An explicitly designed paratope of amyloid-β prevents neuronal apoptosis <i>in vitro</i> and hippocampal damage in rat brain

Paul, Ashim; Kumar, Sourav; Kalita, Sujan; Kalita, Sourav; Sarkar, Debasree; Bhunia, Anirban; Bandyopadhyay, Anupam; Mondal, Amal Chandra; Mandal, Bhubaneswar

doi:10.1039/d0sc04379f

Cited by 10 publications

(8 citation statements)

References 73 publications

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“…The protective behavior of N -Me-F , N -Me-L and N -Me-F/L counteracting cytotoxicity is expressed in the assay measuring caspase-3 activity, where they significantly decrease caspase-3 activation compared to the WT and partly to the control. This is in alignment with other N -methylated peptides in the literature 70 .…”

Section: Discussionsupporting

confidence: 89%

Peptide backbone modifications of amyloid β (1–40) impact fibrillation behavior and neuronal toxicity

Schwarze

Korn

Höfling

et al. 2021

Sci Rep

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Fibril formation of amyloid β (Aβ) peptides is one of the key molecular events connected to Alzheimer’s disease. The pathway of formation and mechanism of action of Aβ aggregates in biological systems is still object of very active research. To this end, systematic modifications of the Phe19–Leu34 hydrophobic contact, which has been reported in almost all structural studies of Aβ40 fibrils, helps understanding Aβ folding pathways and the underlying free energy landscape of the amyloid formation process. In our approach, a series of Aβ40 peptide variants with two types of backbone modifications, namely incorporation of (i) a methylene or an ethylene spacer group and (ii) a N-methylation at the amide functional group, of the amino acids at positions 19 or 34 was applied. These mutations are expected to challenge the inter-β-strand side chain contacts as well as intermolecular backbone β-sheet hydrogen bridges. Using a multitude of biophysical methods, it is shown that these backbone modifications lead, in most of the cases, to alterations in the fibril formation kinetics, a higher local structural heterogeneity, and a somewhat modified fibril morphology without generally impairing the fibril formation capacity of the peptides. The toxicological profile found for the variants depend on the type and extent of the modification.

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Section: Discussionsupporting

confidence: 89%

Peptide backbone modifications of amyloid β (1–40) impact fibrillation behavior and neuronal toxicity

Schwarze

Korn

Höfling

et al. 2021

Sci Rep

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“…Recent studies have elucidated the dock-lock mechanism of fibril formation, where unstructured Aβ monomers transiently associate with the fibril surface before undergoing a slower conformational rearrangement and incorporating into the primary fibril lattice. − This process, involving the central K16-A21 and C-terminal M35-V40 regions, plays a critical role in fibrillation and presents a potential avenue for inhibiting amyloidosis. Remarkably, our recent investigation employing a synthetic paratope, SP1, has demonstrated selective binding to the LVFFA epitope, a crucial amyloidogenic region of Aβ peptide . Furthermore, SP1 effectively disaggregated preformed fibrils of Aβ40, leading to the formation of nontoxic species.…”

Section: Gxxxg Motif Targeted Inhibitorsmentioning

confidence: 97%

“…Remarkably, our recent investigation employing a synthetic paratope, SP1, has demonstrated selective binding to the LVFFA epitope, a crucial amyloidogenic region of Aβ peptide. 123 Furthermore, SP1 effectively disaggregated preformed fibrils of Aβ40, leading to the formation of nontoxic species. Solution NMR analysis revealed that SP1 disrupts the essential dock-lock interactions of monomeric Aβ, suggesting molecular interference in the critical domain.…”

Section: ■ Gxxxg Motif Targeted Inhibitorsmentioning

confidence: 99%

“…So far, most of the design strategies include short peptide sequence analogous to part of the native sequence of the protein or peptide responsible for fibril formation. − This approach is based on the fact that the short peptide fragments would self-recognize and thereby should bind to the homologous sequence in the native protein. The most popular approach for the inhibition of Aβ amyloidogenesis have been the design of peptides derived from the central hydrophobic cluster (L17-A21) of Aβ. − Since, amyloid fibrils usually adopt a cross β-structure, structure-based agents such as β-sheet breakers have also been formulated to inhibit fibril formation. − These inhibitory peptides are targeted to disrupt β-sheets by blocking the hydrogen bond formation between β-strands. In addition to peptide mimics, alterations in short peptides such as N -methylation and peptide cyclization have shown enhanced conformational stability with significantly increased inhibitory effect on amyloid aggregation. , …”

Section: Gxxxg Motif Targeted Inhibitorsmentioning

confidence: 99%

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Delineating the Role of GxxxG Motif in Amyloidogenesis: A New Perspective in Targeting Amyloid-Beta Mediated AD Pathogenesis

Sarkar,

Bhunia

2023

ACS Bio Med Chem Au

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The pursuit of a novel structural motif that can shed light on the key functional attributes is a primary focus in the study of protein folding disorders. Decades of research on Alzheimer's disease (AD) have centered on the Amyloid β (Aβ) pathway, highlighting its significance in understanding the disorder. The diversity in the Aβ pathway and the possible silent tracks which are yet to discover, makes it exceedingly intimidating to the interdisciplinary scientific community. Over the course of AD research, Aβ has consistently been at the forefront of scientific inquiry and discussion. In this review, we epitomize the role of a potential structural motif (GxxxG motif) that may provide a new horizon to the Aβ conflict. We emphasize on how comprehensive understanding of this motif from a structure−function perspective may pave the way for designing novel therapeutics intervention in AD and related diseases.

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“…Many materials have been employed to detoxify sulfur mustard and its analogous derivatives; in this context, owing to its attenable functionality, superior chemical and thermal stability, and enhanced porosity, POPs emerge as a judicious choice. 97 POPs are a class of advanced functional materials with structural tailorability, inherent porosity, and high flexibility, which have served for several applications like CO 2 capture, 98,99 CO 2 reduction to solar fuels, 100,101 biomass valorisation, 102,103 organic transformation reactions, 104,105 CO 2 fixation, 99 gas and liquid separation, 106 water purification, 107,108 energy storage, 109 chemo-and biosensing 110 and HD decontamination [111][112][113][114][115] etc. (Fig.…”

Section: •−mentioning

confidence: 99%

A critical review on emerging photoactive porous materials for sulfide oxidation and sulfur mustard decontamination

et al. 2023

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An explicitly designed paratope of amyloid-β prevents neuronal apoptosis in vitro and hippocampal damage in rat brain

Abstract: Herein, the therapeutic potentials of an explicitly designed peptide probe are systematically illuminated in vitro and in vivo against Aβ aggregation. The probe demonstrates remarkable potency for attenuating neurotoxicity and hippocampal damage.

Cited by 10 publications

References 73 publications

Peptide backbone modifications of amyloid β (1–40) impact fibrillation behavior and neuronal toxicity

Peptide backbone modifications of amyloid β (1–40) impact fibrillation behavior and neuronal toxicity

Delineating the Role of GxxxG Motif in Amyloidogenesis: A New Perspective in Targeting Amyloid-Beta Mediated AD Pathogenesis

A critical review on emerging photoactive porous materials for sulfide oxidation and sulfur mustard decontamination

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