitochondrial function and prevented E4 carriers from responding to PPAR␥ activation.…”

Section: Ketosis and Admentioning

confidence: 99%

“…In the rosglitazone study it was proposed that fragments of ApoE4 protein interfered with mitochondrial function and prevented E4 carriers from responding to PPAR␥ activation. 57 It is possible that such damaged mitochondria also fail to metabolize KB.…”

Section: Ketosis and Admentioning

confidence: 99%

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Ketone Bodies as a Therapeutic for Alzheimer's Disease

Henderson¹

2008

Neurotherapeutics

294

116

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Summary: An early feature of Alzheimer's disease (AD) is region-specific declines in brain glucose metabolism. Unlike other tissues in the body, the brain does not efficiently metabolize fats; hence the adult human brain relies almost exclusively on glucose as an energy substrate. Therefore, inhibition of glucose metabolism can have profound effects on brain function. The hypometabolism seen in AD has recently attracted attention as a possible target for intervention in the disease process. One promising approach is to supplement the normal glucose supply of the brain with ketone bodies (KB), which include acetoacetate, ␤-hydroxybutyrate, and acetone. KB are normally produced from fat stores when glucose supplies are limited, such as during prolonged fasting. KB have been induced both by direct infusion and by the administration of a high-fat, low-carbohydrate, low-protein, ketogenic diets. Both approaches have demonstrated efficacy in animal models of neurodegenerative disorders and in human clinical trials, including AD trials. Much of the benefit of KB can be attributed to their ability to increase mitochondrial efficiency and supplement the brain's normal reliance on glucose. Research into the therapeutic potential of KB and ketosis represents a promising new area of AD research.

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Section: Ketosis and Admentioning

confidence: 99%

Section: Ketosis and Admentioning

confidence: 99%

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Ketone Bodies as a Therapeutic for Alzheimer's Disease

Henderson¹

2008

Neurotherapeutics

294

116

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“…A Phase III clinical trial of pioglitazone for MCI due to AD is currently underway (ClinicalTrials.gov identifier: NCT01931566). Rosiglitazone tested in MCI and early AD showed improved delayed recall [94], but failed to show significant cognitive benefits in a subsequent larger trial with over 1400 patients with mild-tomoderate AD (ClinicalTrials.gov identifier: NCT00490568) [95]. One major challenge for these candidates is they have poor BBB penetration [78].…”

Section: Mitochondrial Bioenergetics As a Therapeutic Targetmentioning

confidence: 99%

Targeting the Prodromal Stage of Alzheimer's Disease: Bioenergetic and Mitochondrial Opportunities

2015

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Alzheimer's disease (AD) has a complex and progressive neurodegenerative phenotype, with hypometabolism and impaired mitochondrial bioenergetics among the earliest pathogenic events. Bioenergetic deficits are well documented in preclinical models of mammalian aging and AD, emerge early in the prodromal phase of AD, and in those at risk for AD. This review discusses the importance of early therapeutic intervention during the prodromal stage that precedes irreversible degeneration in AD. Mechanisms of action for current mitochondrial and bioenergetic therapeutics for AD broadly fall into the following categories: 1) glucose metabolism and substrate supply; 2) mitochondrial enhancers to potentiate energy production; 3) antioxidants to scavenge reactive oxygen species and reduce oxidative damage; 4) candidates that target apoptotic and mitophagy pathways to either remove damaged mitochondria or prevent neuronal death. Thus far, mitochondrial therapeutic strategies have shown promise at the preclinical stage but have had little-to-no success in clinical trials. Lessons learned from preclinical and clinical therapeutic studies are discussed. Understanding the bioenergetic adaptations that occur during aging and AD led us to focus on a systems biology approach that targets the bioenergetic system rather than a single component of this system. Bioenergetic system-level therapeutics personalized to bioenergetic phenotype would target bioenergetic deficits across the prodromal and clinical stages to prevent and delay progression of AD.

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“…11 Nonetheless, smaller studies have generated some striking findings. For instance, the PPARg agonist rosiglitazone (RSG) was efficacious only in e4-negative patients, 12 making e4 genotype a candidate RSG responder/ non-responder biomarker for AD. Surprisingly, e4 allele carriers treated with placebo in this study showed a slower rate of cognitive decline than e4 non-carriers.…”

mentioning

confidence: 99%