AI Article Synopsis
- Tensins2 (TNS2) is a protein involved in maintaining podocytes, crucial for kidney function, with specific domains influencing its role.
- Genetic mutations in TNS2, specifically the deletion of the SH2-PTB domain, led to significant kidney damage and protein loss in mice, while other mutations did not show these effects.
- The study indicates that the SH2-PTB domain of TNS2 is essential for its localization at focal adhesions and the overall maintenance of podocytes postnatally.
Article Abstract
Tensin2 (TNS2) is a focal adhesion-localized protein possessing N-terminal tandem protein tyrosine phosphatase (PTPase) and C2 domains, and C-terminal tandem Src homology 2 (SH2) and phosphotyrosine binding (PTB) domains. Genetic deletion of Tns2 in a susceptible murine strain leads to podocyte alterations after birth. To clarify the domain contributions to podocyte maintenance, we generated two Tns2-mutant mice with the genetic background of the susceptible FVB/NJ strain, Tns2 and Tns2 mice, carrying a SH2-PTB domain deletion and a PTPase domain inactivation, respectively. The Tns2 mice developed massive albuminuria, severe glomerular injury and podocyte alterations similarly to those in Tns2-deficient mice. In contrast, the Tns2 mice showed no obvious phenotypic abnormalities. These results indicate that the TNS2 SH2-PTB domain, but not its PTPase activity, plays a role in podocyte maintenance. Furthermore, in a podocyte cell line, the truncated TNS2 mutant lacking the SH2-PTB domain lost the ability to localize to focal adhesion. Taken together, these data suggest that TNS2 recruitment to focal adhesion is required to maintain postnatal podocytes on a susceptible genetic background.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7220710 | PMC |
| http://dx.doi.org/10.1538/expanim.19-0101 | DOI Listing |
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Article Synopsis
- Tensins2 (TNS2) is a protein involved in maintaining podocytes, crucial for kidney function, with specific domains influencing its role.
- Genetic mutations in TNS2, specifically the deletion of the SH2-PTB domain, led to significant kidney damage and protein loss in mice, while other mutations did not show these effects.
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