 TGF-β ligand cross-subfamily interactions in the response of Caenorhabditis elegans to a bacterial pathogenEmma Jo Ciccarelli, Zachary Wing, Moshe Bendelstein, Ramandeep Kaur Johal, Gurjot Singh, Ayelet Monas and Cathy Savage-Dunn PLOS Genetics, 2024, vol. 20, issue 6, 1-20 Abstract: The Transforming Growth Factor beta (TGF-β) family consists of numerous secreted peptide growth factors that play significant roles in cell function, tissue patterning, and organismal homeostasis, including wound repair and immunity. Typically studied as homodimers, these ligands have the potential to diversify their functions through ligand interactions that may enhance, repress, or generate novel functions. In the nematode Caenorhabditis elegans, there are only five TGF-β ligands, providing an opportunity to dissect ligand interactions in fewer combinations than in vertebrates. As in vertebrates, these ligands can be divided into bone morphogenetic protein (BMP) and TGF-β/Activin subfamilies that predominantly signal through discrete signaling pathways. The BMP subfamily ligand DBL-1 has been well studied for its role in the innate immune response in C. elegans. Here we show that all five TGF-β ligands play a role in survival on bacterial pathogens. We also demonstrate that multiple TGF-β ligand pairs act nonredundantly as part of this response. We show that the two BMP-like ligands–DBL-1 and TIG-2–function independently of each other in the immune response, while TIG-2/BMP and the TGF-β/Activin-like ligand TIG-3 function together. Structural modeling supports the potential for TIG-2 and TIG-3 to form heterodimers. Additionally, we identify TIG-2 and TIG-3 as members of a rare subset of TGF-β ligands lacking the conserved cysteine responsible for disulfide linking mature dimers. Finally, we show that canonical DBL-1/BMP receptor and Smad signal transducers function in the response to bacterial pathogens, while components of the DAF-7 TGF-β/Activin signaling pathway do not play a major role in survival. These results demonstrate a novel potential for BMP and TGF-β/Activin subfamily ligands to interact and may provide a mechanism for distinguishing the developmental and homeostatic functions of these ligands from an acute response such as the innate immune response to bacterial pathogens.Author summary: The first line of defense upon exposure to a pathogen consists of innate immunity, which includes barrier functions and cell-cell communication. These cell-cell communication signaling pathways are highly conserved across species, enabling the use of simpler genetically tractable model organisms for their study. One such signaling pathway is the Transforming Growth Factor beta (TGF-β) pathway, which is conserved from invertebrates to vertebrates. TGF-β signaling ligands can be broadly divided into two major groups: the TGF-β/Activin group and the bone morphogenetic protein (BMP) group. There is compelling evidence that heterodimers have biological activities that differ from homodimers, but to this time, heterodimers have only been observed within subfamilies and not across subfamilies. In humans, there are 33 TGF-β ligands. In comparison, there are only five ligands in the nematode C. elegans, providing an opportunity to dissect ligand interactions in fewer combinations than in vertebrates. In this work, we show that all five ligands contribute to survival on bacterial pathogens to different extents and with specificity concerning the pathogen. Strikingly, genetic evidence and structural modeling support the existence of cross-subfamily interaction between BMP and TGF-β/Activin ligands. Date: 2024 Downloads: (external link) Related works: Export reference: BibTeX RIS (EndNote, ProCite, RefMan) HTML/Text Persistent link: https://EconPapers.repec.org/RePEc:plo:pgen00:1011324 DOI: 10.1371/journal.pgen.1011324 Access Statistics for this article More articles in PLOS Genetics from Public Library of Science |
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