AUTHOR=Mitsogiannis Manuela D. , Pancho Anna , Aerts Tania , Sachse Sonja M. , Vanlaer Ria , Noterdaeme Lut , Schmucker Dietmar , Seuntjens Eve 

TITLE=Subtle Roles of Down Syndrome Cell Adhesion Molecules in Embryonic Forebrain Development and Neuronal Migration

JOURNAL=Frontiers in Cell and Developmental Biology

VOLUME=8

YEAR=2021

URL=https://www.frontiersin.org/journals/cell-and-developmental-biology/articles/10.3389/fcell.2020.624181

DOI=10.3389/fcell.2020.624181

ISSN=2296-634X

ABSTRACT=<p>Down Syndrome (DS) Cell Adhesion Molecules (DSCAMs) are transmembrane proteins of the immunoglobulin superfamily. Human DSCAM is located within the DS critical region of chromosome 21 (duplicated in Down Syndrome patients), and mutations or copy-number variations of this gene have also been associated to Fragile X syndrome, intellectual disability, autism, and bipolar disorder. The DSCAM paralogue DSCAM-like 1 (DSCAML1) maps to chromosome 11q23, implicated in the development of Jacobsen and Tourette syndromes. Additionally, a spontaneous mouse DSCAM deletion leads to motor coordination defects and seizures. Previous research has revealed roles for DSCAMs in several neurodevelopmental processes, including synaptogenesis, dendritic self-avoidance, cell sorting, axon growth and branching. However, their functions in embryonic mammalian forebrain development have yet to be completely elucidated. In this study, we revealed highly dynamic spatiotemporal patterns of <italic>Dscam</italic> and <italic>Dscaml1</italic> expression in definite cortical layers of the embryonic mouse brain, as well as in structures and ganglionic eminence-derived neural populations within the embryonic subpallium. However, an in-depth histological analysis of cortical development, ventral forebrain morphogenesis, cortical interneuron migration, and cortical-subcortical connectivity formation processes in Dscam and Dscaml1 knockout mice (<italic>Dscam</italic><sup><italic>del</italic>17</sup> and <italic>Dscaml1</italic><sup><italic>GT</italic></sup>) at several embryonic stages indicated that constitutive loss of <italic>Dscam</italic> and <italic>Dscaml1</italic> does not affect these developmental events in a significant manner. Given that several <italic>Dscam</italic>- and <italic>Dscaml1</italic>-linked neurodevelopmental disorders are associated to chromosomal region duplication events, we furthermore sought to examine the neurodevelopmental effects of <italic>Dscam</italic> and <italic>Dscaml1</italic> gain of function (GOF). <italic>In vitro, ex vivo</italic>, and <italic>in vivo</italic> GOF negatively impacted neural migration processes important to cortical development, and affected the morphology of maturing neurons. Overall, these findings contribute to existing knowledge on the molecular etiology of human neurodevelopmental disorders by elucidating how dosage variations of genes encoding adhesive cues can disrupt cell-cell or cell-environment interactions crucial for neuronal migration.</p>