Expert Opinion on Orphan Drugs最新文献_第10页

Monitoring progression of retinitis pigmentosa: current recommendations and recent advances. 监测视网膜色素变性的进展:目前的建议和最新进展。

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2020-01-01 Epub Date: 2020-03-02 DOI: 10.1080/21678707.2020.1735352

Moreno Menghini, Jasmina Cehajic-Kapetanovic, Robert E MacLaren

ABSTRACT Introduction: Retinitis pigmentosa (RP) is the most common form of inherited retinal degenerations with an estimated prevalence of 1 in 4,000 and more than 1 million individuals affected worldwide. With the introduction of the first retinal gene therapy in 2017, the importance of understanding the mechanisms of retinal degeneration and its natural progression has shifted from being of academic interest to being of pivotal for the development of new therapies. Areas covered: This review covers standard and innovative diagnostic techniques and complementary examinations needed for the evaluation and treatment of RP. It includes chapters on the assessment of visual function, retinal morphology, and genotyping. Expert opinion: Monitoring the progression of RP can best be achieved by combining assessments of both visual function and morphology. Visual acuity testing using ETDRS charts should be complemented by low-luminance visual acuity and color vision tests. Assessment of the visual field can also be useful in less advanced cases. In those with central RP involvement measuring retinal sensitivity using microperimetry is recommended. Retinal morphology is best assessed by OCT and autofluorescence. Genetic testing is pivotal as it contributes to the pathophysiological understanding and can guide clinical management as well as identify individuals that could benefit from retinal gene therapy.

色素性视网膜炎(RP)是遗传性视网膜变性最常见的形式，估计患病率为1 / 4000，全世界有超过100万人受到影响。随着2017年首个视网膜基因疗法的引入，了解视网膜变性及其自然进展机制的重要性已经从学术兴趣转变为开发新疗法的关键。涵盖领域:本综述涵盖了RP评估和治疗所需的标准和创新诊断技术以及补充检查。它包括章节视觉功能的评估，视网膜形态，和基因分型。专家意见:通过结合视觉功能和形态学评估来监测RP的进展是最好的。使用ETDRS图表进行视力测试应辅以低亮度视力和色觉测试。视野评估在不太严重的病例中也很有用。在中枢性RP受累的患者中，建议使用显微镜测量视网膜灵敏度。视网膜形态最好通过OCT和自身荧光来评估。基因检测是至关重要的，因为它有助于病理生理学的理解，可以指导临床管理以及识别个体，可以从视网膜基因治疗中受益。

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引用次数: 28

The future of gene-targeted therapy for hereditary tyrosinemia type 1 as a lead indication among the inborn errors of metabolism. 基因靶向治疗遗传性1型酪氨酸血症作为先天性代谢错误的主要指征的未来。

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2020-01-01 Epub Date: 2020-07-21 DOI: 10.1080/21678707.2020.1791082

Whitney S Thompson, Gourish Mondal, Caitlin J Vanlith, Robert A Kaiser, Joseph B Lillegard

Introduction: Inborn errors of metabolism (IEMs) often result from single-gene mutations and collectively cause liver dysfunction in neonates leading to chronic liver and systemic disease. Current treatments for many IEMs are limited to maintenance therapies that may still require orthotropic liver transplantation. Gene therapies offer a potentially superior approach by correcting or replacing defective genes with functional isoforms; however, they face unique challenges from complexities presented by individual diseases and their diverse etiology, presentation, and pathophysiology. Furthermore, immune responses, off-target gene disruption, and tumorigenesis are major concerns that need to be addressed before clinical application of gene therapy.

Areas covered: The current treatments for IEMs are reviewed as well as the advances in, and barriers to, gene therapy for IEMs. Attention is then given to ex vivo and in vivo gene therapy approaches for hereditary tyrosinemia type 1 (HT1). Of all IEMs, HT1 is particularly amenable to gene therapy because of a selective growth advantage conferred to corrected cells, thereby lowering the initial transduction threshold for phenotypic relevance.

