1993
DOI: 10.1073/pnas.90.22.10764
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Intraarticular expression of biologically active interleukin 1-receptor-antagonist protein by ex vivo gene transfer.

Abstract: Gene therapy offers a radical different approach to the treatment of arthritis. Here we have demonstrated that two marker genes (lacZ and neo) and cDNA coding for a potentially therapeutic protein (human interleukin 1-receptor-antagonist protein; IRAP or IL-lra) can be delivered, by ex vivo techniques, to the synovial lining of joints; intraarticular expression of IRAP inhibited intraarticular responses to interleukin 1. To achieve this, lapine synoviocytes were first transduced in culture by retroviral infect… Show more

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Cited by 278 publications
(150 citation statements)
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“…The lack of inflammatory cells or inflamed pannus has also been previously described in the rat model of iodoacetate-induced OA, where an inflammatory process that is not associated with cell infiltration may underlie the development of OA, and there is pain behavior related to the joints (29). Conversely, previous studies using IL-1␤ in rodent models of arthritis have shown RA-like pathologic development in the joint for up to 1 month following intraarticular cytokine injection of methylated bovine serum albumin (10) or ex vivo administration of IL-1-transduced synovial cells (30,31), which resolved shortly thereafter. In contrast to these short-term models, the Col1-IL-1␤ XAT -transgenic mouse may serve as a model for long-term studies of arthritis.…”
Section: Discussionmentioning
confidence: 99%
“…The lack of inflammatory cells or inflamed pannus has also been previously described in the rat model of iodoacetate-induced OA, where an inflammatory process that is not associated with cell infiltration may underlie the development of OA, and there is pain behavior related to the joints (29). Conversely, previous studies using IL-1␤ in rodent models of arthritis have shown RA-like pathologic development in the joint for up to 1 month following intraarticular cytokine injection of methylated bovine serum albumin (10) or ex vivo administration of IL-1-transduced synovial cells (30,31), which resolved shortly thereafter. In contrast to these short-term models, the Col1-IL-1␤ XAT -transgenic mouse may serve as a model for long-term studies of arthritis.…”
Section: Discussionmentioning
confidence: 99%
“…28 Plasmid P41ICPO-IL-1Ra: This plasmid was constructed in the same manner as p41ICP0-TNFSRexcept that the IL1Ra cDNA fused to the SV40 polyadenylation sequence was inserted into p41ICP0lacZ in place of the TNFSR cDNA. 3 Vectors S/0-TNFSR and T/0-sTNF␣R: The TNFSR recombination plasmid described above was introduced into the genome of SOZ.1 using the previously described PacI recombination strategy. 26 Briefly, PacI endonuclease digested SOZ.1 genomic DNA was co-transfected along with the recombination plasmid p41ICP0-TNFSRinto 7b cells using standard calcium phosphate methods.…”
Section: Plasmid and Vector Constructionmentioning
confidence: 99%
“…For this procedure, cells were surgically harvested from the synovial lining of the joint, cultured and transduced by a retroviral vector in vitro, and the genetically modified cells injected into the joint space to recolonize the synovium. 3,4 Ex vivo delivery of the interleukin-1 receptor antagonist cDNA to the joints of rabbits with experimental arthritis was found to have significant therapeutic benefit. 5 More recently, a phase I clinical trial was implemented to evaluate the safety and feasibility of using ex vivo gene delivery in the treatment of RA.…”
Section: Introductionmentioning
confidence: 99%
“…Several recent studies have been successful in introducing genes into the synovium of the knee joints of rabbits by both ex vivo 30,31 and in vitro 32,33 methods. One potentially therapeutic gene encoding the human interleukin-1 (IL-1) receptor antagonist has been tested in some detail.…”
Section: Figure 4 Immunohistochemical Analysis Of the Effects Of Hfasmentioning
confidence: 99%