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AdDLP

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AdDLP is an antimicrobial peptide produced by Anaeromyxobacter dehalogenans. It is a bacterial defensin-like peptide and exhibits anti-plasmodium activity.

Category
Functional Peptides
Catalog number
BAT-013209
Molecular Formula
C226H367N69O74S6
Molecular Weight
5427.19
Synonyms
Anaeromyxobacter dehalogenans defensin-like peptide; A. dehalogenans defensin-like peptide; Val-Asn-Pro-Ser-Tyr-Arg-Leu-Asp-Pro-Glu-Ser-Arg-Pro-Gln-Cys-Glu-Ala-His-Cys-Gly-Gln-Leu-Gly-Met-Arg-Leu-Gly-Ala-Ile-Val-Ile-Met-Gly-Thr-Ala-Thr-Gly-Cys-Val-Cys-Glu-Pro-Lys-Glu-Ala-Ala-Thr-Pro-Glu-Ser-Arg (Disulfide bridge: Cys15-Cys38, Cys19-Cys40)
Purity
>98%
Sequence
VNPSYRLDPESRPQCEAHCGQLGMRLGAIVIMGTATGCVCEPKEAATPESR (Disulfide bridge: Cys15-Cys38, Cys19-Cys40)
1. Discovery of ADDL--targeting small molecule drugs for Alzheimer's disease
Gary C Look, et al. Curr Alzheimer Res. 2007 Dec;4(5):562-7. doi: 10.2174/156720507783018271.
Amyloid beta-derived diffusible ligands (ADDLs) comprise the neurotoxic subset of soluble Abeta(1-42) oligomers, now widely considered to be the molecular cause of memory malfunction and neurodegeneration in Alzheimer's disease (AD). We have developed a screening cascade which identifies small molecule modulators of ADDL-mediated neurotoxicity. The primary screen involves a fluorescence resonance energy transfer (FRET)-based assay which selects inhibitors of Abeta1-42 oligomer assembly. The identified hits were further characterized by assessing their ability to inhibit the assembly and binding of ADDLs to cultures of primary hippocampal neurons. This approach has led to the identification of a number of small molecules which inhibit ADDL assembly and their subsequent binding to neurons. Here we describe our small molecule discovery efforts to identify ADDL assembly blocker and ADDL binding inhibitors, and to transform validated hits into pre-clinical lead compounds.
2. Anti-ADDL antibodies differentially block oligomer binding to hippocampal neurons
P J Shughrue, P J Acton, R S Breese, W-Q Zhao, E Chen-Dodson, R W Hepler, A L Wolfe, M Matthews, G J Heidecker, J G Joyce, S A Villarreal, G G Kinney Neurobiol Aging. 2010 Feb;31(2):189-202. doi: 10.1016/j.neurobiolaging.2008.04.003.
Abeta-derived diffusible ligands (ADDLs) are abundant in AD brain, bind to hippocampal neurons and induce deficits in rodent cognition. To further investigate ADDL binding to neurons and identify antibodies that block this association, a panel of anti-Abeta and anti-ADDL antibodies was characterized for their ability to immuno-detect neuronally bound ADDLs and attenuate the binding of ADDLs to neurons. The results showed that anti-Abeta and anti-ADDL antibodies were able to abate ADDLs binding to hippocampal neurons, but to different degrees. Quantitative assessment of binding showed that one antibody, ACU-954 was markedly more effective at blocking ADDL binding than other antibodies assessed. ACU-954 was also found to block ADDL binding to hippocampal slice cultures, attenuate the ADDL-induced loss of dendritic spines and detect "natural ADDLs" in human AD tissue. These results demonstrated that antibodies that bind to and block ADDL binding to neurons can be identified, although their efficacy is conformationally specific since it is not readily apparent or predictable based on the core linear epitope or affinity for monomeric Abeta.
3. Mitochondrial defects and oxidative stress in Alzheimer disease and Parkinson disease
Michael H Yan, Xinglong Wang, Xiongwei Zhu Free Radic Biol Med. 2013 Sep;62:90-101. doi: 10.1016/j.freeradbiomed.2012.11.014. Epub 2012 Nov 29.
Alzheimer disease (AD) and Parkinson disease (PD) are the two most common age-related neurodegenerative diseases characterized by prominent neurodegeneration in selective neural systems. Although a small fraction of AD and PD cases exhibit evidence of heritability, among which many genes have been identified, the majority are sporadic without known causes. Molecular mechanisms underlying neurodegeneration and pathogenesis of these diseases remain elusive. Convincing evidence demonstrates oxidative stress as a prominent feature in AD and PD and links oxidative stress to the development of neuronal death and neural dysfunction, which suggests a key pathogenic role for oxidative stress in both AD and PD. Notably, mitochondrial dysfunction is also a prominent feature in these diseases, which is likely to be of critical importance in the genesis and amplification of reactive oxygen species and the pathophysiology of these diseases. In this review, we focus on changes in mitochondrial DNA and mitochondrial dynamics, two aspects critical to the maintenance of mitochondrial homeostasis and function, in relationship with oxidative stress in the pathogenesis of AD and PD.
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