NEJM: PD-1单抗对多种癌症有极好

波士顿(EGMN)——在经过一系列加速函数调用的实体病变当中，近1/4对名为BMS-936558的新型免疫细胞膜药物有；也，大多病变的；也持续超过1年。第一原作者、约翰霍普金斯大学乳癌项目副校长Suzanne Topalian耶鲁大学在美国临床研究工作常务理事(ASCO)大会的新闻官网上介绍：“该药物的一个显著特性是，它对其他病人无效的病变仍可可借不止非常持久的；也。

BMS-936558是一种抗击病毒，可切断活化T细胞膜较厚的程序性丧命(PD)-1受体。通过依赖性PD-1和PD-1羰基(PD-L 1)通路可无法挽回过剩的T细胞膜，加强抗击免疫细胞膜力。Topalian耶鲁大学及其同事招募了296举例放弃1~5种病人后显现不止结核病成效的转移性乳癌、结直肠胰脏、非小细胞膜肺胰脏、胰脏或脾胰脏等病变，对其每2周静脉注射1.0、3.0或10 mg/kg增重的BMS-936558，最多病人2年。

结果表明，在这项Ⅰ期检验当中，236举例放弃评估的病变的普遍性；也(假设为完全恢复或明显大多恢复)率为18%~28%。28%的乳癌病变显现不止普遍性；也，脾细胞膜胰脏病变为27%，二者当中分别有6%和27%简报援引中风平稳。结直肠胰脏和胰腺胰脏病变当中未显现不止；也。仅有31举例病变在将近1年前显现不止；也，其当中20举例；也持续时间约达1年以上。

对肺胰脏具有临床研究工作活性也是BMS-936558的最主要特性，因为始终以来肺胰脏都对免疫细胞膜药物耐药。在这项检验当中，肺胰脏病变的普遍性；也率为18%，7%中风平稳约达到24周或以上。除此以外，55%的病变此前已放弃了将近前三线药物。虽然由于病变数量少而须认真解读该研究工作数据，但BMS-936558看来对突起细胞膜更加有效，；也率为33%，而对非突起细胞膜的；也率为12%。

对42份函数调用标本顺利进行免疫细胞膜组化分析的结果上会，PD-L1表约达可能带入病人；也的一种标志物。在所有25举例PD-L1阳性病变当中，9举例造成了了普遍性；也，而在17举例PD-L1阴性病变当中无1举例造成了普遍性；也(P=0.006)。

Topalian援引，在所有296举例病变当中，14%辨别到轻微病症。他将在ASCO大会上简报这项研究工作的结果。最常见的所致血案为疲劳、皮疹、头痛、尘症、恶心、食欲或血红蛋白下滑，以及发热。3 /4级病人相关性所致血案在各剂量组当中均完全相同，除了结核病之外均有白癜风、细菌性、肝尘、轴突尘和甲状腺尘。尽管已采取了20世纪比对、积极病人结核病这一病人病症的更加佳紧急措施，但仍有3举例病变应结核病而丧命。

Topalian耶鲁大学援引，上述结果使BMS-936558都是其他免疫细胞膜药物，如伊匹嘌呤，后者对转移性乳癌的；也率为10%~15%，然而同时也有20%~30%的病变显现不止临床研究工作显著毒性。BMS-936558最终将可能带入主力药物，或与其他免疫细胞膜药物或靶向病人共同作为成效期结核病的主力药物。她声援引，一项评价伊匹嘌呤与BMS-936558联合病人的检验正在纪念斯隆-凯特林胰脏症当为中心顺利进行。目前还计划在非小细胞膜肺胰脏、乳癌和脾细胞膜胰脏病变当中积极参与Ⅲ期检验。

这项20世纪检验同时刊不止在《弗吉尼亚医学杂志》上(N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200690])，同期刊不止的另一项有关PD-L1切断的研究工作断定了相比之下的；也率和所致血案发生率(N. Engl. J. Med. 2012 [doi:10.1056/NEJMoa1200694])。马里兰大学免疫细胞膜项目副校长Antoni Ribas耶鲁大学在随刊概述当中声援引，这2项初步研究工作共同声称，切断PD-1或PD-L1有可能带入免疫细胞膜药物抗击活性的新基准(doi:10.1056/NEJMe1205943)。

这项研究工作取得了百时美-施贵宝、Ono制药的支持，并从国立卫生研究工作院和乳癌研究工作三巨头取得红利。Topalian耶鲁大学还简报援引为百时美-施贵宝和Amplimmune提供咨询，其合著者简报援引与百时美-施贵宝有利益关系。Ribas耶鲁大学简报援引无纠纷。

零碎史籍:

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.