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Spinal V1 inhibitory interneuron clades differ in birthdate, projections to motoneurons, and heterogeneity.

Authors :
Worthy AE
Anderson JT
Lane AR
Gomez-Perez LJ
Wang AA
Griffith RW
Rivard AF
Bikoff JB
Alvarez FJ
Source :
ELife [Elife] 2024 Nov 28; Vol. 13. Date of Electronic Publication: 2024 Nov 28.
Publication Year :
2024

Abstract

Spinal cord interneurons play critical roles shaping motor output, but their precise identity and connectivity remain unclear. Focusing on the V1 interneuron cardinal class we defined four major V1 subsets in the mouse according to neurogenesis, genetic lineage-tracing, synaptic output to motoneurons, and synaptic inputs from muscle afferents. Sequential neurogenesis delineates different V1 subsets: two early born (Renshaw and Pou6f2) and two late born (Foxp2 and Sp8). Early born Renshaw cells and late born Foxp2-V1 interneurons are tightly coupled to motoneurons, while early born Pou6f2-V1 and late born Sp8-V1 interneurons are not, indicating that timing of neurogenesis does not correlate with motoneuron targeting. V1 clades also differ in cell numbers and diversity. Lineage labeling shows that the Foxp2-V1 clade contains over half of all V1 interneurons, provides the largest inhibitory input to motoneuron cell bodies, and includes subgroups that differ in birthdate, location, and proprioceptive input. Notably, one Foxp2-V1 subgroup, defined by postnatal Otp expression, is positioned near the LMC and receives substantial input from proprioceptors, consistent with an involvement in reciprocal inhibitory pathways. Combined tracing of ankle flexor sensory afferents and interneurons monosynaptically connected to ankle extensors confirmed placement of Foxp2-V1 interneurons in reciprocal inhibitory pathways. Our results validate previously proposed V1 clades as unique functional subtypes that differ in circuit placement, with Foxp2-V1 cells forming the most heterogeneous subgroup. We discuss how V1 organizational diversity enables understanding of their roles in motor control, with implications for their diverse ontogenetic and phylogenetic origins.<br />Competing Interests: AW, JA, AL, LG, AW, RG, AR, JB, FA No competing interests declared<br /> (© 2024, Worthy et al.)

Details

Language :
English
ISSN :
2050-084X
Volume :
13
Database :
MEDLINE
Journal :
ELife
Publication Type :
Academic Journal
Accession number :
39607843
Full Text :
https://doi.org/10.7554/eLife.95172