Investigating alternative signaling pathways regulated by Kindlin-3
A three-membered, FERM-domain containing, focal adhesion protein family known as Kindlin mediates cellular adhesion and migration by promoting Integrin activation. This protein family comprises Kindlin-1, Kindlin-2 and Kindlin-3. Both Kindlin-1 and Kindlin-2 mediate the activation of various sign...
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| Format: | Thesis-Doctor of Philosophy |
| Language: | English |
| Published: |
Nanyang Technological University
2025
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| Online Access: | https://hdl.handle.net/10356/182569 |
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| Institution: | Nanyang Technological University |
| Language: | English |
| Summary: | A three-membered, FERM-domain containing, focal adhesion protein family known as
Kindlin mediates cellular adhesion and migration by promoting Integrin activation. This
protein family comprises Kindlin-1, Kindlin-2 and Kindlin-3. Both Kindlin-1 and Kindlin-2
mediate the activation of various signaling pathways, whether Kindlin-3 plays a similar role
remains to be studied. In this thesis, we examine the role Kindlin-3 plays in regulating
alternative signaling pathways. Using PTEN-deficient T-ALL cells, we show that Kindlin-3
facilitates MAPK/ERK activation to promote cell proliferation by mediating DDR.
Mechanistically, the Kindlin-3-RACK1-MEK1/2 ternary complex is transported to the PIP3-
rich plasma membrane via Kindlin-3 binding to PIP3. Following PIP3 binding, RACK1-
MEK1/2 dissociates from Kindlin-3, leading to RACK1 scaffolding MEK1/2 and b-RAF.
This brings the MAPK/ERK components in proximity to promote MAPK/ERK activation.
Ablation of Kindlin-3 expression leads to diminished ERK1/2 activation, elevated levels of
DNA damage and delayed mitotic completion. Interestingly, the Kindlin-3 splice isoform,
Kindlin-3L is unable to facilitate MAPK/ERK activation due to its poor PIP3-binding ability.
During TCR activation, PIP3 production and Integrin LFA-1 activation promotes Kindlin-3
plasma membrane recruitment, contributing to MAPK/ERK activation. We also provide
preliminary evidence that Kindlin-3 interacts with the cytokine receptor, IL2Rβ to facilitate
its recruitment to the T-T homotypic synapse. Ablation of Kindlin-3 expression leads to
diminished IL2Rβ levels at the T-T homotypic synapse. We identified the binding interface
to be formed by the Kindlin-3 F0 subdomain and the C-terminal 21 amino acid stretch found
within the IL2Rβ STAT binding region. |
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