Expert opinion: It is proposed that not only is HT1 a safe indication for gene therapy, its unique characteristics position it to be an ideal IEM to develop for clinical investigation.

先天性代谢错误(IEMs)通常由单基因突变引起，并共同导致新生儿肝功能障碍，导致慢性肝脏和全身性疾病。目前许多IEMs的治疗仅限于维持治疗，可能仍然需要原位异位肝移植。基因治疗提供了一种潜在的优越方法，通过功能同种异构体纠正或替换有缺陷的基因;然而，他们面临着来自个体疾病及其不同病因、表现和病理生理的复杂性的独特挑战。此外，免疫反应、脱靶基因破坏和肿瘤发生是基因治疗临床应用前需要解决的主要问题。涵盖领域:综述了目前的基因治疗方法，以及基因治疗的进展和障碍。然后关注遗传性1型酪氨酸血症(HT1)的体外和体内基因治疗方法。在所有的IEMs中，HT1特别适合基因治疗，因为被纠正的细胞具有选择性生长优势，从而降低了表型相关性的初始转导阈值。专家意见:HT1不仅是一种安全的基因治疗适应症，而且其独特的特性使其成为一种理想的用于临床研究的IEM。

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引用次数: 9

Inhibiting inflammatory cytokines in adult onset Still’s disease. Current trends and new therapeutic perspectives 在成人斯蒂尔病中抑制炎性细胞因子。当前趋势和新的治疗前景

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-12-02 DOI: 10.1080/21678707.2019.1701431

P. Ruscitti, A. Conforti, V. Pavlych, R. Giacomelli

ABSTRACT Introduction: Multiple lines of evidence suggest the clinical usefulness of inhibiting inflammatory cytokines in patients affected by adult onset Still’s disease (AOSD), a rare inflammatory disease. The lack of response to the first therapeutic strategy with glucocorticoids and synthetic disease-modifying anti-rheumatic drugs (DMARDs) identifies ‘refractory patients’, to be subsequently treated with biologic DMARDs. Areas covered: In this article, evidence has been reviewed about the clinical usefulness of biologic DMARDs, targeting inflammatory cytokines, in AOSD, analyzing current trends and suggesting future therapeutic perspectives. Expert opinion: Therapeutic management of AOSD is directed at targeting inflammatory signs and symptoms, preventing life-threating complications, and minimizing the adverse effects of immunosuppressive therapies. In this context, over the last decade, the clinical usefulness of inhibiting inflammatory cytokines has shown in AOSD with multiple benefits, since a large percentage of patients attain a clinical response. The inhibition of inflammatory cytokines could also be helpful in managing life-threating complications of AOSD. Going forward, this field of research is rapidly growing, and in the next future, the results about ongoing randomized controlled trials and the development of clinical tools readily transferable in clinical practice, would improve the management of AOSD providing more targeted treatment and improving the outcomes of these patients.

摘要:多项证据表明，抑制炎症细胞因子在成人发病斯蒂尔病(AOSD)患者中的临床应用价值。斯蒂尔病是一种罕见的炎症性疾病。对糖皮质激素和合成疾病缓解抗风湿药物(DMARDs)的第一种治疗策略缺乏反应确定了“难治性患者”，随后用生物DMARDs治疗。涉及领域:本文回顾了针对炎症细胞因子的生物DMARDs在AOSD中的临床应用，分析了目前的趋势，并提出了未来的治疗前景。专家意见:AOSD的治疗管理是针对炎症体征和症状，预防危及生命的并发症，并尽量减少免疫抑制治疗的不良反应。在此背景下，在过去的十年中，抑制炎症细胞因子的临床用途已经在AOSD中显示出多种益处，因为很大比例的患者获得了临床反应。抑制炎症细胞因子也可能有助于控制危及生命的AOSD并发症。展望未来，这一领域的研究正在迅速发展，在未来，正在进行的随机对照试验的结果和临床工具的开发很容易在临床实践中转移，将改善AOSD的管理，提供更有针对性的治疗，改善这些患者的预后。

