Calcium flux control by Pacs1-Wdr37 promotes lymphocyte quiescence and lymphoproliferative diseases.
Evan Nair-GillMassimo BonoraXue ZhongAijie LiuAmber MirandaNathan StewartSara LudwigJamie RussellThomas GallagherPaolo PintonBruce A BeutlerPublished in: The EMBO journal (2021)
Endoplasmic reticulum (ER) calcium (Ca2+ ) stores are critical to proteostasis, intracellular signaling, and cellular bioenergetics. Through forward genetic screening in mice, we identified two members of a new complex, Pacs1 and Wdr37, which are required for normal ER Ca2+ handling in lymphocytes. Deletion of Pacs1 or Wdr37 caused peripheral lymphopenia that was linked to blunted Ca2+ release from the ER after antigen receptor stimulation. Pacs1-deficient cells showed diminished inositol triphosphate receptor expression together with increased ER and oxidative stress. Mature Pacs1-/- B cells proliferated and died in vivo under lymphocyte replete conditions, indicating spontaneous loss of cellular quiescence. Disruption of Pacs1-Wdr37 did not diminish adaptive immune responses, but potently suppressed lymphoproliferative disease models by forcing loss of quiescence. Thus, Pacs1-Wdr37 plays a critical role in stabilizing lymphocyte populations through ER Ca2+ handling and presents a new target for lymphoproliferative disease therapy.
Keyphrases
- endoplasmic reticulum
- epstein barr virus
- peripheral blood
- oxidative stress
- estrogen receptor
- immune response
- breast cancer cells
- induced apoptosis
- cell proliferation
- cell cycle arrest
- gene expression
- metabolic syndrome
- genome wide
- dna damage
- dendritic cells
- binding protein
- skeletal muscle
- stem cells
- ischemia reperfusion injury
- diffuse large b cell lymphoma
- genetic diversity
- insulin resistance
- cell death
- dna methylation
- mesenchymal stem cells
- wild type
- high fat diet induced
- chemotherapy induced
- heat shock protein