- INMARK®試驗結(jié)果已在柳葉刀呼吸醫(yī)學(xué)雜志上發(fā)表1
- 與安慰劑相比���,使用尼達尼布治療12周后�����,并未影響生物標記物--降解C反應(yīng)蛋白的變化率��,但與用力肺活量(FVC)下降率的減少相關(guān)1
- 早期研究表明���,肺功能保持良好的患者與入組時肺功能較差的患者 �����,兩者用力肺活量下降率相當(dāng)����。1
德國殷格翰2019年7月23日 /美通社/ -- 勃林格殷格翰宣布INMARK®試驗結(jié)果已于7月17日在柳葉刀醫(yī)學(xué)雜志上發(fā)表���。INMARK®是一項隨機���、雙盲,在特發(fā)性肺纖維化(IPF)患者中進行的維加特®(尼達尼布)與安慰劑的對照研究(研究持續(xù)12周)���,隨后為40周的開放性研究���,勃林格殷格翰是該試驗的參與方之一。INMARK®試驗是首個在特發(fā)性肺纖維化(IPF)患者中使用抗纖維化治療(尼達尼布)��,研究生物標記物預(yù)測值的的臨床試驗���。研究結(jié)果進一步證明�����,即使在肺功能保持良好的早期IPF患者中���,接受尼達尼布和安慰劑治療12周后����,兩組患者的用力肺活量(FVC)下降值也存在顯著差異���。1,2
IPF是一種罕見但嚴重的�����,具有致命性的肺部疾病��,全球約有300萬人受累�����。3 該疾病可引起肺部瘢痕的不斷加重,導(dǎo)致肺功能持續(xù)且不可逆轉(zhuǎn)的退化以及呼吸困難�����。4由于IPF的不可預(yù)測性以及肺功能喪失的不可逆性��,專家認為患者應(yīng)獲得及時有效的治療。1,5
INMARK®評估了患者從入組到12周后生物標記物 -- 降解C反應(yīng)蛋白的變化率��。降解C反應(yīng)蛋白是一種生物標記物����,之前被證實可預(yù)測特發(fā)性肺纖維化(IPF)患者的死亡率。此外試驗還評估了發(fā)生疾病進展的入組患者比例��,其定義為預(yù)測用力肺活量絕對下降>=10%���,或在52周內(nèi)死亡��。1
與安慰劑相比����,接受尼達尼布治療12周后并未影響生物標記物降解C反應(yīng)蛋白的變化率�,但與用力肺活量下降率的降低有關(guān)1。
29%的入組患者在隨訪52周內(nèi)�����,用力肺活量下降>=10%或死亡��,強調(diào)了特發(fā)性肺纖維化(IPF)疾病進展也存在于用力肺活量≥80%的人群中�。
在12周時間內(nèi)���,與安慰劑組相比,尼達尼布組患者的用力肺活量下降率更低(尼達尼布組為5.9(18.5)ml/12周���,安慰劑組為?70.2(13.1)ml/12周)�。
“即使肺功能維持良好的患者在分別使用尼達尼布與安慰劑治療12周后����,也展現(xiàn)出了用力肺活量下降的明顯差異?���?紤]到特發(fā)性肺纖維化(IPF)的不可預(yù)測性以及肺功能喪失的不可逆性,越來越多的證據(jù)表明盡早治療特發(fā)性肺纖維化(IPF)才是最佳方案���?�!?nbsp;英國倫敦皇家布朗普頓醫(yī)院呼吸內(nèi)科顧問兼該研究的主要研究者托比·馬赫教授評論道���。
勃林格殷格翰呼吸醫(yī)學(xué)副主管Susanne Stowasser博士說道:“生物標記物研究是現(xiàn)代醫(yī)學(xué)的一個關(guān)鍵驅(qū)動力���,對了解健康和疾病狀態(tài)��、診斷���、藥物開發(fā)以及疾病進程或治療效果的預(yù)測都有著巨大的影響����。INMARK是首個在使用抗纖維治療的特發(fā)性肺纖維化(IPF)患者中探索生物標志物預(yù)測值的臨床試驗�����。由于對IPF知之甚少��,多年來生物標志物研究一直是該病的研究熱點����,其主要研究方向是識別疾病預(yù)后的標記物?!彼a充道:“肺纖維化持續(xù)對人們的生活造成毀滅性的影響。勃林格殷格翰致力于諸如INMARK試驗之類的研究�,以便讓我們更好地了解間質(zhì)性肺疾病(如IPF)在個體患者中的進展情況�,并識別出那些可以獲得最佳治療效果的患者?���!?/p>
關(guān)于INMARK®
INMARK®試驗包含347名患者(其中116名使用尼達尼布治療�����,另外231名對照組患者使用安慰劑治療)��,評估從入組到第12周(以ng/mL/月表示)的降解C反應(yīng)蛋白變化率(斜率)�,以及疾病進展的受試者比例�����。疾病進展的定義為在52周內(nèi)FVC預(yù)測值的絕對下降>=10%或死亡�。1
