[CSCO2017]关于肺癌领域的热议话题,听韩宝惠教授与国际大咖怎么说

作者:肿瘤瞭望   日期:2017/10/17 15:24:59  浏览量:27590

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编者按:在不久前召开的2017年CSCO年会上,CSCO-IASLC联合专场聚焦了肺癌领域的热门话题。肺癌靶向治疗药物研究进展迅速,目前临床上有了多个TKI药物可供这些患者选择,讨论如何选用TKI以及TKI的使用顺序非常必要。而免疫疗法也非常有前景,很多临床试验正如火如荼地开展。在今年的CSCO-IASLC联合专场,国内外相关领域的专家针对以上问题进行了讨论。《肿瘤瞭望》邀请了该专场的两位国际讲者——加利福尼亚大学戴维斯综合癌症中心Jonathan W. Riess和马萨诸塞州总医院Justin F. Gainor,与上海市胸科医院韩宝惠教授分别这些热门话题进行深入讨论。

目前已有好几种表皮生长因子受体(EGFR)酪氨酸激酶抑制剂(TKI)上市,包括第一代、二代和三代TKI,如何为EGFR突变肺癌患者选择药物?

Dr. Riess:对于第一代和第二代EGFR-TKI药物厄洛替尼、吉非替尼和阿法替尼,多项临床试验已经证实,对于EGFR突变型晚期非小细胞肺癌(NSCLC),一线EGFR-TKI优于含铂双药化疗,显著提高患者的无进展生存(PFS)。如果第一代和第二代EGFR-TKI治疗后疾病进展,对肿瘤组织进行活检,存在T790M突变的患者可选第三代EGFR-TKI奥希替尼治疗。EGFR突变阳性NSCLC患者的T790M突变概率大约是50%~60%。过去我们认为,如果患者是T790突变阴性,患者只能接受标准化疗或参加其他新药临床试验。但在FLAURA 研究中,奥希替尼一线潜质崭露锋芒,改变了以上观点。很多人会采用奥希替尼作为一线治疗新标准,之后面临的问题是,奥希替尼治疗耐药后怎么办,后续治疗应该是什么?耐药机制不太可能再是T790M。
 
Dr. Gainor:我同意Riess博士的意见。一直以来,我们选择治疗药物是基于药物的活性和安全性。既往我们将靶向药物与化疗对比,现在又进行不同靶向药物之间的头对头试验,研究结果会证明靶向药物的使用顺序。
 
韩宝惠教授:靶向药物在肺癌的应用已经超过了十年。对于第一代EGFR-TKI吉非替尼、厄洛替尼和埃克替尼,无论是单独使用、联合使用,用于一线还是二线治疗,都有了充分的循证医学证据。第二代EGFR-TKI药物有阿法替尼和Dacomitinib,国内上市的阿法替尼为不可逆pan-HER酪氨酸激酶抑制剂,能够对整个ErbB受体家族(酪氨酸激酶受体家族)进行阻滞,而且与EGFR的结合是不可逆的,它用于治疗部分少见或罕见EGFR突变类型可能有优势。2017年的ESMO会议发布了第三代EGFR-TKI奥希替尼对比一代药物的数据,奥希替尼的PFS达到了令人印象深刻的18.9个月。
 
对于EGFR突变型NSCLC的一线治疗,就我们国家而言,常见EGFR突变的患者还是使用一代产品为主,因为一代产品相对来说物美价廉,临床医生已经积累了丰富的经验。第三代产品有很大优势,但价格高昂,目前可能只有小部分患者负担得起,我看好它的未来应用前景。由于一代产品和三代产品的存在,目前二代产品的临床使用面较窄,如果是少见罕见EGFR突变,我个人建议阿法替尼作为首选。
 
靶向TKI治疗是否是驱动基因肿瘤患者的第一选择?如果患者也适合化疗,应怎样安排治疗策略?
 
Dr. Gainor:首先要看患者携带的是哪种致癌基因。例如KRAS突变的肺癌,历经多年研究,目前仍无很好的靶向药物,所以KRAS肺癌的治疗,要么是化疗,要么是最新的免疫疗法。对于EGFR、ALK、ROS1和BRAF基因突变,我们已经研发出能获得高反应率的靶向药物,靶向治疗成为首选。而对于没有基因突变的患者,我们的标准策略是,应用NGS技术检测患者是否携带其他潜在靶点,至少我所在医疗机构是这样。我们认识到,大多数致癌驱动基因都是相互排斥的,所以如果患者有这个突变,就可能没有另一个突变。我们正在对肺癌致癌驱动基因进行精细划分,并基于此对患者进行治疗。
 
