The Primate-specific Peptide Y-P30 Regulates Morphological Maturation of Neocortical Dendritic Spines

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2019 Feb 14

PMID 30759095

Citations 3

Authors

Janine R Neumann

Suvarna Dash-Wagh

Alexander Jack

Andrea Rak

Kay Jungling

Mohammad I K Hamad

Hans-Christian Pape

Michael R Kreutz

Martin Puskarjov

Petra Wahle

Affiliations

Soon will be listed here.

Abstract

The 30-amino acid peptide Y-P30 corresponds to the N-terminus of the primate-specific, sweat gland-derived dermcidin prepropeptide. Previous work has revealed that Y-P30 enhances the interaction of pleiotrophin and syndecans-2/3, and thus represents a natural ligand to study this signaling pathway. In immature neurons, Y-P30 activates the c-Src and p42/44 ERK kinase pathway, increases the amount of F-actin in axonal growth cones, and promotes neuronal survival, cell migration and axonal elongation. The action of Y-P30 on axonal growth requires syndecan-3 and heparan sulfate side chains. Whether Y-P30 has the potential to influence dendrites and dendritic protrusions has not been explored. The latter is suggested by the observations that syndecan-2 expression increases during postnatal development, that syndecan-2 becomes enriched in dendritic spines, and that overexpression of syndecan-2 in immature neurons results in a premature morphological maturation of dendritic spines. Here, analysing rat cortical pyramidal and non-pyramidal neurons in organotypic cultures, we show that Y-P30 does not alter the development of the dendritic arborization patterns. However, Y-P30 treatment decreases the density of apical, but not basal dendritic protrusions at the expense of the filopodia. Analysis of spine morphology revealed an unchanged mushroom/stubby-to-thin spine ratio and a shortening of the longest decile of dendritic protrusions. Whole-cell recordings from cortical principal neurons in dissociated cultures grown in the presence of Y-P30 demonstrated a decrease in the frequency of glutamatergic mEPSCs. Despite these differences in protrusion morphology and synaptic transmission, the latter likely attributable to presynaptic effects, calcium event rate and amplitude recorded in pyramidal neurons in organotypic cultures were not altered by Y-P30 treatment. Together, our data suggest that Y-P30 has the capacity to decelerate spinogenesis and to promote morphological, but not synaptic, maturation of dendritic protrusions.

Citing Articles

GluN2B but Not GluN2A for Basal Dendritic Growth of Cortical Pyramidal Neurons.

Gonda S, Giesen J, Sieberath A, West F, Buchholz R, Klatt O Front Neuroanat. 2020; 14:571351.

PMID: 33281565 PMC: 7691608. DOI: 10.3389/fnana.2020.571351.

Pleiotrophin: Activity and mechanism.

Wang X Adv Clin Chem. 2020; 98:51-89.

PMID: 32564788 PMC: 7672882. DOI: 10.1016/bs.acc.2020.02.003.

Distinct regulation of bioenergetics and translation by group I mGluR and NMDAR.

Ghosh Dastidar S, Das Sharma S, Chakraborty S, Chattarji S, Bhattacharya A, Muddashetty R EMBO Rep. 2020; 21(6):e48037.

PMID: 32351028 PMC: 7271334. DOI: 10.15252/embr.201948037.

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