NEJM: PD-1单抗对多种胃癌有良好

纽约市(EGMN)——在经过一系列大幅提高预处理的也就是说病患中会，近1/4对叫作BMS-936558的新型免疫治疗有转发，其余部分病患的转发接下来多达1年。第一所作、约翰霍普金斯大学阿兹海默工程项目副校长Suzanne Topalian哈佛大学在宾夕法尼亚州临床学会(ASCO)年会的报导发布讲话介绍：“该治疗的一个值得注意特点是，它对其他病患无效的病患仍可诱导借助于非常越来越为重要的转发。

BMS-936558是一种单克隆抑止体，可绕过酪氨酸T细胞内颗粒的程序性丧生(PD)-1受体。通过抑制PD-1和PD-1阳离子(PD-L 1)通路可挽救耗竭的T细胞内，增强抑止免疫力。Topalian哈佛大学及其同事招揽了296由此可知放弃1~5种病患后借助于现传染病十分困难的转移性阿兹海默、常为直肠肿瘤、非小细胞内肺肿瘤、肿瘤或消化道肿瘤等病患，对其每2周肌肉注射1.0、3.0或10 mg/kg体重的BMS-936558，最多病患2年。

常为果显示，在这项Ⅰ期检验中会，236由此可知放弃指标的病患的普遍性转发(定义为完全恢复或明显其余部分恢复)率为18%~28%。28%的阿兹海默病患借助于现普遍性转发，消化道细胞内肿瘤病患为27%，二者中会分别有6%和27%份文件援引病情平衡。常为直肠肿瘤和肝肿瘤病患中会未借助于现转发。共有31由此可知病患在非常少1早先借助于现转发，其中会20由此可知转发接下来时间达1年以上。

对肺肿瘤具有临床活性也是BMS-936558的一大特点，因为仍然以来肺肿瘤都对免疫治疗脑膜凝。在这项检验中会，肺肿瘤病患的普遍性转发率为18%，7%病情平衡降至24周或以上。除此以外，55%的病患在此之后已放弃了非常少前一环治疗。虽然由于病患生产量少而须谨慎解读该科学研究数据集，但BMS-936558似乎对粒状细胞内越来越有效，转发率为33%，而对非粒状细胞内的转发率为12%。

对42份预处理新种进行免疫组化分析的常为果查看，PD-L1暗示可能会视作病患转发的一种标志物。在所有25由此可知PD-L1感染性病患中会，9由此可知产生了普遍性转发，而在17由此可知PD-L1阴性病患中会无1由此可知产生普遍性转发(P=0.006)。

Topalian援引，在所有296由此可知病患中会，14%仔细观察到严重抑止抑郁药。他将在ASCO年讲话份文件这项科学研究的常为果。最常见的所致暴力事件为憔悴、皮疹、腹泻、瘙痒、恶心、荷尔蒙或人体内急剧下降，以及发热。3 /4级病患相关性所致暴力事件在各药物组中会均相似，除了肺凝外则有白癜风、常为肠凝、乙型肝凝、垂体凝和甲状腺凝。尽管已作出了后期辨认、鼓励病患肺凝这一病患抑止抑郁药的充份措施，但仍有3由此可知病患应肺凝而丧生。

Topalian哈佛大学援引，上述常为果使BMS-936558都是以其他免疫治疗，如伊匹单抑止，后者对转移性阿兹海默的转发率为10%~15%，然而同时也有20%~30%的病患借助于现临床值得注意毒性。BMS-936558终究将可能会视作主力药物，或与其他免疫治疗或靶向病患一同作为十分困难期传染病的主力治疗。她指借助于，一项评论伊匹单抑止与BMS-936558联合病患的检验正在缅怀斯隆-凯特林肿瘤症中会心进行。现有还计划在非小细胞内肺肿瘤、阿兹海默和消化道细胞内肿瘤病患中会开展Ⅲ期检验。

这项后期检验同时刊登在《缅因州医学杂志》上(N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200690])，同期刊登的另一项有关PD-L1绕过的科学研究得借助于了略低的转发率和所致暴力事件比率(N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200694])。加州大学洛杉矶分校免疫工程项目副校长Antoni Ribas哈佛大学在随刊简述中会指借助于，这2项可行性科学研究一同确实，绕过PD-1或PD-L1有可能会视作免疫治疗抑止活性的新原则上(doi:10.1056/NEJMe1205943)。

这项科学研究取得了百时美-施贵宝、Ono制药的全力支持，并从国立卫生科学科技学院和阿兹海默科学研究该联盟取得补助金。Topalian哈佛大学还份文件援引为百时美-施贵宝和Amplimmune发放建议，其月出版者份文件援引与百时美-施贵宝有公共利益关系。Ribas哈佛大学份文件援引无公共利益冲突。

原始文献:

Brahmer JR, Safety and Activity of Anti-PD-L1 Antibody in Patients with Advanced Cancer.N Engl J Med. 2012 Jun 2.

Topalian SL,et al.Safety, Activity, and Immune Correlates of Anti-PD-1 Antibody in Cancer. N Engl J Med. 2012 Jun 2

Ribas A.Tumor Immunotherapy Directed at PD-1. N Engl J Med. 2012 Jun 2.

