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8001. Herbal medicines for the treatment of osteoarthritis: a systematic review.
Limitations in the conventional medical management of osteoarthritis indicate a real need for safe and effective treatment of osteoarthritis patients. Herbal medicines may provide a solution to this problem. The aim of this article was to review systematically all randomized controlled trials on the effectiveness of herbal medicines in the treatment of osteoarthritis.
8002. Comparison of three active therapies for chronic low back pain: results of a randomized clinical trial with one-year follow-up.
To examine the relative efficacy of three active therapies for patients with chronic low back pain.
8003. Churg-Strauss syndrome: outcome and long-term follow-up of 32 patients.
作者: R Solans.;J A Bosch.;C Pérez-Bocanegra.;A Selva.;P Huguet.;J Alijotas.;R Orriols.;L Armadans.;M Vilardell.
来源: Rheumatology (Oxford). 2001年40卷7期763-71页
To study the clinical spectrum and evolution of Churg-Strauss syndrome in order to assess the clinicopathological features of the disease, the response to treatment and the long-term outcome.
8004. Evidence for inadequate construct validity of the Disease Repercussions Profile in people with rheumatoid arthritis.
To re-evaluate the construct validity of the Disease Repercussions Profile (DRP), a measure of handicap in arthritis populations.
8005. Monoclonal antibodies against human ribosomal P proteins penetrate into living cells and cause apoptosis of Jurkat T cells in culture.
作者: K H Sun.;S J Tang.;M L Lin.;Y S Wang.;G H Sun.;W T Liu.
来源: Rheumatology (Oxford). 2001年40卷7期750-6页
This study was designed to determine the role of autoantibodies to the ribosomal P protein (anti-P Abs) in the pathogenesis of systemic lupus erythematosus (SLE) using monoclonal anti-P antibodies (anti-P mAbs).
8006. Cytokines play an aetiopathogenetic role in fibromyalgia: a hypothesis and pilot study.
作者: D J Wallace.;M Linker-Israeli.;D Hallegua.;S Silverman.;D Silver.;M H Weisman.
来源: Rheumatology (Oxford). 2001年40卷7期743-9页
To measure soluble factors having a possible role in fibromyalgia (FM) and compare the profiles of patients with recent onset of the syndrome with patients with chronic FM.
8007. Alternatively spliced EDA-containing fibronectin in synovial fluid as a predictor of rheumatoid joint destruction.
Fibronectin containing the EDA region (EDA(+)Fn), a molecule important for rheumatoid joint destruction, was measured in relation to the progression of joint destruction in rheumatoid arthritis (RA).
8008. From bench to bedside: discovering rules for antibody design, and improving serotherapy with monoclonal antibodies.
Anti-T-cell monoclonal antibodies (mAbs) form a unique class of therapeutic agent. Their precise specificity offers tremendous potential for the treatment of autoimmune and inflammatory diseases but also prevents meaningful preclinical animal studies. In particular, adverse reactions to therapy may be unanticipated, and the first administration of a novel T-cell mAb to a patient thus marks the beginning of a unique experiment. By comparing clinical parameters and laboratory measurements, small-scale pilot studies can provide detailed information about mAb biology that both predicts and suggests solutions to the complications of therapy. In this essay I illustrate this concept with reference to three specific areas: lymphocyte depletion, mAb immunogenicity and cytokine-release syndromes. In each case, systematic clinical and laboratory science has improved our understanding of the problem and suggested solutions; most of these solutions have been or are being adopted. Thus, small, open studies are an essential step in the development of novel mAbs, provide an ideal platform for the study of mAb biology, and serve as an early warning system for potential adverse effects.
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