Comer Brian S, Ba Mariam, Singer Cherie A, Gerthoffer William T
Department of Biochemistry and Molecular Biology, University of South Alabama, Mobile, AL, 36688, USA.
Department of Pharmacology, University of Nevada School of Medicine, Reno, NV 89557, USA.
Pharmacol Ther. 2015 Mar;147:91-110. doi: 10.1016/j.pharmthera.2014.11.006. Epub 2014 Nov 15.
In spite of substantial advances in defining the immunobiology and function of structural cells in lung diseases there is still insufficient knowledge to develop fundamentally new classes of drugs to treat many lung diseases. For example, there is a compelling need for new therapeutic approaches to address severe persistent asthma that is insensitive to inhaled corticosteroids. Although the prevalence of steroid-resistant asthma is 5-10%, severe asthmatics require a disproportionate level of health care spending and constitute a majority of fatal asthma episodes. None of the established drug therapies including long-acting beta agonists or inhaled corticosteroids reverse established airway remodeling. Obstructive airways remodeling in patients with chronic obstructive pulmonary disease (COPD), restrictive remodeling in idiopathic pulmonary fibrosis (IPF) and occlusive vascular remodeling in pulmonary hypertension are similarly unresponsive to current drug therapy. Therefore, drugs are needed to achieve long-acting suppression and reversal of pathological airway and vascular remodeling. Novel drug classes are emerging from advances in epigenetics. Novel mechanisms are emerging by which cells adapt to environmental cues, which include changes in DNA methylation, histone modifications and regulation of transcription and translation by noncoding RNAs. In this review we will summarize current epigenetic approaches being applied to preclinical drug development addressing important therapeutic challenges in lung diseases. These challenges are being addressed by advances in lung delivery of oligonucleotides and small molecules that modify the histone code, DNA methylation patterns and miRNA function.
尽管在界定肺部疾病中结构细胞的免疫生物学和功能方面取得了重大进展,但对于开发治疗多种肺部疾病的全新药物类别,仍缺乏足够的认识。例如,迫切需要新的治疗方法来应对对吸入性糖皮质激素不敏感的重度持续性哮喘。尽管激素抵抗性哮喘的患病率为5%至10%,但重度哮喘患者需要不成比例的医疗保健支出,且占致命哮喘发作的大多数。包括长效β受体激动剂或吸入性糖皮质激素在内的现有药物疗法,均无法逆转已形成的气道重塑。慢性阻塞性肺疾病(COPD)患者的阻塞性气道重塑、特发性肺纤维化(IPF)中的限制性重塑以及肺动脉高压中的闭塞性血管重塑,同样对当前药物治疗无反应。因此,需要药物来实现对病理性气道和血管重塑的长效抑制和逆转。表观遗传学的进展催生出了新的药物类别。细胞适应环境信号的新机制正在出现,其中包括DNA甲基化的变化、组蛋白修饰以及非编码RNA对转录和翻译的调控。在本综述中,我们将总结目前应用于临床前药物开发的表观遗传学方法,这些方法应对了肺部疾病中的重要治疗挑战。寡核苷酸和小分子的肺部递送进展正在解决这些挑战,这些寡核苷酸和小分子可改变组蛋白编码、DNA甲基化模式和miRNA功能。