CHICAGO (EGMN) – Nearly one-quarter of patients with a range of heily pretreated solid tumors responded to a new immunotherapy called BMS-936558, with some responses persisting for more than 1 year.

“One of the remarkable features about this therapy is that it can induce very durable responses in patients with otherwise treatment-refractory disease,” lead author Dr. Suzanne Topalian said at a press briefing at the annual meeting of the American Society of Clinical Oncology.

BMS-936558 is a monoclonal antibody that blocks the programmed death (PD)-1 receptor on the surface of activated T cells. Inhibition of the PD-1 and the PD-1 ligand (PD-L1) pathway rescues exhausted T-cells and enhances anti-tumor immunity.

When tested in the phase I trial, objective responses, defined as complete regression or significant partial regression, were reported in 18%-28% of 236 evaluable patients.

Serious side effects were observed in 14% of the 296 patients in the entire cohort, said Dr. Topalian, who will present the results at the ASCO meeting.

This sets BMS-936558 apart from other immunotherapies such as ipilimumab, which results in response rates of 10%-15% in metastatic melanoma but also clinically significant toxic effects in 20%-30% of patients.

Three treatment-related deaths occurred as a result of pneumonitis or lung inflammation, although better methods he been developed for aggressive treatment and early recognition of patients at risk for this side effect, she said.

BMS-936558 is also unique in that it was clinically active in lung cancer, which historically has been resistant to immunotherapy. In this subset, the objective response rate was 18%, with 7% achieving stable disease lasting 24 weeks or more. Notably, 55% of patients had received at least three prior lines of therapy, said Dr. Topalian, director of the melanoma program and professor of surgery and oncology at Johns Hopkins University in Baltimore.

“It’s a remarkable result; it’s something we didn’t expect to see,” she said in an interview. “I’ve been in the field of cancer immunotherapy since 1985 and this was a genuine surprise.”

Although the data should be interpreted with caution because of the small patient numbers, BMS-936558 appears to be more beneficial in squamous tumors, for which the response rate was 33%, compared with 12% among nonsquamous tumors, she added.

The results represent years of basic science and proof-of-concept that targeting the PD-1 pathway is valuable in cancer therapy. The early phase trial is generating enough excitement to be simultaneously published in the New England Journal of Medicine (N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200690]), along with a second study involving PD-L1 blockade that reported slightly lower response and adverse event rates (N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200694]).

Taken together, “these initial observations suggest that antibodies blocking PD-1 or PD-L1 are likely to provide a new benchmark for antitumor activity in immunotherapy,” wrote Dr. Antoni Ribas in an editorial accompanying the two studies (doi:10.1056/NEJMe1205943).

Dr. Topalian and her associates administered BMS-936558 at doses of 1.0, 3.0, or 10 mg/kg of body weight as an intrenous infusion every 2 weeks for up to 2 years in 296 patients with metastatic melanoma, colorectal, non–small-cell lung cancer, prostate, and renal cancer that had progressed after at least one and up to five previous therapies.

Objective responses were observed in 28% of patients with melanoma and 27% with renal cell cancer, with stable disease reported in 6% and 27%, respectively. Patients with colon and pancreatic cancer did not he tumor responses, Dr. Topalian said.

Overall, 31 patients had a response that occurred at least 1 year ago and, of these, 20 responses persisted for more than 1 year.

The most common adverse events were fatigue, rash, diarrhea, pruritus, nausea, decreased appetite or hemoglobin, and pyrexia. Grade 3/4 treatment-related adverse events were similar across all doses, and included vitiligo, colitis, hepatitis, hypophysitis, and thyroiditis in addition to pneumonitis.

Ultimately, BMS-936558 may be used first line or in combination with other immunotherapies or targeted therapies in advanced disease, Dr. Topalian said.

“There may be rational ways to combine these agents, that by themselves he limitations, but when combined with PD-1 blockade there is a synergistic effect,” she said. “And there is laboratory evidence to suggest that certain kinds of combinations can be synergistic.”

A trial evaluating the combination of ipilimumab and BMS-936558 is already underway at Memorial Sloan Kettering Cancer Center, she observed. Phase III trials also are being planned in non–small-cell lung cancer, melanoma, and renal cell cancer.

Finally, an immunohistochemical ysis performed on 42 pretreatment tumor specimens suggests that PD-L1 expression could serve as a potential marker of treatment response. In all, 9 of 25 patients with PD-L1–positive tumors had an objective response, compared with no objective responses among 17 patients with PD-L1–negative tumors (P value = .006).

In his editorial, Dr. Ribas, director of the tumor immunology program at the University of California, Los Angeles, Jonsson Comprehensive Cancer Center, remarked: “The use of PD-1 blockade – with its reduced rate of toxic effects and potential ability to further select patients who he increased likelihood of tumor response – may well he a major effect on cancer treatment.”

The study was supported by Bristol-Myers Squibb, Ono Pharmaceuticals, and grants from the National Institutes of Health and the Melanoma Research Alliance. Dr. Topalian also reported consulting for BMS and Amplimmune, and her coauthors reported financial relationships with BMS, including stock ownership, employment, and leadership positions. Dr. Ribas reported no relevant conflicts of interest.