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引用次数: 0

The senseless orphanage of Chagas disease 恰加斯病的孤儿院

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-12-02 DOI: 10.1080/21678707.2019.1701432

C. Alonso-Vega, Irene Losada-Galván, M. Pinazo, Javier Sancho Mas, J. G. Brustenga, J. Alonso-Padilla

ABSTRACT Introduction: Chagas disease is caused by the parasite Trypanosoma cruzi. Endemic in 21 American countries, there are ~7 million people infected, of which 14,000 die every year. Despite this burden, Chagas remains an orphan disease as it mainly affects poor communities with low economic and political power. Areas covered: There are two drugs available to treat the infection, but both have safety and efficacy issues. Investment in new treatments and other control measures has been historically neglected. This trend is changing and there are novel perspectives to put an end to this senseless orphanage. Research and development agenda of new therapies, diagnostic tools and biomarkers have moved forward during the last decade; and patients associations have been active in promoting awareness of the disease all along. Besides, the WHO recently declared April 14th as the ‘World Chagas disease day’, which will increase the visibility of the disease and attract attention internationally. Expert opinion: Efforts must focus on the prevention of new infections, but also in the management of the millions already chronically infected. This will require an integral approach where increasing the number of trained health workers and generalizing access to diagnosis and treatment will be fundamental.

摘要简介：恰加斯病是由克氏锥虫引起的。在21个美国国家流行，约有700万人感染，其中每年有14000人死亡。尽管有这种负担，查加斯仍然是一种孤儿病，因为它主要影响经济和政治权力低下的贫困社区。涵盖领域：有两种药物可用于治疗感染，但都存在安全性和有效性问题。对新治疗和其他控制措施的投资历来被忽视。这种趋势正在改变，有新的视角来结束这个毫无意义的孤儿院。新疗法、诊断工具和生物标志物的研发议程在过去十年中取得了进展；患者协会一直在积极提高人们对该疾病的认识。此外，世界卫生组织最近宣布4月14日为“世界恰加斯病日”，这将提高该病的知名度，并引起国际关注。专家意见：工作必须集中在预防新的感染上，但也要集中在管理数百万已经长期感染的人上。这将需要一种综合方法，增加受过培训的卫生工作者的数量和普及诊断和治疗将是至关重要的。

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引用次数: 5

An update on the progress of preclinical models for guiding therapeutic management of neuronal ceroid lipofuscinosis 指导神经元类脂褐质病治疗管理的临床前模型进展

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-12-02 DOI: 10.1080/21678707.2019.1703672

Hemanth R. Nelvagal, J. Cooper

ABSTRACT Introduction: The neuronal ceroid lipofuscinoses (NCLs) are a group of pediatric inherited neurodegenerative disorders affecting children and young adults. All forms of NCL are fatal and with no curative therapies available there is a pressing need to model their pathology in biological model systems to enable the systematic and rigorous testing of preclinical therapies. Areas covered: This article discusses and provides an update on the recent advances in modelling NCL disease pathology in various different model systems and their relevance to testing preclinical therapies so as to ensure optimal translation into human patients. The research articles discussed here were curated from PubMed (Last accessed-12.4.19) and Google Scholar (Last access-12.4.19) databases. Expert opinion: Both in vitro and in vivo biological model systems have been established for various forms of NCL. These have informed us about pathophysiology, revealed novel therapeutic targets, and provided landmarks of disease progression against which to test potential therapies. Studying NCL pathology across different species has been very informative regarding where therapies need to be delivered with an increasing focus on disease outside the brain. Testing such therapies in animal models of increasing complexity has allowed the translation of more efficacious therapies for clinical trials.

