The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy

TNFAIP8 and other mammalian TIPE family proteins have attracted increased interest due to their associations with disease-related processes including oncogenic transformation, metastasis, and inflammation. The molecular and cellular functions of TIPE family proteins are still not well understood. He...

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Autores principales: Chittaranjan, Suganthi, Xu, Jing, Kuzyk, Michael, Dullat, Harpreet K., Wilton, James, DeVorkin, Lindsay, Lebovitz, Chandra, Morin, Gregg B., Marra, Marco A., Gorski, Sharon M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4434819/
https://www.ncbi.nlm.nih.gov/pubmed/25836674
http://dx.doi.org/10.1242/bio.20148417
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author Chittaranjan, Suganthi
Xu, Jing
Kuzyk, Michael
Dullat, Harpreet K.
Wilton, James
DeVorkin, Lindsay
Lebovitz, Chandra
Morin, Gregg B.
Marra, Marco A.
Gorski, Sharon M.
author_facet Chittaranjan, Suganthi
Xu, Jing
Kuzyk, Michael
Dullat, Harpreet K.
Wilton, James
DeVorkin, Lindsay
Lebovitz, Chandra
Morin, Gregg B.
Marra, Marco A.
Gorski, Sharon M.
author_sort Chittaranjan, Suganthi
collection PubMed
description TNFAIP8 and other mammalian TIPE family proteins have attracted increased interest due to their associations with disease-related processes including oncogenic transformation, metastasis, and inflammation. The molecular and cellular functions of TIPE family proteins are still not well understood. Here we report the molecular and genetic characterization of the Drosophila TNFAIP8 homolog, CG4091/sigmar. Previous gene expression studies revealed dynamic expression of sigmar in larval salivary glands prior to histolysis. Here we demonstrate that in sigmar loss-of-function mutants, the salivary glands are morphologically abnormal with defects in the tubulin network and decreased autophagic flux. Sigmar localizes subcellularly to microtubule-containing projections in Drosophila S2 cells, and co-immunoprecipitates with the Ste20-like kinase Misshapen, a regulator of the JNK pathway. Further, the Drosophila TNF ligand Eiger can induce sigmar expression, and sigmar loss-of-function leads to altered localization of pDJNK in salivary glands. Together, these findings link Sigmar to the JNK pathway, cytoskeletal remodeling and autophagy activity during salivary gland development, and provide new insights into TIPE family member function.
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spelling pubmed-44348192015-06-11 The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy Chittaranjan, Suganthi Xu, Jing Kuzyk, Michael Dullat, Harpreet K. Wilton, James DeVorkin, Lindsay Lebovitz, Chandra Morin, Gregg B. Marra, Marco A. Gorski, Sharon M. Biol Open Research Article TNFAIP8 and other mammalian TIPE family proteins have attracted increased interest due to their associations with disease-related processes including oncogenic transformation, metastasis, and inflammation. The molecular and cellular functions of TIPE family proteins are still not well understood. Here we report the molecular and genetic characterization of the Drosophila TNFAIP8 homolog, CG4091/sigmar. Previous gene expression studies revealed dynamic expression of sigmar in larval salivary glands prior to histolysis. Here we demonstrate that in sigmar loss-of-function mutants, the salivary glands are morphologically abnormal with defects in the tubulin network and decreased autophagic flux. Sigmar localizes subcellularly to microtubule-containing projections in Drosophila S2 cells, and co-immunoprecipitates with the Ste20-like kinase Misshapen, a regulator of the JNK pathway. Further, the Drosophila TNF ligand Eiger can induce sigmar expression, and sigmar loss-of-function leads to altered localization of pDJNK in salivary glands. Together, these findings link Sigmar to the JNK pathway, cytoskeletal remodeling and autophagy activity during salivary gland development, and provide new insights into TIPE family member function. The Company of Biologists 2015-04-02 /pmc/articles/PMC4434819/ /pubmed/25836674 http://dx.doi.org/10.1242/bio.20148417 Text en © 2015. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0), which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Article
Chittaranjan, Suganthi
Xu, Jing
Kuzyk, Michael
Dullat, Harpreet K.
Wilton, James
DeVorkin, Lindsay
Lebovitz, Chandra
Morin, Gregg B.
Marra, Marco A.
Gorski, Sharon M.
The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title_full The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title_fullStr The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title_full_unstemmed The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title_short The Drosophila TIPE family member Sigmar interacts with the Ste20-like kinase Misshapen and modulates JNK signaling, cytoskeletal remodeling and autophagy
title_sort drosophila tipe family member sigmar interacts with the ste20-like kinase misshapen and modulates jnk signaling, cytoskeletal remodeling and autophagy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4434819/
https://www.ncbi.nlm.nih.gov/pubmed/25836674
http://dx.doi.org/10.1242/bio.20148417
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