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Retinoic acid breakdown is required for proximodistal positional identity during amphibian limb regeneration.

ABSTRACT: Regenerating limbs retain their proximodistal (PD) positional identity following amputation. This positional identity is genetically encoded by PD patterning genes that instruct blastema cells to regenerate the appropriate PD limb segment. Retinoic acid (RA) is known to specify proximal limb identity, but how RA signaling levels are established in the blastema is unknown. Here, we show that RA breakdown via CYP26B1 is essential for determining RA signaling levels within blastemas. CYP26B1 inhibition molecularly reprograms distal blastemas into a more proximal identity, phenocopying the effects of administering excess RA. We identify Shox as an RA-responsive gene that is differentially expressed between proximally and distally amputated limbs. Ablation of Shox results in shortened limbs with proximal skeletal elements that fail to initiate endochondral ossification. These results suggest that PD positional identity is determined by RA degradation and RA-responsive genes that regulate PD skeletal element formation during limb regeneration.

SUBMITTER: Duerr TJ 

PROVIDER: S-EPMC11326211 | biostudies-literature | 2024 Aug

REPOSITORIES: biostudies-literature

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Retinoic acid breakdown is required for proximodistal positional identity during amphibian limb regeneration.

Duerr Timothy J TJ   Miller Melissa M   Kumar Sage S   Bakr Dareen D   Griffiths Jackson R JR   Gautham Aditya K AK   Douglas Danielle D   Voss S Randal SR   Monaghan James R JR  

bioRxiv : the preprint server for biology 20240809

Regenerating limbs retain their proximodistal (PD) positional identity following amputation. This positional identity is genetically encoded by PD patterning genes that instruct blastema cells to regenerate the appropriate PD limb segment. Retinoic acid (RA) is known to specify proximal limb identity, but how RA signaling levels are established in the blastema is unknown. Here, we show that RA breakdown via CYP26B1 is essential for determining RA signaling levels within blastemas. CYP26B1 inhibi  ...[more]

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