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[医学前沿] 宾夕法尼亚大学CAR-T的最新成果

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发表于 2014-12-10 09:30:44 | 显示全部楼层 |阅读模式 来自: 中国北京
本帖最后由 橙色雨丝 于 2014-12-10 10:20 编辑

Penn Medicine Researchers Announce Latest Results of Investigational Cellular Therapy CTL019Findings Include Response Rates Over 90 Percent in Pediatric Acute Lymphoblastic Leukemia, and First Results of Non-Hodgkin Lymphoma Trial
SAN FRANCISCO – The latest results of clinical trials of more than 125 patients testing an investigational personalized cellular therapy known as CTL019 will be presented by a University of Pennsylvania research team at the 56th American Society of Hematology Annual Meeting and Exposition. Highlights of the new trial results will include a response rate of more than 90 percent among pediatric acute lymphoblastic leukemia patients, and results from the first lymphoma trials testing the approach, including a 100 percent response rate among follicular lymphoma patients and 45 percent response rate among those with diffuse large B-cell lymphoma.

“We have now treated more than 125 patients in our trials of the chimeric antigen receptor (CAR) therapy CTL019, and with each patient, we learn more and more about the potential of this therapy,” said the research team’s leader, Carl June, MD, the Richard W. Vague Professor in Immunotherapy in the department of Pathology and Laboratory Medicine in Penn’s Perelman School of Medicine, and director of Translational Research in the Abramson Cancer Center. “We are continuing to refine our approach to ensure the best outcomes for patients who may be eligible for this experimental therapy, and we hope our findings will contribute to the emerging field of cellular therapy as a whole.”
This personalized cellular therapy approach begins with patients’ own immune cells, collected through a procedure similar to dialysis. The cells are then engineered in a laboratory and infused back into patients’ bodies after being trained to hunt and kill their cancer cells. All patients who enroll in the trials have cancers that have progressed despite multiple conventional therapies.

Updated results of a CTL019 trial for children and young adults with relapsed, treatment-resistant acute lymphocytic leukemia who were treated at the Children’s Hospital of Philadelphia (Abstract #380) includes data on 39 patients.  The findings, which will be presented by Stephan Grupp, MD, PhD, the Yetta Deitch Novotny Professor of Pediatrics and director of Translational Research in the Center for Childhood Cancer Research at the Children's Hospital of Philadelphia, build on the team’s report on 25 pediatric and five adult patients which was published in the New England Journal of Medicine in October.
Thirty six of 39 children (92 percent) achieved a complete response (CR) after receiving an infusion of the modified cells. After a median follow-up of six months, more than two-thirds (70 percent) of children who responded remained in remission and 75 percent were alive, including the first patient to receive the therapy, in the spring of 2012. These results were achieved with only 3 of the patients going on to receive stem cell transplant while in remission.

All pediatric patients who responded to the therapy experienced a cytokine release syndrome (CRS) within a few days after receiving their infusions – a key indicator that the engineered cells have begun proliferating and killing tumor cells in the body, but also a known potentially lethal type of toxicity. Patients who experience a CRS typically have varying degrees of flu-like symptoms, with high fevers, nausea, muscle pain, and sometimes, low blood pressure and breathing difficulties. Some patients require treatment with anti-cytokine agents and steroids to manage these symptoms.
The research team will also report the first results of a CTL019 study of patients with relapsed or refractory non-Hodgkin lymphomas (NHL) (Abstract #3087). In patients with follicular lymphoma (FL) or diffuse large B cell lymphoma (DLBCL) who received infusions of CTL019, assessments at three months after treatment revealed that all five FL patients (100 percent) and five out of 11 DLBCL patients (45 percent) responded to the therapy, including complete responses in four patients (80 percent) with FL and four patients (36 percent) with DLBCL. All patients who received infusions developed varying degrees of CRS. The longest complete response durations are ongoing, at 8.8 months for DLBCL and 7.4 months for FL; all other responses continue, as well. The findings will be presented by Jakub Svoboda, MD, an assistant professor of Medicine in the Abramson Cancer Center, on behalf of the Lymphoma Program under the leadership of the study’s principal investigator, Stephen J. Schuster, MD, the Robert and Margarita Louis-Dreyfus Associate Professor of Chronic Lymphocytic Leukemia and Lymphoma.