Dr. Riess:我的个人观点是,如果靶向药物反应率超过50%,我就会给予患者一线靶向治疗。在美国,EGFR、ALK、ROS1和BRAF,靶向药物疗效已经达到了这个标准。靶向药物在KRAS突变肺癌中的反应率是30%左右,HER2突变者是15%~30%,没达到这个标准,对于这部分患者我会首选化疗。
 
韩宝惠教授:对于EGFR突变患者的一线治疗选择,我们可以参考NCCN指南推荐的变化规律,在NCCN指南中,化疗和TKI曾并驾齐驱。但近些年,NCCN指南渐渐把化疗作为后续治疗的推荐。在中国,靶向药物最近才进入医保,我认为这是一个时间问题,过去受到了靶向药物价格的限制。在循证医学证据方面,一线治疗到底是先用化疗还是先用靶向,从OS上来看,似乎没有明显的优劣之分。但临床医生和患者的倾向是,一线治疗选择高效、低毒、使用方便和物美价廉的药物,对于EGFR敏感突变肺癌患者,靶向药物符合以上标准。我相信未来几年内EGFR-TKI会成为临床一线治疗首选,化疗会退居后线。

携带常见驱动基因突变的肺癌患者接受免疫治疗的效果如何?
 
Dr. Gainor:对于EGFR和ALK阳性肺癌的治疗,在使用免疫疗法之前,应首先最大程度地发挥靶向治疗的作用。因为免疫检查点抑制剂在这部分患者的疗效不佳。但是,即使在EGFR阳性的患者中,仍有一些人能从免疫治疗中受益,虽然概率较低,但我们要对免疫治疗获益的这部分患者进行探索,以指导未来的治疗手段,研发有潜力的组合治疗方案,进一步提高这些人群中的治疗反应率。
 
Dr. Riess:Gainor博士给出了一个很好的总结。我想强调的是,对于驱动基因阳性NSCLC,我的偏好是,首先最大限度地发挥靶向治疗和化疗的疗效,再考虑免疫治疗。即使在我进行免疫治疗时,我也在寻找联合疗法的临床试验。PD-1/PD-L1单药疗法适用于PD-L1高表达、肿瘤突变负荷高的情况,而这种因素在EGFR突变患者通常不存在,我认为联合疗法是最好的选择。
 
韩宝惠教授:我国国家这方面的研究经验较少,需要参考国外的研究和文献。文献报道的高加索人的EGFR基因敏感突变率远远低于亚裔患者。根据免疫治疗在有限的EGFR驱动基因阳性患者中的研究结果,这些患者靶向治疗耐药后使用免疫治疗,其疗效远远低于野生型患者。免疫治疗的疗效与肿瘤突变负荷、PD-L1表达可能密切相关;而驱动基因阳性患者,往往PD-L1表达水平较低,肿瘤突变负荷较低,这就解释免疫治疗效果不佳的原因。所以,驱动基因阳性患者的治疗还是需要二代、三代以及后续EGFR-TKI。
 
应该在哪些领域增大临床试验开展力度,以推动肺癌治疗研究进展?
 
Dr. Riess:我主要谈一谈靶向治疗领域。对于Alectinib、奥希替尼等最新的研究进展,我认为这些药物不仅仅是需要进入一线,它们往往比上一代TKI具有更好的耐受性,还应将其用于一线联合疗法,进行创新,更好地防止患者耐药;开展耐药机制的血浆检测研究,以期早期发现耐药突变。虽然这还需要数年的试验研究。在免疫治疗方面,我认为联合治疗策略可以再一次瞄准潜在的耐药机制,可最大限度地治疗那些难以从单药PD-1疗法中获益的患者。
 
Dr. Gainor:我同意这个观点。目前肺癌领域有很多不同的联合疗法正在研究中,特别是基于免疫疗法的联合方案,我们发现几乎每个药物都在和PD-1/PD-L1抑制剂联合。我们应该开展理性的临床试验,开发能快速评估联合疗法的新型试验设计,加速的有效联合方案的研究,淘汰无用的联合方案。与此同时,对所有的组合方案进行严格的转化科学研究,搞清楚为何某些疗法的组合失败,而另一些组合则能使患者获益。
 
韩宝惠教授:对于中国的肺癌研究,很多专家认为患者数量庞大是我国的优势,但我们还需要加强GCP基础培训,加强临床研究质量控制的培训,使临床研究质量能和国际接轨。尤其在免疫治疗蓬勃兴起的时代,我们应该拿出中国人自己的数据,把好质量关,做好临床设计,从学习模仿到实现赶超和创新。
 
Dr. Reiss and Dr. Gainor’s comments with Oncology Frontier
 
Oncology Frontier: There have been several choices available for EGFR mutation positive lung cancer, including 1st, 2nd, and 3rd generation EGFR-TKIs,how to choose among them? 
 