摘要简介：神经元类脂褐质病（NCLs）是一组影响儿童和年轻人的儿童遗传性神经退行性疾病。所有形式的NCL都是致命的，由于没有可用的治疗方法，迫切需要在生物模型系统中对其病理进行建模，以实现临床前治疗的系统和严格测试。涵盖领域：本文讨论并提供了在各种不同模型系统中建模NCL疾病病理学的最新进展，以及它们与测试临床前疗法的相关性，以确保最佳转化为人类患者。这里讨论的研究文章来自PubMed（上次访问12.4.19）和Google Scholar（上次访问12.4.19）数据库。专家意见：已经建立了各种形式的NCL的体外和体内生物模型系统。这些为我们了解了病理生理学，揭示了新的治疗靶点，并为测试潜在的治疗方法提供了疾病进展的标志。研究不同物种的NCL病理学，对于需要在哪里提供治疗提供了非常丰富的信息，越来越关注脑外疾病。在日益复杂的动物模型中测试这种疗法，可以将更有效的疗法转化为临床试验。

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引用次数: 0

Pharmacological therapy in a rare disease: challenges in the long-term management of granulomatosis with polyangiitis 一种罕见疾病的药物治疗：肉芽肿伴多血管炎长期治疗的挑战

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-12-02 DOI: 10.1080/21678707.2019.1701433

J. Sultana, N. Azzopardi-Muscat, B. Coleiro, L. Grech, M. Muscat, D. Santoro, G. Trifirò

Department of Biomedical and Dental Sciences and Morpho-functional Imaging, University of Messina, Messina, Italy; Directorate for Health Information and Research, Guardamangia, Malta; Rheumatology Unit, Mater Dei Hospital, Msida, Malta; Pharmacy Department, Faculty of Medicine and Surgery, University of Malta, Msida, Malta; National Alliance for Rare Disease Support, Malta; Department of Clinical and Experimental Medicine, University of Messina, Messina, Italy

意大利墨西拿大学生物医学和牙科科学与形态功能成像系;卫生信息和研究局，瓜达曼吉亚，马耳他;马耳他姆西达Mater Dei医院风湿病科;马耳他大学医学和外科学院药学系，马耳他姆西达;马耳他全国罕见病支持联盟;意大利墨西拿大学临床与实验医学系

引用次数: 2

Variability in management and outcomes of therapy with eculizumab in atypical hemolytic uremic syndrome 异珠单抗治疗非典型溶血性尿毒症综合征的管理和结果的可变性

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-12-02 DOI: 10.1080/21678707.2019.1703108

E. García-Martín, S. Manrique-Rodríguez, C. Martínez Fernández-Llamazares, Marian Goicoechea-Diezhondino, Olalla Álvarez-Blanco, M. García-Morin, M. Sanjurjo-Sáez

ABSTRACT Objectives: Atypical hemolytic uremic syndrome (aHUS) is a thrombotic microangiopathy caused by complement dysregulation. The aim of this study was to establish the efficacy and safety of eculizumab in patients with aHUS in clinical practice and to describe different individualization strategies. Methods: Authors performed an observational, longitudinal, and ambispective study at a tertiary care center. Clinical histories of patients in treatment with eculizumab were reviewed. Effectiveness and safety were assessed with the evolution of analytical parameters, symptoms and concomitant therapies required. Results: Authors included five patients (two children). The patients were followed up from diagnosis and first administration of eculizumab. Four patients discontinued eculizumab: one because he had anti-factor H autoantibodies that could be managed with immunosuppressive therapy, another because of non-response, and the other two because of clinical stabilization, resolution of TMA, and no findings of high-risk mutations in complement factors. Therapy was tapered in the remaining patients in aHUS remission. No adverse events were identified during or after treatment. Conclusion: Eculizumab is an effective and safe treatment for patients diagnosed with primary or secondary aHUS. Personalized treatment, tapering or discontinuation should be taken on an individual basis by a multidisciplinary team in order to increase the cost-effectiveness of this therapy.