與安慰劑相比,接受尼達尼布治療12周并未影響新表位CRPM血藥濃度的變化率����。1與安慰劑組相比,在12周內(nèi)�����,使用尼達尼布治療的患者的用力肺活量下降率較低�。1在接受安慰劑治療12周的患者中, 12周內(nèi)降解C反應(yīng)蛋白水平的升高與52周內(nèi)疾病進展相關(guān)����。1
此次試驗患者入組時平均用力肺活量預(yù)測值為97.5%,被認為肺容量保持良好���。超過四分之一的患者在52周內(nèi)出現(xiàn)疾病進展(FVC預(yù)測值下降≥10%或死亡)���。1 用力肺活量是一項肺功能測試,用于測量最大程度深呼吸后從肺部用力呼出的空氣量��。5肺功能會隨著特發(fā)性肺纖維化(IPF)的進展而逐步�、不可逆轉(zhuǎn)地惡化,這就是用用力肺活量下降來衡量的���。
關(guān)于維加特(尼達尼布)
尼達尼布(維加特)�,是一種小分子的酪氨酸激酶抑制劑����,由勃林格殷格翰開發(fā)用于治療特發(fā)性肺纖維化(IPF)成人患者。6 2015年�,尼達尼布被納入更新版的特發(fā)性肺纖維化(IPF)國際治療指南。在各種IPF患者類型中�����,維加特均可延緩疾病進展,降低肺功能年下降率達50%����。8-16維加特已在全球超過70個國家及地區(qū)獲批上市用于治療特發(fā)性肺纖維化(IPF)。
References
1. REF TO BE UPDATED WHEN FULL DETAILS AVAILABLE
2. Kolb M, et al. Nintedanib in patients with idiopathic pulmonary fibrosis and preserved lung function. Thorax, 2017; 72(4): 340-346.
3. Ley B, et al. Clinical course and prediction of survival in idiopathic pulmonary fibrosis. Am J Respir Crit Care Med. 2011;183(4):431-40.
4. NHLBI, NIH. What Is Idiopathic Pulmonary Fibrosis? Accessed at: www.nhlbi.nih.gov/health/health-topics/topics/ipf/ Accessed April 2017.
5. Data on file. Boehringer Ingelheim. 2016.
6. Hilberg F, et al. BIBF 1120: triple angiokinase inhibitor with sustained receptor blockade and good antitumor efficacy. Cancer Res. 2008;68:4774-4782.
7. Raghu G, et al. An Official ATS/ERS/JRS/ALAT Clinical Practice Guidelines: Treatment of Idiopathic Pulmonary Fibrosis: Executive Summary. Am J Respir Crit Care Med. 2015; 192(2)238 – 248.
8. OFEV Summary of Product Characteristics. Boehringer lngelheim International GmbH. July 2017.
9. Richeldi L, et al; for the INPULSIS Trial Investigators. Efficacy and safety of nintedanib in idiopathic pulmonary fibrosis. N Eng J Med. 2014;370(22):2071-2082.
10. Kolb M, et al. Nintedanib in patients with idiopathic pulmonary fibrosis and preserved lung volume. Thorax. 2016. doi:l0.1136/thoraxjnl-2016-208710.
