Soluble Fas ligand (sFasL) as a predictor of reduction of general psychopathology in schizophrenia after antipsychotic treatment

Szymona, Kinga; Karakuła-Juchnowicz, Hanna; Zdzisińska, Barbara; Flis, Marta; Kaławaj, Katarzyna; Rosa, Wojciech; Kandefer‐Szerszeń, Martyna

doi:10.1016/j.eurpsy.2016.01.096

Cited by 1 publication

(1 citation statement)

References 0 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…There is a substantial translational potential for our understanding of the roles and regulation of various forms of released Fas ligand. This includes development of novel approaches to treatment with, for example, FasL-fused humanized antibodies to sensitize target cells to cell death [ 108 , 109 , 110 ] as suggested in glaucoma treatment [ 111 , 112 ], novel forms of RNA therapy [ 113 ], prognosis of long-term allergic outcomes at birth [ 114 ] or even for schizophrenia treatment [ 115 ]. However, there remain a number of outstanding problems that need to be addressed with regard to soluble Fas ligand as a therapeutic target.…”

Section: Discussionmentioning

confidence: 99%

sFasL—The Key to a Riddle: Immune Responses in Aging Lung and Disease

Wallach-Dayan

Petukhov

Ahdut-HaCohen

et al. 2021

IJMS

View full text Add to dashboard Cite

By dint of the aging population and further deepened with the Covid-19 pandemic, lung disease has turned out to be a major cause of worldwide morbidity and mortality. The condition is exacerbated when the immune system further attacks the healthy, rather than the diseased, tissue within the lung. Governed by unremittingly proliferating mesenchymal cells and increased collagen deposition, if inflammation persists, as frequently occurs in aging lungs, the tissue develops tumors and/or turns into scars (fibrosis), with limited regenerative capacity and organ failure. Fas ligand (FasL, a ligand of the Fas cell death receptor) is a key factor in the regulation of these processes. FasL is primarily found in two forms: full length (membrane, or mFasL) and cleaved (soluble, or sFasL). We and others found that T-cells expressing the mFasL retain autoimmune surveillance that controls mesenchymal, as well as tumor cell accumulation following an inflammatory response. However, mesenchymal cells from fibrotic lungs, tumor cells, or cells from immune-privileged sites, resist FasL+ T-cell-induced cell death. The mechanisms involved are a counterattack of immune cells by FasL, by releasing a soluble form of FasL that competes with the membrane version, and inhibits their cell death, promoting cell survival. This review focuses on understanding the previously unrecognized role of FasL, and in particular its soluble form, sFasL, in the serum of aged subjects, and its association with the evolution of lung disease, paving the way to new methods of diagnosis and treatment.

show abstract