目的:非典型溶血性尿毒症综合征(aHUS)是一种由补体失调引起的血栓性微血管疾病。本研究的目的是在临床实践中确定eculizumab在aHUS患者中的有效性和安全性，并描述不同的个体化策略。方法:作者在一家三级保健中心进行了一项观察性、纵向和双视角研究。我们回顾了接受eculizumab治疗的患者的临床病史。根据分析参数、症状和所需的伴随治疗的演变评估有效性和安全性。结果:作者纳入5例患者(2例儿童)。患者从诊断和首次给药开始随访。4例患者停用eculizumab: 1例患者有抗因子H自身抗体，可通过免疫抑制治疗，另1例患者无应答，另外2例患者临床稳定，TMA消退，补体因子未发现高危突变。其余aHUS缓解患者的治疗逐渐减少。在治疗期间或治疗后未发现不良事件。结论:Eculizumab对于原发性或继发性aHUS患者是一种有效且安全的治疗方法。个体化治疗，减量或停药应由多学科团队在个体基础上采取，以提高该治疗的成本效益。

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引用次数: 0

Sydenham’s chorea: an update on pathophysiology, clinical features and management 西德纳姆舞蹈病:病理生理学、临床特征和治疗的最新进展

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-11-02 DOI: 10.1080/21678707.2019.1684259

L. Vasconcelos, M. Vasconcelos, M. C. Nunes, A. Teixeira

ABSTRACT Introduction: Sydenham’s chorea is an autoimmune hyperkinetic movement disorder that emerges after a group A beta-hemolytic streptococcal (GABHS) pharyngitis. It is the neurological manifestation of acute rheumatic fever. Low quality studies are the current reference for the symptomatic and/or immunomodulatory treatment of Sydenham’s chorea. Areas covered: This review contemplates the clinical features and pathophysiological aspects of Sydenham’s chorea focusing on their implications for therapeutics. It also provides an updated perspective on treatment based on antipsychotics, corticosteroids and other immunomodulatory strategies. Expert opinion: Therapeutic options for Sydenham’s chorea are still largely empirical. Based on the available evidence on the natural history of Sydenham’s chorea and other immune-mediated movement disorders, an early anti-inflammatory or immune-based approach could prevent and/or attenuate chorea, cognitive and behavioral dysfunction. A treatment algorithm for Sydenham’s chorea is proposed.

摘要简介：Sydenham舞蹈病是一种自身免疫性高动力运动障碍，发生在a组β-溶血性链球菌（GABAS）咽炎之后。这是急性风湿热的神经系统表现。低质量研究是目前Sydenham舞蹈病症状和/或免疫调节治疗的参考。涵盖的领域：这篇综述考虑了Sydenham舞蹈病的临床特征和病理生理方面，重点是它们对治疗的影响。它还提供了基于抗精神病药物、皮质类固醇和其他免疫调节策略的治疗的最新视角。专家意见：Sydenham舞蹈病的治疗方案在很大程度上仍然是经验性的。根据Sydenham舞蹈病和其他免疫介导的运动障碍的自然史的现有证据，早期抗炎或基于免疫的方法可以预防和/或减轻舞蹈病、认知和行为功能障碍。提出了一种Sydenham舞蹈病的治疗算法。

引用次数: 6

Duodenal adenocarcinoma: neoadjuvant and adjuvant therapy strategies 十二指肠腺癌：新辅助和辅助治疗策略

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-11-02 DOI: 10.1080/21678707.2019.1684257

A. Dave, Jason T. Wiseman, J. Cloyd

ABSTRACT Introduction: Duodenal adenocarcinoma (DA) is a relatively rare gastrointestinal malignancy associated with poor outcomes. The mainstay of treatment is surgical resection with regional lymphadenectomy but recurrence rates remain high. Due to the relatively low incidence of DA, the lack of randomized controlled trials, and its inclusion with heterogeneous groups of periampullary and other small bowel cancers, strong evidence for the use of neoadjuvant or adjuvant treatment approaches is lacking. Areas covered: The purpose of this article is to review the existing literature on neoadjuvant and adjuvant therapy options along with surgical options for patients with DA. Expert opinion: The primary management of localized DA is surgical resection with negative margins and regional lymphadenectomy. Adjuvant therapy should be recommended for all patients with high-risk pathologic features such as positive lymph nodes or microscopically positive margins. The use of neoadjuvant therapy should be reserved for those patients with locally advanced disease who require downstaging to facilitate resectability. Nevertheless, given the relative rarity of DA, the available literature to guide optimal multimodality treatment decisions is minimal and additional research is needed. In the meantime, patients with DA should be treated at experienced tertiary centers by multidisciplinary oncology teams.