In updated results of the Penn research team’s Phase II dose optimization study of patients with chronic lymphocytic leukemia (CLL) who were treated with CTL019 (Abstract #1982), 10 out of 24  (42 percent) patients responded to the cellular therapy. Of those, five (21 percent) had complete responses, and five (21 percent) had partial responses. After a median follow-up of nine months, overall survival was 68 percent. Eleven patients, including five who responded to the therapy, experienced a cytokine release syndrome (CRS), though the severity of CRS did not correlate with response.
Patients in this trial were randomized to receive two different doses of modified cells. The findings revealed no association between with the amount of cells and greater toxicities, but the researchers say it is still unclear if the amount of cells will affect the response of CLL to CTL019. These results will be presented by David Porter, MD, the Jodi Fisher Horowitz Professor in Leukemia Care Excellence and director of Blood and Marrow Transplantation in Penn’s Abramson Cancer Center.

The Penn researchers will also report on three adult ALL patients who died due to refractory CRS within several weeks after receiving infusions of CTL019 (Abstract #2296). These patients were found to have significant concomitant infections: one patient had influenza, a second patient had pseudomonas sepsis and pneumonia, and a third patient had stenotrophomonas sepsis. These significant concomitant infections may have exacerbated the CRS. These findings will be presented by Noelle Frey, MD, MSCE, an assistant professor of Medicine in the Abramson Cancer Center. A companion abstract (Abstract #1983) also presented by Dr. Porter outlines a novel CRS grading system, developed from data on the first 125 patients to receive CTL019, to better identify CRS severity and more accurately guide timing of medication and other therapies to care for patients who develop this side effect. Results from all trials of CTL019 indicate that CRS tends to be most severe among ALL patients with the highest tumor burden.
In July 2014, the U.S. Food and Drug Administration granted CTL019 its Breakthrough Therapy designation for the treatment of relapsed and refractory adult and pediatric ALL, a step which is intended to expedite the development and review of new medicines that treat serious or life-threatening conditions, if a therapy has demonstrated substantial advantages over available treatments. CTL019 is the first personalized cellular therapy to receive the designation.

The research was supported by the National Institutes of Health (R01CA165206, R01CA102646 and R01CA116660), multi-year research funding under The Leukemia & Lymphoma Society’s Specialized Centers of Research grant program, and a Stand Up To Cancer-St. Baldrick’s Pediatric Dream Team Translational Research Grant.

Editor’s note: The University of Pennsylvania has licensed technologies involved in this trial to Novartis. Some of the scientists involved in these trials are inventors of these technologies, including Drs. June and Porter (collectively, the “Penn Inventors”), and Dr. Grupp (“CHOP Inventor”). As a result of Penn-Novartis licensing relationship, the University of Pennsylvania receives significant financial benefit and the Penn Inventors have benefitted financially.  It is possible that in the future, the University of Pennsylvania, The Children's Hospital of Philadelphia (CHOP), the Penn Inventors, and the CHOP Inventor may benefit financially.

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博学多才一生平安康复0-1年

 楼主| 发表于 2014-12-10 10:14:36 | 显示全部楼层 来自: 中国北京
病理会诊:专家看切片
本帖最后由 橙色雨丝 于 2014-12-10 10:27 编辑