Dr. Riess: So, previous to just a few weeks ago the management strategy was to start patients off with EGFR activating mutations, in the United States either on erlotin, afatinib, gefitinib, they are first or second-generation EGFR-TKI inhibitors, and they have been studied in multiple clinical trials compared to chemotherapy, and in those trials there was a substantial progression free-survival benefit to the EGFR-TKI patients whose tumors had EGFR activated mutations. And then when they progress, you would do a biopsy and if they were positive to the T790M mutation, which was about 50 to 60% of EGFR mutant non-small cell lung cancer, osimertinib is approved for that indication. and that for T790M positive had about a 60% response rate in a 10-month progression free-survival, so that was the optimal choice. If they were negative for T790M they would either go on a clinical trial or be treated with standard of care chemotherapy, but that’s changed with the new FLAURA study that shows about a PFS benefit of 19 months and a signal of a potential overall survival benefit, so I think many people will adopt first-line osimertinib as the new standard of care for EGFR lung cancer and then the question is what comes after that? Because the resistance mechanisms will shift and will unlikely be T790M. I think Dr. Gainor has some additional thoughts on this as well.
 
Dr. Gainor: I tend to agree. I think historically we made our decisions based on activity and safety profile. And so, historically all of our first and second generations inhibitors were always compared against chemotherapy and we were always doing cross trial comparisons. We’ve now started doing clinical trials comparing EGFR inhibitors and I think that started to uncover what the proper sequence should be. I agree, I think in light of the FLAURA data showing profound improvement in PFS on top of a very favorable side effect profile with osimertinib that will immerge as a new standard of care, at least in first line. And then future questions are going to be what comes next after that.
 
Oncology Frontier: Molecular testing enable us to move from stratified treatment strategy (chemo era) to the precision treatment strategy (onco-target era), does it mean the oncogene specified treatment should always come first while the patient may also be a chemotherapy candidate? Or is there any sequencing strategy?

Dr. Gainor: I think it depends on the oncogene. So for example KRAS lung cancer, KRAS is the most common oncogene in non-small cell lung cancer. We’ve known about it for the longest, yet it is something that we really have been unable to target today with effective targeted therapy. And so for KRAS lung cancer we’ve been stuck with our standard therapies, either chemotherapy or more recently immunotherapy. What we found though for anther oncogenic drivers, EGFR, ALK, ROS1 and BRAF, those are on the oncogenes where we have good targeted therapies that have shown high response rates in either single or even randomized studies depending on oncogene. And for those subsets I think the standard of care right now is to start with targeted therapy. And then for patients who don’t have those specific alterations our current standard of care, at least at my institution, is to perform broad based next generation sequencing to identify additional potential targets. We recognize that most of these oncogenic drivers are mutually exclusive, so if you have one you don’t have the other. And we are trying to carve out smaller and smaller pieces of the pie of the oncogenic drivers in lung cancer.

Dr. Riess: I generally agree with that, with what Dr. Gainor said. My philosophy is if the response rate is more than 50%, I give the front-line targeted therapy. I think in the US, EGFR, ROS1 and ALK, and now BRAF approved and I think I fit that mold.  KRAS fusions have a response rate of targeted therapy as for lung have 30% or so range, HER2 mutations have a response rate at a 15 to 30% to certain targeted therapies; so those types of mutations where we don’t have a targeted therapy that has quite the response rate of an EGFR or ROS1, TKI, I do chemotherapy first. 
 
Oncology Frontier: What’s the role of immunotherapy in oncogene driven lung cancer?
 
Dr. Gainor: So I think it goes back to again what is the oncogene that we are talking about. For EGFR and ALK-positive lung cancers I think in general, immunotherapy should be de-prioritized compared to the targeted therapies, and patients should really should try to maximize and optimize targeted therapy in those patients first, before exploring immuno checkpoint inhibitors. Because today immune checkpoint inhibitors have shown relatively low response rates at no specific molecular subsets. Moving forward we need to do better and try to understand that there are still some patients who derive benefit even among EGFR patients. The frequency is low but we need to identify what is about those patients in order to guide our therapies while also exploring potential combinations to try to improve the response rates in those subsets.
 
