AI Article Synopsis

  • The study utilizes RNA in situ hybridization (RISH) to investigate the long noncoding RNA (lncRNA) Klhl14as in the development of the intervertebral disc (IVD) in mouse embryos, particularly focusing on loss-of-function mutations in key transcription factors (TFs).
  • The objective is to validate Klhl14as within the developing IVD, as understanding its role can help clarify the complex processes behind IVD formation, which is significant for regenerative medicine.
  • Results indicate that Klhl14as expression is notably influenced by specific transcription factors, suggesting its important role in the gene regulatory network involved in axial skeleton development.

Article Abstract

Study Design: RNA in situ hybridization (RISH) allows for validation and characterization of the long noncoding (lnc) natural antisense RNA (NAT) Klhl14as in the embryonic murine intervertebral disc (IVD) in the context of loss-of-function mutants for key transcription factors (TFs) in axial skeleton development.

Objective: Validation of Klhl14as in the developing murine IVD.

Summary Of Background Data: The IVD is a focus of regenerative medicine; however, processes and signaling cascades resulting in the different cell types in a mature IVD still require clarification in most animals including humans. Technological advances increasingly point to implications of lnc NATs in transcription/translation regulation. Transcriptome data generation and analysis identified a protein encoding transcript and related noncoding antisense transcript as downregulated in embryos devoid of key TFs during axial skeleton development. Here, primarily, the antisense transcript is analyzed in this loss-of-function context.

Methods: 4930426D05Rik and 6330403N15Rik were identified as Klhl14as and sense, respectively, two transcripts downregulated in the vertebral column of midgestation Pax1 and Pax9 mutant mouse embryos. RISH on wildtype and mutant embryos for the TF encoding genes Pax1/Pax9, Sox5/Sox6/Sox9, and Bapx1 was used to further analyze Klhl14as in the developing IVD.

Results: Klhl14as and Klhl14 were the top downregulated transcripts in Pax1; Pax9 E12.5 embryos. Our data demonstrate expression of Klhl14as and sense transcripts in the annulus fibrosus (AF) and notochord of the developing IVD. Klhl14as expression in the inner annulus fibrosus (iAF) seems dependent on the TFs Pax1/Pax9, Sox6, Sox9, and Bapx1.

Conclusion: We are the first to suggest a role for the lncRNA Klhl14as in the developing IVD. Our data link Klhl14as to a previously established gene regulatory network during axial skeleton development and contribute further evidence that lnc NATs are involved in crucial gene regulatory networks in eukaryotic cells.

Level Of Evidence: N/A.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10426336PMC
http://dx.doi.org/10.1097/BRS.0000000000002827DOI Listing

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