1)美国宾夕法尼亚大学的研究小组宣布将在第56届美国血液学协会年会上公布关于CTL019临床试验的详细结果。
2)超过125位患者参加了这个临床试验,CAR-T疗法分别在儿童急性淋巴细胞白血病,滤泡性淋巴瘤和弥漫大B淋巴瘤上取得了90%,100%和45%的有效率。
3)对于复发难治型的儿童ALL,39位病人中有36位获得了CR,六个月后有70%仍处于缓解中,包括于2012年春季收治的5位病人,其中仅有3位进行了移植。
4)参加试验的复发难治型滤泡性淋巴瘤和弥漫大B淋巴瘤病人分别有5位和11位,3个月后的评估表明CR率分别为80%和36%,这些病人仍在持续缓解中。
5)对于CLL即慢性淋巴细胞白血病患者,响应率为42%,CR率为21%。
6)大部分患者在治疗过程中经历了CRS即细胞因子风暴,CRS的严重程度似乎与回注细胞的数量和最终的疗效无关,少数死亡的患者与治疗时存在的感染以及高肿瘤负荷有关。
7)宾夕法尼亚大学是公认的在CART技术上处在世界最前沿的机构之一,其研究成果应该可以代表目前该技术所能够达到的高度。

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模范家属一生平安

发表于 2014-12-10 11:13:42 来自手机 | 显示全部楼层 来自: 中国北京
橙色雨丝 发表于 2014-12-10 10:14
1)美国宾夕法尼亚大学的研究小组宣布将在第56届美国血液学协会年会上公布关于CTL019临床试验的详细结果。
...

我昨天得到了另外两组关于弥漫大b的数据,其实还是挺打击人的,不知道是不是因为大b病灶的特殊性,或者活性太高抗原极易改变,算了,不看数据看疗效吧!
原发胃部弥漫大B,非生发中心,7个R-CHOP、1个DICE、2个GEMOX、来那度胺+CEPP全口服方案、CAR-T治疗后缓解。

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博学多才一生平安家人平安康复1-3年

发表于 2014-12-10 14:15:37 | 显示全部楼层 来自: 中国北京
英文的就不要发了吧 ,哈哈哈

感谢中文
2010年老爸离世  2011年确诊癌症  2012年离婚失去了家庭   2013年的我开始了正常的工作和生活  2014年顺利度过!2015年终于见到了儿子!2016年一切顺利,平安度过!2017年我收获最大!2018年要更加开心的活着!
只要我活着,就会有希望!--有些事不是看到了希望才去坚持,而是因为坚持了才会看到希望!

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一生平安家人平安康复0-1年康复1-3年博学多才

发表于 2014-12-10 14:27:59 | 显示全部楼层 来自: 中国北京
乐山乐水 发表于 2014-12-10 11:13
我昨天得到了另外两组关于弥漫大b的数据,其实还是挺打击人的,不知道是不是因为大b病灶的特殊性,或者活 ...

还在摸索阶段,需要过程!希望是有滴!大家要有信心!

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发表于 2014-12-11 12:37:01 来自手机 | 显示全部楼层 来自: 中国四川广元
本帖最后由 春秋三十三 于 2014-12-11 12:39 编辑
乐山乐水 发表于 2014-12-10 11:13
我昨天得到了另外两组关于弥漫大b的数据,其实还是挺打击人的,不知道是不是因为大b病灶的特殊性,或者活 ...


数据是怎么样的?大B发展快,肿瘤负荷会比较高。且抗原不稳定。多靶点的CART出来后应该会比较好的。

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一生平安康复0-1年

发表于 2014-12-13 08:57:57 | 显示全部楼层 来自: 中国四川成都
成就令人鼓舞,问题总会克服,肿瘤治疗思路很多,百花齐放最好,现在这枝夺目

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一生平安

发表于 2014-12-19 17:54:37 来自手机 | 显示全部楼层 来自: 中国北京
靠 大b真是无语了 但是毕竟接近50%也不低了
一个普通人

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发表于 2014-12-19 21:01:43 来自手机 | 显示全部楼层 来自: 中国黑龙江七台河
乐山乐水 发表于 2014-12-10 11:13
我昨天得到了另外两组关于弥漫大b的数据,其实还是挺打击人的,不知道是不是因为大b病灶的特殊性,或者活 ...

你家做了cart么?进展的怎么样了?我哥哥也打算做呢

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