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IFITM3 functions as a PIP3 scaffold to amplify PI3K signalling in B cells
- Lee, Jaewoong;
- Robinson, Mark E;
- Ma, Ning;
- Artadji, Dewan;
- Ahmed, Mohamed A;
- Xiao, Gang;
- Sadras, Teresa;
- Deb, Gauri;
- Winchester, Janet;
- Cosgun, Kadriye Nehir;
- Geng, Huimin;
- Chan, Lai N;
- Kume, Kohei;
- Miettinen, Teemu P;
- Zhang, Ye;
- Nix, Matthew A;
- Klemm, Lars;
- Chen, Chun Wei;
- Chen, Jianjun;
- Khairnar, Vishal;
- Wiita, Arun P;
- Thomas-Tikhonenko, Andrei;
- Farzan, Michael;
- Jung, Jae U;
- Weinstock, David M;
- Manalis, Scott R;
- Diamond, Michael S;
- Vaidehi, Nagarajan;
- Müschen, Markus
- et al.
Published Web Location
https://doi.org/10.1038/s41586-020-2884-6Abstract
Interferon-induced transmembrane protein 3 (IFITM3) has previously been identified as an endosomal protein that blocks viral infection1-3. Here we studied clinical cohorts of patients with B cell leukaemia and lymphoma, and identified IFITM3 as a strong predictor of poor outcome. In normal resting B cells, IFITM3 was minimally expressed and mainly localized in endosomes. However, engagement of the B cell receptor (BCR) induced both expression of IFITM3 and phosphorylation of this protein at Tyr20, which resulted in the accumulation of IFITM3 at the cell surface. In B cell leukaemia, oncogenic kinases phosphorylate IFITM3 at Tyr20, which causes constitutive localization of this protein at the plasma membrane. In a mouse model, Ifitm3-/- naive B cells developed in normal numbers; however, the formation of germinal centres and the production of antigen-specific antibodies were compromised. Oncogenes that induce the development of leukaemia and lymphoma did not transform Ifitm3-/- B cells. Conversely, the phosphomimetic IFITM3(Y20E) mutant induced oncogenic PI3K signalling and initiated the transformation of premalignant B cells. Mechanistic experiments revealed that IFITM3 functions as a PIP3 scaffold and central amplifier of PI3K signalling. The amplification of PI3K signals depends on IFITM3 using two lysine residues (Lys83 and Lys104) in its conserved intracellular loop as a scaffold for the accumulation of PIP3. In Ifitm3-/- B cells, lipid rafts were depleted of PIP3, which resulted in the defective expression of over 60 lipid-raft-associated surface receptors, and impaired BCR signalling and cellular adhesion. We conclude that the phosphorylation of IFITM3 that occurs after B cells encounter antigen induces a dynamic switch from antiviral effector functions in endosomes to a PI3K amplification loop at the cell surface. IFITM3-dependent amplification of PI3K signalling, which in part acts downstream of the BCR, is critical for the rapid expansion of B cells with high affinity to antigen. In addition, multiple oncogenes depend on IFITM3 to assemble PIP3-dependent signalling complexes and amplify PI3K signalling for malignant transformation.
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