11. Raghu G, et al. Effect of nintedanib in subgroups of idiopathic pulmonary fibrosis by diagnostic criteria. Am Journal Respir and Critl Care Med. 2016. doi:l0.1164/rccm.201602-04020C.
12. Cottin V, et al. Effect of baseline emphysema on reduction in FVC decline with nintedanib in the INPULSIS® trials. Abstract presented at: the 18th International Colloquium on Lung and Airway Fibrosis; Mont Tremblant, Canada, September 20-24, 2014.
13. Ryerson CJ, et al. Effect of baseline GAP index stage on decline in lung function with nintedanib in patients with idiopathic pulmonary fibrosis (IPF). Abstract presented at: the lllth American Thoracic Society Conference; San Francisco, California, May 13-18, 2016..
14. Wells A, et al. Effect of baseline composite physiologic index on benefit of nintedanib in IPF. Abstract presented at: the European Respiratory Society International Congress; London, England, September 3-7, 2015.
15. Maher TM, et al. No effect of baseline diffusing capacity of lung for carbon monoxide on benefit of nintedanib. Abstract presented at: the European Respiratory Society International Congress; London, England, September 3-7, 2015.
16. Keating GM. Nintedanib: a review of its use in patients with idiopathic pulmonary fibrosis. Drugs. 2015;75(10):1131-1140.
17. REF TO BE UPDATED WHEN FULL DETAILS AVAILABLE
18. Kolb M, et al. Nintedanib in patients with idiopathic pulmonary fibrosis and preserved lung function. Thorax, 2017; 72(4): 340-346.
19. Ley B, et al. Clinical course and prediction of survival in idiopathic pulmonary fibrosis. Am J Respir Crit Care Med. 2011;183(4):431-40.
20. NHLBI, NIH. What Is Idiopathic Pulmonary Fibrosis? Accessed at: www.nhlbi.nih.gov/health/health-topics/topics/ipf/ Accessed April 2017.
21. Data on file. Boehringer Ingelheim. 2016.
22. Hilberg F, et al. BIBF 1120: triple angiokinase inhibitor with sustained receptor blockade and good antitumor efficacy. Cancer Res. 2008;68:4774-4782.
23. Raghu G, et al. An Official ATS/ERS/JRS/ALAT Clinical Practice Guidelines: Treatment of Idiopathic Pulmonary Fibrosis: Executive Summary. Am J Respir Crit Care Med. 2015; 192(2)238 – 248.
24. OFEV Summary of Product Characteristics. Boehringer lngelheim International GmbH. July 2017.
25. Richeldi L, et al; for the INPULSIS Trial Investigators. Efficacy and safety of nintedanib in idiopathic pulmonary fibrosis. N Eng J Med. 2014;370(22):2071-2082.
26. Kolb M, et al. Nintedanib in patients with idiopathic pulmonary fibrosis and preserved lung volume. Thorax. 2016. doi:l0.1136/thoraxjnl-2016-208710.
27. Raghu G, et al. Effect of nintedanib in subgroups of idiopathic pulmonary fibrosis by diagnostic criteria. Am Journal Respir and Critl Care Med. 2016. doi:l0.1164/rccm.201602-04020C.
28. Cottin V, et al. Effect of baseline emphysema on reduction in FVC decline with nintedanib in the INPULSIS® trials. Abstract presented at: the 18th International Colloquium on Lung and Airway Fibrosis; Mont Tremblant, Canada, September 20-24, 2014.
29. Ryerson CJ, et al. Effect of baseline GAP index stage on decline in lung function with nintedanib in patients with idiopathic pulmonary fibrosis (IPF). Abstract presented at: the lllth American Thoracic Society Conference; San Francisco, California, May 13-18, 2016..
30. Wells A, et al. Effect of baseline composite physiologic index on benefit of nintedanib in IPF. Abstract presented at: the European Respiratory Society International Congress; London, England, September 3-7, 2015.
31. Maher TM, et al. No effect of baseline diffusing capacity of lung for carbon monoxide on benefit of nintedanib. Abstract presented at: the European Respiratory Society International Congress; London, England, September 3-7, 2015.
32. Keating GM. Nintedanib: a review of its use in patients with idiopathic pulmonary fibrosis. Drugs. 2015;75(10):1131-1140.
