当前位置: 首页 > 期刊 > 《英国眼科学杂志》 > 2004年第8期 > 正文
编号:11325180
How do you know?
http://www.100md.com 《英国眼科学杂志》
     1 Casey Eye Institute, Oregon Health and Science University, Portland, OR, USA

    2 Department of Medicine, Oregon Health and Science University, Portland, OR, USA

    3 Department of Cell and Developmental Biology, Oregon Health and Science University, Portland, OR, USA

    Some thoughts on judging efficacy in treating patients with uveitis

    Keywords: uveitis; treatment; efficacy

    How do you know if your patient improves with any particular therapy? In the treatment of patients with vision threatening uveitis, the primary goal of therapy is far from universally accepted. Should the end point be improvement in visual acuity? An obvious choice but flawed since many patients benefit without a discernable change in acuity measurements. Cataract and macular scars can limit the improvement in acuity even as inflammation is controlled. In addition, acuity measurements do not reflect lighting, effort, or the sporadic variability that some patients observe with uveitis. Should the goal be reduced inflammation as judged by examination? How about improved visual function as judged by patient questionnaire or by physician assessment? Can a drug be deemed efficacious if it results solely in the reduction in a potentially toxic medication such as corticosteroid? Is stabilisation of acuity an adequate goal? If judging benefit is so complex, is there a way to use a single instrument to accommodate multiple potential end points? As we enter an era of trying to base medical decision making on evidence, we need to decide what evidence to accept.

    Rheumatologists have long faced a similar dilemma in judging the efficacy of treatments for autoimmune diseases such as rheumatoid arthritis and systemic lupus erythematosus. The solution has been to rely on expert panels that have tested composite scores which combine objective measures of disease activity with functional outcomes. These disease indices include the ACR20, ACR50, ACR70, ACR-N, ACR-AUC, and DAS.1,2 For example, the ACR20 is defined as 20% improvement in tender and swollen joint scores plus 20% improvement in three out of the following five parameters: patient’s global assessment, physician’s global assessment, level of pain on a visual analogue scale, health assessment questionnaire measuring function, and sedimentation rate.1 This instrument has been widely employed in judging benefit in clinical trials for rheumatoid arthritis.

    The randomised controlled trial (RCT) is generally considered the gold standard for assessing clinical efficacy. RCTs are frequent in some medical fields such as oncology and they are increasingly common in the treatment of rheumatological diseases. RCTs in ophthalmology such as the ONTT,3 COMS,4 OHTS,5 and the ETDRS6 have provided insights that now guide many therapeutic decisions. RCTs have only rarely been undertaken for ocular inflammatory disease, in part because of the relative rarity of these diseases. But RCTs for uveitis are also challenging because judging efficacy is not a straightforward task. Thus, some trials begin with inflammation that is quiescent and ascribe efficacy if other systemic immunosuppressive therapy is reduced.7 Other trials judge efficacy based on the more conventional improvement in visual acuity. A measure of efficacy that could accommodate patients with active disease who are failing conventional therapy, patients with controlled disease who are receiving potentially toxic therapy, and patients whose visual function improves even without a measurable change in visual acuity would be a major boon to encouraging clinical trials.

    Both patients and physicians would benefit on agreement as to what constitutes clinical improvement

    There is a need for the development of a standardised approach in choosing outcome measures in clinical trials of therapies in uveitis by the international ophthalmology community. End points or outcome measures may quantify: objective physical signs such as cell counts on slit lamp examination, vitreous haze, or visual acuity; macular oedema as measured by ocular coherence tomography or fluorescein angiography; reduction in a potentially toxic medication; and visual functional status as perceived by the patient and the physician. Each individual outcome measure will need to be "weighted" for importance according to the evidence from previous trials, their validity (see table 1), reliability, and their discriminatory power to assess "change over time."8,9 Each outcome measure should contribute significant and non-duplicated information. Once a "core set" of such outcome measures is prepared from the recommendations from the experts in the field, consensus could be reached by discussions to develop a composite outcome measure that incorporates separate individual end points. Future clinical trials could then test the robustness of this new instrument.

