Second signals rescue B cells from activation-induced mitochondrial dysfunction and death.
Munir AkkayaJavier TrabaAlexander S RoeslerPietro MiozzoBillur AkkayaBrandon P TheallHaewon SohnMirna PenaMargery SmelkinsonJuraj KabatEric DahlstromDavid W DorwardJeff SkinnerMichael N SackSusan K PiercePublished in: Nature immunology (2018)
B cells are activated by two temporally distinct signals, the first provided by the binding of antigen to the B cell antigen receptor (BCR), and the second provided by helper T cells. Here we found that B cells responded to antigen by rapidly increasing their metabolic activity, including both oxidative phosphorylation and glycolysis. In the absence of a second signal, B cells progressively lost mitochondrial function and glycolytic capacity, which led to apoptosis. Mitochondrial dysfunction was a result of the gradual accumulation of intracellular calcium through calcium response-activated calcium channels that, for approximately 9 h after the binding of B cell antigens, was preventable by either helper T cells or signaling via the receptor TLR9. Thus, BCR signaling seems to activate a metabolic program that imposes a limited time frame during which B cells either receive a second signal and survive or are eliminated.
Keyphrases
- dendritic cells
- acute lymphoblastic leukemia
- regulatory t cells
- binding protein
- tyrosine kinase
- oxidative stress
- chronic myeloid leukemia
- toll like receptor
- immune response
- diabetic rats
- quality improvement
- high glucose
- cell death
- emergency department
- cell proliferation
- adverse drug
- endothelial cells
- nuclear factor
- transcription factor
- light emitting