Dr. Riess: I think that Dr. Gainor gave a great summary. I would just amplify that for oncogene driven non-small cell lung cancer, my preference is to give immunotherapy later in the course of treatment and to maximize targeted therapy, chemotherapy. Even when I’ve given immunotherapy, I am generally looking for clinical trials with combination therapies. I think single agent PD-1, PD-L1 in the absence of something compelling like very high PD-L1 status, something unusual like a high mutation in EGFR mutant patient which is pretty much non-existent. I think that trials of combinations are the best.
 
Oncology Frontier: What will be the most beneficial and fruitful clinical trials in the new future to fuel the treatment evolution of lung cancer? 
 
Dr. Riess: That is a great question, but a very broad question. To be concise about it, I talked a little bit about in the talk I think targeted therapy, now that we have advances with lung cancer with alectinib, osimertinib and EGFR mutant lung cancer, I think not just bring them up front, but bring them upfront in combination as those drugs tend to be better tolerated than some of the older generation TKI inhibitors. And coming up with those schemes in combination we are heading to bypass tract as well as the on target in innovation and doing it first-line to prevent resistance, I think that will be the next step and you can envision trials that even do something like serial plasma moderate resistance mutations, almost like they do in chronic myeloid leukemia, and the finding the resistance mutations early. But I think that is going to take years of trial to sort out any benefit. But I think that is what he future is going to hold. In terms of immunotherapy I think combination strategy is once again targeting potential resistance mechanisms, maximizing treatment of the patients that hat don’t seem to benefit as much from single agent PD-1 therapy.

Dr. Gainor: Yes, I will agree with that. That one of the major challenges is going to be that we have so many different potential combinations in lung cancer right now, especially around immunotherapies based where we are seeing basically every agent that we have combine with PD-1 inhibitor, and it is up to us to develop more rational clinical trials, to develop novel clinical trial designs where we can rapidly evaluate combinations, move combinations that are promising for faster while also eliminating futile combinations. And I think that is going to be only way to evaluate all of these combinations that reach futility. And I think that is going to be the only way, that we are going to actually be evaluate all these combinations, in parallel with doing so with rigorous translational science so that to understand why certain combinations fail while other are of benefit.

Oncology Frontier: At the upcoming 2017 World Conference on Lung Cancer(WCLC), there will be a pro and con session on “what’s the optimal sequence of ALK-TKI for ALK-positive lung cancer?” In your opinion, is it still a controversial question?
 
Dr. Gainor: Personally, I think that the best data that we have so far is with the ALEXs data showing an upfront treatment with alectinib was superior to crizotinib producing a very impressive progression free-survival around 26 months, and that was similar to what was observe in the ALKs data. So, for me I think that treatment with a more potent penetrant ALK inhibitor, alectinib, first-line looks superior to using sequential crizotinib followed by a second-generation inhibitor. And so that to me, once it achieves regulatory approval, I think should be the new standard of care.   
 
Dr. Riess: I agree, what I presented today I stand by. I was pretty firm that I think alectinib based on magnitude of PFS benefit the CNS activity and tolerability as the first sign standard of care. The details are going to be sorting out what comes next. But I think 26 months vs 11 eleven-month is pretty substantial and I think patients tolerated better and they don’t get, almost 43% of patients on crizotinib had and in the IALSC study had CNS progression within a year and that is devastating for patients. So the longer you can delay that, the better. 
 
Thank you!
 
专家简介
韩宝惠
 
上海市胸科医院副院长、呼吸内科学科带头人,上海市领军人才、优秀学科带头人,博士及博士后导师,医院药物试验管理机构主任,国务院特贴享有者。任中国临床肿瘤协会(CSCO)执行委员,CSCO肿瘤血管靶向专委会主委,中国抗癌协会肺癌专委会委员,中国医师学会肿瘤专委会常委。中华医学生物免疫学会副会长,肿瘤专委会主任委员。上海市医学会肿瘤靶分子专委会副主委,主持及参加数十项国际及国内肺癌新药临床多中心研究,发表200余篇肺癌领域的文章,带教博士、硕士生三十余名。主编:《肿瘤生物免疫靶向治疗》等多部专著;参编专著10余部。获中华医学科技二等奖、第八届中国呼吸医师奖,多次获上海市医学科技二、三等奖。
Jonathan W. Riess
 
加利福尼亚大学戴维斯综合癌症中心内科副教授,曾就职于斯坦福大学医学院、加利福尼亚大学旧金山分校和穆拉戈医院(Mulago Hospital)。
Justin F. Gainor
 
马萨诸塞州总医院,哈佛医学院副教授,哈佛癌症中心和达娜法伯癌症研究所的科学审查委员会委员。美国临床肿瘤学会、国际肺癌研究协会和美国癌症研究协会成员。主要研究领域为肺癌靶向治疗和免疫治疗。

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