Nonpeptidic Lysosomal Modulators Derived from Z-Phe-Ala-Diazomethylketone for Treating Protein Accumulation Diseases

Viswanathan, Kishore; Hoover, Dennis J.; Hwang, Jeannie; Wisniewski, Meagan L.; Ikonne, Uzoma; Bahr, Ben A.; Wright, Dennis L.

doi:10.1021/ml300197h

Cited by 15 publications

(15 citation statements)

References 23 publications

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“…Note Added in Proof-A recent paper by K. Viswanathan et al (33) identified new cathepsin B-enhancing small molecules that protect against synaptic deficits in a transgenic model of AD.…”

Section: Acknowledgments-we Thank Drs Hidde Ploegh and Christoph Petmentioning

confidence: 99%

Cathepsin B Degrades Amyloid-β in Mice Expressing Wild-type Human Amyloid Precursor Protein

Wang

Sun

Zhou

et al. 2012

Journal of Biological Chemistry

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Background:The CysC-CatB axis affects levels of A␤ from hAPP with familial mutations. How it affects A␤ from wild-type hAPP remains unknown. Results: Enhancing CatB reduces and deleting CatB elevates levels of A␤ derived from wild-type hAPP. Conclusion: The CysC-CatB axis regulates A␤ degradation similarly regardless of familial mutations. Significance: Enhancing CatB activity as an A␤-lowering strategy might be applicable in familial and sporadic AD.

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“…Note Added in Proof-A recent paper by K. Viswanathan et al (33) identified new cathepsin B-enhancing small molecules that protect against synaptic deficits in a transgenic model of AD.…”

Section: Acknowledgments-we Thank Drs Hidde Ploegh and Christoph Petmentioning

confidence: 99%

Cathepsin B Degrades Amyloid-β in Mice Expressing Wild-type Human Amyloid Precursor Protein

Wang

Sun

Zhou

et al. 2012

Journal of Biological Chemistry

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“…Note that the positive modulation of CatB by E64d was less pronounced than the enhancing effect produced by PADK (increase of 76% vs. 549%; p<0.001). Other weak cysteine protease inhibitors were also found to up-regulate active CatB to varying degrees, including i ) SD1002, a non-peptidyl PADK analogue previously found to promote Aβ 42 clearance (Viswanathan et al, 2012), ii ) the polyphenol quercetin that, like PADK and E64d, exhibits very weak CatB inhibitory action (Ramalho et al, 2015), and iii ) Cathepsin Inhibitor 1 (CATI-1, also known as Z-Phe-Gly-NHO-Bz), a broad inhibitor of papain and several cathepsins (Table 2). The potent CatB inhibitors CA074, CA074me, and E64 did not exhibit positive modulation of CatB-30.…”

Section: Resultsmentioning

confidence: 99%

“…Accordingly, a growing number of studies has investigated agents that enhance enzymes appropriately involved in protein clearance. The CatB cysteine protease is one such enzyme: it is a lysosomal hydrolase that degrades Aβ into less amyloidogenic species (Mueller-Steiner et al, 2006; Butler et al, 2011; Wang et al, 2012; Cermak et al, 2016; Park et al, 2016) and it is neuroprotective when up-regulated, reducing synaptic and behavioral deficits related to AD (Mueller-Steiner et al, 2006; Sun et al, 2008; Butler et al, 2011; Yang et al, 2011; Viswanathan et al, 2012). The PADK and E64d compounds compared here are both very weak inhibitors of the Aβ-degrading CatB, but both were found to up-regulate CatB levels which may explain their beneficial actions in AD mouse models (see Butler et al, 2011; Hook et al, 2011; Bahr et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

“…3. Other IC 50 values for inhibiting CatB and calpain were obtained from the following references: a Butler et al, 2011; b Jeon et al, 2016; c Huang et al, 1992; d Viswanathan et al, 2012; e Ramalho et al, 2015; f Je Ma et al, 2009; g Weiss et al, 2009 and Coers et al, 2004 J Biol Chem 279:36397-404 h Montagne et al, 2017; i Inubushi et al, 1994; j Trinchese et al, 2008. CATI-1, Cathepsin Inhibitor 1; n.d., not determined.…”