摘要简介：十二指肠腺癌是一种相对罕见的胃肠道恶性肿瘤，预后较差。主要的治疗方法是手术切除局部淋巴结切除术，但复发率仍然很高。由于DA的发病率相对较低，缺乏随机对照试验，且其与壶腹周围癌和其他小肠癌的异质性组相结合，因此缺乏使用新辅助或辅助治疗方法的有力证据。所涵盖的领域：本文的目的是回顾关于DA患者的新辅助和辅助治疗方案以及手术方案的现有文献。专家意见：局限性DA的主要治疗方法是阴性边缘手术切除和区域淋巴结切除。对于所有具有高风险病理特征（如淋巴结阳性或镜检阳性边缘）的患者，应推荐辅助治疗。新辅助治疗的使用应保留给那些需要降低分期以促进可切除性的局部晚期疾病患者。然而，鉴于DA相对罕见，指导最佳多模式治疗决策的现有文献很少，还需要更多的研究。同时，DA患者应在经验丰富的三级中心接受多学科肿瘤学团队的治疗。

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引用次数: 1

How many zebras are there, and where are they hiding in medical literature? A literature review of publications on rare diseases 那里有多少斑马，它们在医学文献中藏在哪里？罕见病文献综述

IF 0.8 4区医学 Q4 PHARMACOLOGY & PHARMACY

Expert Opinion on Orphan Drugs

Pub Date : 2019-11-01 DOI: 10.1080/21678707.2019.1684260

J. Walewski, Daniel L. Donovan, Mukund Nori

ABSTRACT Background: Reliable and accurate medical literature is essential for patients with rare diseases (affecting ~400 million people globally), their advocates, and caregivers (PACs), and health-care professionals (HCPs). Methods: We quantified the number of English-language publications on rare diseases in PubMed from 2009 to 2018. To test our search strategy, we evaluated inclusion of articles on 20 randomly selected rare diseases. We further examined 100 randomly selected articles from 2009 to 2013 and from 2014 to 2018 for journal type, article access, and PAC involvement. Results: Of the 10,882,681 articles published, 14,202 (0.13%) mentioned the MeSH term ‘rare disease’ in the title or abstract. Nineteen of 20 randomly selected diseases were included in our search results; an independent search for the ‘missing’ disease yielded no articles. Despite a numerical increase over time, there was little change in the proportion of rare disease articles. Most articles were in specialty journals, and ~2/3 were behind paywalls. The majority of rare disease manuscripts were case reports; almost no articles included PACs as authors. Conclusions: The number of high-quality medical publications on rare diseases is not commensurate with their overall prevalence and there are access barriers, highlighting an unmet need in medical literature that would benefit all stakeholders.

摘要背景：可靠和准确的医学文献对罕见病患者（影响全球约4亿人）、其倡导者和护理人员（PAC）以及医疗保健专业人员（HCP）至关重要。方法：我们量化了2009年至2018年PubMed上罕见病英文出版物的数量。为了测试我们的搜索策略，我们评估了20篇随机选择的罕见病文章的收录情况。我们进一步检查了2009年至2013年和2014年至2018年随机选择的100篇文章的期刊类型、文章访问和PAC参与情况。结果：在发表的10882681篇文章中，14202篇（0.13%）在标题或摘要中提到了MeSH术语“罕见病”。在我们的搜索结果中包括了20种随机选择的疾病中的19种；对这种“失踪”疾病的独立搜索没有发现任何文章。尽管数量随着时间的推移而增加，但罕见病文章的比例几乎没有变化。大多数文章发表在专业期刊上，约有2/3的文章发表在付费墙后面。大多数罕见病手稿是病例报告；几乎没有任何文章将PAC作为作者。结论：关于罕见病的高质量医学出版物的数量与其总体流行率不相称，而且存在获取障碍，这突出了医学文献中未满足的需求，这将使所有利益相关者受益。

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引用次数: 3