    Table 1 Validity parameters for outcome measures

    Biological therapies that alter immune mediated diseases are emerging for difficult therapeutic challenges including rheumatoid arthritis,10 Crohn’s disease,11 systemic lupus erythematosus,12 psoriasis,13 spondyloarthropathy,14 and transplant rejection.15 It is extremely likely that some of these therapies will find a niche in the treatment of patients with uveitis. Indeed, some uncontrolled trials for several of the biological therapies are very encouraging,7,16 while some small RCTs have been less enthusiastic for other biological treatments.17

    We believe that the testing of biological and other novel therapies for uveitis needs to be encouraged, that this testing can be facilitated by utilising a composite index which recognises that improvement can be reflected in different fashions, and that such an index is best validated by a panel of experts using consensus to assess benefit similar to what has been achieved in rheumatology based on testing of the index on illustrative cases.

    Currently, we are not able to answer the question, "How do you know?" While a hug from a grateful patient is gratifying, hugs are difficult to measure in RCTs. Both patients and physicians would benefit on agreement as to what constitutes clinical improvement. As our treatment decisions become evidence based, we need to look critically at what evidence should be employed.

    REFERENCES

    Felson DT, Anderson JJ, Boers M, et al. American College of Rheumatology. Preliminary definition of improvement in rheumatoid arthritis. Arthritis Rheum 1995;38:727–35.

    Fleisher LN, Ferrell JB, McGahan MC. Synergistic uveitic effects of tumor necrosis factor alpha and interleukin-1 beta. Invest Ophthalmol Vis Sci 1992;33:2120–7.

    Beck RW, Trobe JD, Moke PS, et al. High- and low-risk profiles for the development of multiple sclerosis within 10 years after optic neuritis: experience of the optic neuritis treatment trial. Arch Ophthalmol 2003;121:944–9.

    Group COMS. Trends in size and treatment of recently diagnosed choroidal melanoma. Arch Ophthalmol 2003;121:1156–62.

    Gordon MO, Beiser JA, Brandt JD, et al. The ocular hypertension treatment study: baseline factors that predict the onset of primary open-angle glaucoma. Arch Ophthalmol 2002;120:714–20.

    Chew EY, Klein ML, Murphy RP, et al. Effects of aspirin on vitreous/preretinal hemorrhage in patients with diabetes mellitus. Early Treatment Diabetic Retinopathy Study report no 20. Arch Ophthalmol 1995;113:52–5.

    Nussenblatt RB, Fortin E, Schiffman R, et al. Treatment of noninfectious intermediate and posterior uveitis with the humanized anti-Tac mAb: a phase I/II clinical trial. Proc Natl Acad Sci USA 1999;96:7462–6.

    Tugwell P , Bombardier C. A methodologic framework for developing and selecting endpoints in clinical trials. J Rheumatol 1982;9:758–62.

    Van der Heijde DM, Van’t Hof MA, van Riel PL, et al. Validity of single variables and composite indices for measuring disease activity in rheumatoid arthritis. Ann Rheum Dis 1992;51:177–81.

    Weinblatt ME, Kremer JM, Bankhurst AD, et al. A trial of etanercept, a recombinant tumor necrosis factor receptor: Fc fusion protein, in patients with rheumatoid arthritis receiving methotrexate. N Engl J Med 1999;340:253–9.

    Ghosh S , Goldin E, Gordon FH, et al. Natalizumab for active Crohn’s disease. N Engl J Med 2003;348:68–72.

    Leandro MJ, Edwards JC, Cambridge G, et al. An open study of B lymphocyte depletion in systemic lupus erythematosus. Arthritis Rheum 2002;46:2673–7.

    Weinberg JM. An overview of infliximab, efalizumab, and alefacept as biologic therapy for psoriasis. Clin Ther 2003;25:2487–505.

    Braun J , Brandt J, Listing J, et al. Long-term efficacy and safety of infliximab in the treatment of ankylosing spondylitis. Arthritis Rheum 2003;48:2224–33.

    Beniaminovitz A , Itescu S, Lietz K, et al. Prevention of rejection in cardiac transplantation by blockade of the interleukin-2 receptor with a monoclonal antibody. N Engl J Med 2000;342:613–19.

    Sfikakis PP, Theodossiadis PG, Katsiari CG, et al. Effect of infliximab on sight-threatening panuveitis in Beh?et’s disease. Lancet 2001;358:295–6.

    Foster CS, Tufail F, Waheed NK, et al. Efficacy of etanercept in preventing relapse of uveitis controlled by methotrexate. Arch Ophthalmol 2003;12:437–40.(J T Rosenbaum1,2,3, A Deo)