慢性鼻-鼻窦炎
表型
医学
鼻窦炎
炎症
免疫学
生物
遗传学
基因
作者
A. V. Chufistova,Е. В. Шабалдина,А. В. Бедарева,I N Vakhrameev,N.A. Abramova,А. В. Шабалдин
出处
期刊:Vestnik otorinolaringologii
[Media Sphere Publishing Group]
日期:2024-01-01
卷期号:89 (4): 60-60
标识
DOI:10.17116/otorino20248904160
摘要
Recently, significant progress has been made in identifying the cellular and molecular mechanisms responsible for the pathogenesis of chronic rhinosinusitis (CRS). Cohort studies of CRS have led to advances in the clinical understanding of this disease. New therapeutic agents have been approved or are undergoing clinical trials to expand treatment options for this disease. One of the promising areas in medicine is the provision of personalized clinical care. From this perspective, CRS can be divided into three different endotypes depending on the type of underlying inflammatory response. In the United States, CRS with and without nasal polyps is predominantly characterized as the second inflammatory endotype. CRS with nasal polyps (about 17%) and without nasal polyps (up to 20%) belongs to the 1st and 3rd inflammatory endotypes, respectively. And if for the second inflammatory endotype the effectiveness of targeted biological therapy is beyond doubt, then for the first and third inflammatory endotypes the principles of such conservative therapy are under active development. Moreover, large validated studies to confirm associations between CRS phenotypes and endotypes, as well as to find effective biological markers of inflammatory endotypes, remain to be performed.
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