Efficacy as well as safety and tolerability of this regimen were evaluated. Result: Thirty-two patients with nephrotic IMN (56% male, age 51.5 ± 12.6 years, estimated Roxadustat price glomerular filtration rate 73.7 ± 20.0 mL/min per 1.73 m2) were included in our study. During the median follow-up duration of 30.0 (12.5–42.8) months, 40.6% of patients achieved complete remission, while 40.6% achieved partial remission. Relapse occurred in five patients in a median of 16 (11.5–26) months after cessation of immunosuppressive treatment. No patients developed renal insufficiency during
the follow up, while 16 side-effects were noted in 10 patients. Complete remission rates at 3, 6 and 15 months were 0%, 12.5% and 40.6% and remission rates were 21.9%, 68.8% and 81.2%, respectively. Complement 3 deposition was significantly associated with the probability of non-remission. Conclusion: Monthly i.v. pulse cyclophosphamide plus oral steroids may be an alternative treatment option in Chinese patients with nephrotic IMN. “
“T AZD6244 ic50 helper
(Th) cells are an integral part of the host’s immune response to eliminate invading pathogens. However, autoimmune or ‘autoinflammatory’ diseases can develop if Th cell responses are not effectively regulated. Several subsets of Th cells exist, including the Th17 subset that produces interleukin-17A, important in experimental models of organ-specific autoimmune inflammation. Its discovery has explained paradoxical observations in model systems thought to be
Th1 mediated but were exacerbated in the absence of interferon-γ, the prototypic Th1 effector cytokine. Th17 cells express unique transcription factors and secrete a unique pattern of cytokines. Interleukin-17A induces pro-inflammatory cytokines and chemokines and mediates neutrophil recruitment. Th17 cells have a reciprocal relationship with T regulatory cells and can also mediate suppression of Th1 responses. Recent studies also suggest that Th17 cells are not terminally differentiated but can switch into Th1 cells. Ergoloid Th17 cells have themselves been recently shown to induce antigen-specific cell-mediated proliferative glomerulonephritis. There is increasing evidence implicating Th17 cells in anti-glomerular basement membrane disease, lupus nephritis and pauci-immune glomerulonephritis. This review will review the discovery of the Th17 subset, its properties, its relationship with other Th subsets and assess the current evidence implicating Th17 cells in glomerulonephritis. T helper (Th) cells play a central role in adaptive immune responses. These antigen-specific cells are activated by antigen presenting cells and orchestrate the elimination of invading pathogens. Seminal studies by Mosmann and Coffman1 have led to the categorization of Th cell subsets identified by the cytokines they produce. Th1 cells secrete γ-interferon (IFN-γ) and LT-α, and are important in directing cell-mediated immunity against intracellular pathogens.