Section: Figurementioning

confidence: 99%

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Potential Alzheimer’s Disease Therapeutics Among Weak Cysteine Protease Inhibitors Exhibit Mechanistic Differences Regarding Extent of Cathepsin B Up-Regulation and Ability to Block Calpain

Romine

Rentschler

Smith

et al. 2017

ESJ

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Cysteine protease inhibitors have long been part of drug discovery programs for Alzheimer’s disease (AD), traumatic brain injury (TBI), and other disorders. Select inhibitors reduce accumulating proteins and AD pathology in mouse models. One such compound, Z-Phe-Aladiazomethylketone (PADK), exhibits a very weak IC50 (9–11 μM) towards cathepsin B (CatB), but curiously PADK causes marked up-regulation of the Aβ-degrading CatB and improves spatial memory. Potential therapeutic and weak inhibitor E64d (14 μM IC50) also up-regulates CatB. PADK and E64d were compared regarding the blockage of calcium-induced cytoskeletal deterioration in brain samples, monitoring the 150-kDa spectrin breakdown product (SBDP) known to be produced by calpain. PADK had little to no effect on SBDP production at 10–100 μM. In contrast, E64d caused a dose-dependent decline in SBDP levels with an IC50 of 3–6 μM, closely matching its reported potency for inhibiting μ-calpain. Calpain also cleaves the cytoskeletal organizing protein gephyrin, producing 49-kDa (GnBDP49) and 18-kDa (GnBDP18) breakdown products. PADK had no apparent effect on calcium-induced gephyrin fragments whereas E64d blocked their production. E64d also protected the parent gephyrin in correspondence with reduced BDP levels. The findings of this study indicate that PADK’s positive and selective effects on CatB are consistent with human studies showing exercise elevates CatB and such elevation correlates with improved memory. On the other hand, E64d exhibits both marginal CatB enhancement and potent calpain inhibition. This dual effect may be beneficial for treating AD. Alternatively, the potent action on calpain-related pathology may explain E64d’s protection in AD and TBI models.

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“…Currently, enhancing the autophagy-lysosomal pathway of protein clearance is becoming widely accepted as a plausible treatment avenue for many indications, including CNS, metabolic, inflammatory, infectious, and muscle disorders [5][6][7][8][9][10]. Regarding the treatment of multi-proteinopathy, small-molecule cathepsin B modulators not only reduce intracellular Aβ, and consequently extracellular Aβ levels, they also reduce pathogenic forms of tau, and for both Aβ and tau, their enhanced clearance was associated with recovery of synaptic proteins [11,12]. In addition, an 18-residue peptide that promotesthe lysosomal degradation pathway of autophagy was found to enhance clearance of polyglutamine aggregates related to Huntington's disease [13].…”

Section: Introductionmentioning

confidence: 99%

A One-Drug Strategy is Needed to Attenuate the Multi-Proteinopathy that Leads to Age-Related Diseases

Bahr

2015

J Gerontol Geriatr Res

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Nonpeptidic Lysosomal Modulators Derived from Z-Phe-Ala-Diazomethylketone for Treating Protein Accumulation Diseases

Cited by 15 publications

References 23 publications

Cathepsin B Degrades Amyloid-β in Mice Expressing Wild-type Human Amyloid Precursor Protein

Cathepsin B Degrades Amyloid-β in Mice Expressing Wild-type Human Amyloid Precursor Protein

Potential Alzheimer’s Disease Therapeutics Among Weak Cysteine Protease Inhibitors Exhibit Mechanistic Differences Regarding Extent of Cathepsin B Up-Regulation and Ability to Block Calpain

A One-Drug Strategy is Needed to Attenuate the Multi-Proteinopathy that Leads to Age-Related Diseases

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