Orally Administered Amyloidophilic Compound Is Effective in Prolonging the Incubation Periods of Animals Cerebrally Infected with Prion Diseases in a Prion Strain-Dependent Manner

Kawasaki, Yoshihisa; Kawagoe, Kei-ichi; Chen, Chun‐Jen; Teruya, Kenta; Sakasegawa, Yuji; Doh‐ura, Katsumi

doi:10.1128/jvi.01563-07

Cited by 99 publications

(126 citation statements)

References 32 publications

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“…4H) and quinacrine (Fig. 4J), consistent with previous reports (11,15). Compound B treatment up to 10 μM was ineffective against the IND24-resistant strain (Fig.…”

Section: -Amt Treatment Altered the Characteristics Of Prions In Brasupporting

confidence: 91%

“…Unlike quinacrine, treatment with Compound B or anle138b substantially extended the survival of prion-infected mice (15)(16)(17). Prions from the brains of mice treated with Compound B showed different ratios of mono-to diglycosylated PrP Sc compared with the inoculum (15), and had a different conformational stability (17), but it was not determined whether the resulting prions were resistant to further treatment with Compound B.…”

mentioning

confidence: 99%

“…Prions from the brains of mice treated with Compound B showed different ratios of mono-to diglycosylated PrP Sc compared with the inoculum (15), and had a different conformational stability (17), but it was not determined whether the resulting prions were resistant to further treatment with Compound B. Importantly, Compound B contains a hydrazone functionality likely under physiologic conditions to produce an aryl hydrazine, a toxic metabolite and carcinogen (18), limiting its utility as a therapeutic (17).…”

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confidence: 99%

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Drug resistance confounding prion therapeutics

Berry

Lü

Geva

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

123

202

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Significance As people live longer, the prevalence and economic impact of neurodegenerative diseases rise. No cures or effective treatments exist for any of these fatal disorders, so identifying potential therapeutics that extend survival in animal models is vital. Many neurodegenerative illnesses have been shown to be caused by the accumulation of self-propagating misfolded proteins—the hallmark of prion diseases. We report the efficacy of 2-aminothiazoles, which were identified in cell-based screens as antiprion compounds, in extending the lives of prion-infected animals. Efficacy was limited by the development of drug-resistant prions, which is likely to have important implications for creating therapeutics in many different neurodegenerative diseases.

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“…4H) and quinacrine (Fig. 4J), consistent with previous reports (11,15). Compound B treatment up to 10 μM was ineffective against the IND24-resistant strain (Fig.…”

Section: -Amt Treatment Altered the Characteristics Of Prions In Brasupporting

confidence: 91%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Drug resistance confounding prion therapeutics

Berry

Lü

Geva

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

123

202

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“…Interestingly, the use of pentosan polysulfate (PPS) combined with iron(III) meso-tetra(4-sulfonatophenyl)porphine (FeTAP) produced a synergistic prolongation of incubation times in prion-infected mice (8). Although the combination of PPS and FeTAP had to be administered intracerebrally to effect a prolongation of the incubation period, the oral administration of 4-pyridinecarboxaldehyde-2-[4-(5-oxazolyl)phenyl]hydrazone (cpd-B) produced a doubling of the incubation time in RML-infected Tga20 mice when started midway through the incubation period (41).…”

Section: Discussionmentioning

confidence: 99%

“…Cpd-B was the most effective in prolonging the incubation times of RML-infected mice but had little effect on the incubation times of either Syrian hamsters or Tg(SHaPrP)7 mice inoculated intracerebrally with 263K prions (41). Combining cpd-B with a GSI will be of interest in the continuing search for an effective therapeutic regimen for CJD.…”

Section: Discussionmentioning

confidence: 99%

A γ-secretase inhibitor and quinacrine reduce prions and prevent dendritic degeneration in murine brains

Spilman¹,

Lessard

Sattavat³

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

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In prion-infected mice, both the Notch-1 intracellular domain transcription factor (NICD) and the disease-causing prion protein (PrP Sc ) increase in the brain preceding dendritic atrophy and loss. Because the drug LY411575 inhibits the ␥-secretase-catalyzed cleavage of Notch-1 that produces NICD, we asked whether this ␥-secretase inhibitor (GSI) might prevent dendritic degeneration in mice with scrapie. At 50 d postinoculation with Rocky Mountain Laboratory (RML) prions, mice were given GSI orally for 43-60 d. Because we did not expect GSI to produce a reduction of PrP Sc levels in brain, we added quinacrine (Qa) to the treatment regimen. Qa inhibits PrP Sc formation in cultured cells. The combination of GSI and Qa reduced PrP Sc by Ϸ95% in the neocortex and hippocampus but only Ϸ50% in the thalamus at the site of prion inoculation. The GSI plus Qa combination prevented dendritic atrophy and loss, but GSI alone did not. Even though GSI reduced NICD levels to a greater extent than GSI plus Qa, it was unable to prevent dendritic degeneration. Whether a balance between NICD and dendrite growth-stimulating factors was achieved with GSI plus Qa but not GSI alone remains to be determined. Although the combination of GSI and Qa diminished PrP Sc in the brains of RML-infected mice, GSI toxicity prevented us from being able to assess the effect the GSI plus Qa combination on incubation times. Whether less toxic GSIs can be used in place of LY411575 to prolong survival remains to be determined.Creutzfeldt-Jakob disease ͉ neuropathology ͉ prion disease ͉ therapy ͉ scrapie

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Prion Disease Therapy: Trials and Tribulations

Sim

Caughey

2010

Protein Misfolding Diseases

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Orally Administered Amyloidophilic Compound Is Effective in Prolonging the Incubation Periods of Animals Cerebrally Infected with Prion Diseases in a Prion Strain-Dependent Manner

Cited by 99 publications

References 32 publications

Drug resistance confounding prion therapeutics

Drug resistance confounding prion therapeutics

A γ-secretase inhibitor and quinacrine reduce prions and prevent dendritic degeneration in murine brains

Prion Disease Therapy: Trials and Tribulations

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