Structural basis of internal peptide recognition by PDZ domains using molecular dynamics simulations

Sain, Neetu; Mohanty, Debasisa

doi:10.1101/575233

Cited by 1 publication

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“…PDZ domains are often associated with receptors (e.g., NMDA and AMPA/kainite) as well as membrane channels (e.g., Shaker K1 and TRP Ca21) and are involved in clustering proteins into functional complexes at the plasma membrane (Kong & Karplus, 2009), in addition to sorting, assembling, and anchoring multidomain interaction complexes (van den Berk et al, 2004). Disruption of PDZ mediated interactions is therefore implicated in the onset of a variety of human diseases including neurological disorders and cancer (Sain & Mohanty, 2019). Usually, the PDZ-containing protein has several PDZ domains (up to 10 domains), which can concurrently interact with different protein, and thereby form functional protein complexes (Kong & Karplus, 2009).…”

Section: The Pdz Protein Domainmentioning

confidence: 99%

Interconnected Protein Networks: Insights Towards CRIB-Par6 Protein Allostery Through a Graph-Theoretic Analysis

Cowan¹

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Towards this aim, I apply and build upon two recently developed network analysis methodologies, MD-Sectors (Fabry, 2020;Lakhani, Thayer, Black, & Beveridge, 2020) and MD-END (Abramson, 2021), for analyzing pairwise residue networks generated from differential forms of biophysical interactions to the same allosteric model system, CRIB-Par6. In a synthesized analysis of both methodologies, I investigate the clustering, cohesiveness, and density of residue communities within these networks resulting from the decomposition of residues' pairwise covariances in motional (MD-Sectors) and non-bonded interaction energic (MD-END) interactions. I additionally develop a pairwise embedding error analysis that works upon the MD-END methodology to analyze the degree of energetic modulation of specific residues between networks that lead to their differential graph embeddings across different protein interactions. Through this combined approach, we hope to find complementary insight into how protein systems such as CRIB-Par6 may use different and potentially overlapping allosteric pathways to confer global and local changes to structure and function incident to protein-specific interactions. In the utility and development of these methodologies we demonstrate that with the significance of conformational dynamics to binding interactions, the role of electrostatically-mediated energetic signalling is equally important towards a comprehensive view of allosteric signalling.

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Section: The Pdz Protein Domainmentioning

confidence: 99%

Interconnected Protein Networks: Insights Towards CRIB-Par6 Protein Allostery Through a Graph-Theoretic Analysis

Cowan¹

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show abstract

Structural basis of internal peptide recognition by PDZ domains using molecular dynamics simulations

Cited by 1 publication

References 41 publications

Interconnected Protein Networks: Insights Towards CRIB-Par6 Protein Allostery Through a Graph-Theoretic Analysis

Interconnected Protein Networks: Insights Towards CRIB-Par6 Protein Allostery Through a Graph-Theoretic Analysis

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