SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W3036682806> ?p ?o ?g. }

Showing items 1 to 100 of ±209 with 100 items per page.

W3036682806 endingPage "629" @default.
W3036682806 startingPage "618" @default.
W3036682806 abstract "Background: Rheumatoid arthritis (RA) is a chronic autoimmune disease that causes inflammation, swelling, and pain in the joints and involves systemic complications. Mouse models of RA have been extensively used to model the pathogenesis of RA and to develop effective therapies. Although many components of the immune system have been studied in these models, the role of crystallizable fragment (Fc) gamma receptors (FcγRs) in RA has been sorely neglected. The aim of this review was to introduce the different mouse models of RA and to describe the different drug development strategies that have been tested in these models to target FcγR function, with the focus being on drugs that have been made from the Fc of immunoglobulin G (IgG). Summary: Evidence suggests that FcγRs play a major role in immune complex-induced inflammation in autoimmune diseases, such as RA. However, there is limited knowledge on the importance of FcγRs in the human disease even though there has been extensive work in mouse models of RA. Numerous mouse models of RA are available, with each model depicting certain aspects of the disease. Induced models of RA have nonspecific immune activation with cartilage-directed autoimmunity, whereas spontaneous models of RA develop without immunization, which results in a more chronic form of arthritis. These models have been used to test FcγR-targeting monoclonal antibodies, intravenous immunoglobulin (IVIg), subcutaneously administered IVIg, and recombinant Fcs for their ability to interact with and modify FcγR function. Recombinant Fcs avidly bind FcγRs and exhibit enhanced therapeutic efficacy in mouse models of RA. Key Message: The therapeutic utility of targeting FcγRs with recombinant Fcs is great and should be explored in human clinical trials for autoimmune diseases, such as RA." @default.
W3036682806 created "2020-06-25" @default.
W3036682806 creator A5009211480 @default.
W3036682806 creator A5040888166 @default.
W3036682806 date "2020-01-01" @default.
W3036682806 modified "2023-09-27" @default.
W3036682806 title "Mouse Models of Rheumatoid Arthritis for Studies on Immunopathogenesis and Preclinical Testing of Fc Receptor-Targeting Biologics" @default.
W3036682806 cites W1176256355 @default.
W3036682806 cites W1222132513 @default.
W3036682806 cites W132781887 @default.
W3036682806 cites W1482301599 @default.
W3036682806 cites W1493742659 @default.
W3036682806 cites W1506260673 @default.
W3036682806 cites W1511428838 @default.
W3036682806 cites W1521993208 @default.
W3036682806 cites W1528655155 @default.
W3036682806 cites W1557312589 @default.
W3036682806 cites W1559576006 @default.
W3036682806 cites W1563290091 @default.
W3036682806 cites W1587080057 @default.
W3036682806 cites W160562812 @default.
W3036682806 cites W1838834699 @default.
W3036682806 cites W1903287340 @default.
W3036682806 cites W1909688331 @default.
W3036682806 cites W1910850885 @default.
W3036682806 cites W1964180982 @default.
W3036682806 cites W1965727970 @default.
W3036682806 cites W1966637800 @default.
W3036682806 cites W1968097109 @default.
W3036682806 cites W1969892170 @default.
W3036682806 cites W1975263472 @default.
W3036682806 cites W1975345897 @default.
W3036682806 cites W1976424613 @default.
W3036682806 cites W1978471536 @default.
W3036682806 cites W1979820418 @default.
W3036682806 cites W1980257318 @default.
W3036682806 cites W1980264776 @default.
W3036682806 cites W1981386893 @default.
W3036682806 cites W1983366184 @default.
W3036682806 cites W1984073642 @default.
W3036682806 cites W1986641742 @default.
W3036682806 cites W1987570598 @default.
W3036682806 cites W1991110217 @default.
W3036682806 cites W1992735759 @default.
W3036682806 cites W1995706666 @default.
W3036682806 cites W1996177911 @default.
W3036682806 cites W1998497661 @default.
W3036682806 cites W1999055902 @default.
W3036682806 cites W2000917302 @default.
W3036682806 cites W2000940419 @default.
W3036682806 cites W2005380915 @default.
W3036682806 cites W2012099358 @default.
W3036682806 cites W2017014846 @default.
W3036682806 cites W2019582534 @default.
W3036682806 cites W2023539775 @default.
W3036682806 cites W2023617209 @default.
W3036682806 cites W2026624868 @default.
W3036682806 cites W2026637485 @default.
W3036682806 cites W2030980006 @default.
W3036682806 cites W2034408745 @default.
W3036682806 cites W2035433348 @default.
W3036682806 cites W2035809826 @default.
W3036682806 cites W2036506588 @default.
W3036682806 cites W2040373810 @default.
W3036682806 cites W2041944580 @default.
W3036682806 cites W2047370882 @default.
W3036682806 cites W2047604325 @default.
W3036682806 cites W2048259741 @default.
W3036682806 cites W2051666192 @default.
W3036682806 cites W2054663993 @default.
W3036682806 cites W2055679334 @default.
W3036682806 cites W2056696895 @default.
W3036682806 cites W2056820060 @default.
W3036682806 cites W2059190713 @default.
W3036682806 cites W2064681913 @default.
W3036682806 cites W2065237510 @default.
W3036682806 cites W2068295318 @default.
W3036682806 cites W2071181996 @default.
W3036682806 cites W2075901113 @default.
W3036682806 cites W2077699888 @default.
W3036682806 cites W2083091113 @default.
W3036682806 cites W2083862543 @default.
W3036682806 cites W2084469556 @default.
W3036682806 cites W2086104998 @default.
W3036682806 cites W2086968511 @default.
W3036682806 cites W2088861734 @default.
W3036682806 cites W2089505245 @default.
W3036682806 cites W2089820020 @default.
W3036682806 cites W2090214639 @default.
W3036682806 cites W2094655231 @default.
W3036682806 cites W2099872624 @default.
W3036682806 cites W2099903298 @default.
W3036682806 cites W2102402967 @default.
W3036682806 cites W2106566540 @default.
W3036682806 cites W2108087703 @default.
W3036682806 cites W2110330644 @default.
W3036682806 cites W2111823261 @default.
W3036682806 cites W2113669085 @default.