Dendritic cells loaded with killed allogeneic melanoma cells can induce objective clinical responses and MART-1 specific CD8+ T-cell immunity.

Palucka AK; Ueno H; Connolly J; Kerneis Norvell F; Blanck JP; Johnston DA; Fay J; Banchereau J

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Dendritic cells loaded with killed allogeneic melanoma cells can induce objective clinical responses and MART-1 specific CD8+ T-cell immunity.

机译：负载有杀死的异源黑色素瘤细胞的树突状细胞可以诱导客观的临床反应和MART-1特异性CD8 + T细胞免疫。

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Dendritic cells (DCs) loaded with killed allogeneic tumors can cross-prime tumor-specific naive CD8 T cells in vitro, thereby providing an option to overcome human leukocyte antigen restriction inherent to loading DC vaccines with peptides. We have vaccinated 20 patients with stage IV melanoma with autologous monocyte-derived DCs loaded with killed allogeneic Colo829 melanoma cell line. DCs were generated by culturing monocytes with granulocyte macrophage-colony stimulating factor (granulocyte macrophage-colony stimulating factor) and interleukin (IL-4) and activated by additional culture with tumor necrosis factor and CD40 ligand. A total of 8 vaccines were administered at monthly intervals. The first patient was accrued December 2002 and the last November 2003. Fourteen patients were alive at 12 months, 9 patients were alive at 24 months, and 8 patients are alive as of January 2006. The estimated median overall survival is 22.5 months with a range of 2 to 35.5 months. Vaccinations were safe and tolerable. They induced, in 2 patients who failed previous therapy, durable objective clinical responses, 1 complete regression (CR) and 1 partial regression (PR) lasting 18 and 23 months, respectively. Three out of 13 analyzed patients showed T-cell immunity to melanoma antigen recognized by autologous T cells (MART-1) tissue differentiation antigen. Two of 3 patients showed improved immune function after vaccinations demonstrated by improved secretion of interferon (IFN)-gamma or T-cell proliferation in response to MART-1 derived peptides. In one of these patients, vaccination led to elicitation of CD8 T-cell immunity specific to a novel peptide-derived from MART-1 antigen, suggesting that cross-priming/presentation of melanoma antigens by DC vaccine had occurred. Thus, the present results justify the design of larger follow-up studies to assess the clinical response to DC vaccines loaded with killed allogeneic tumor cells in patients with metastatic melanoma.

机译：负载了被杀死的同种异体肿瘤的树突状细胞（DC）可以在体外交叉引发肿瘤特异性幼稚CD8 T细胞，从而提供了一种克服DC疫苗中肽固有的人类白细胞抗原限制的选择。我们已经为20例IV期黑色素瘤患者接种了自体单核细胞衍生的DC，并装载了已杀死的同种异体Colo829黑色素瘤细胞系。 DCs是通过将单核细胞与粒细胞巨噬细胞集落刺激因子（粒细胞巨噬细胞集落刺激因子）和白介素（IL-4）一起培养而产生的，并通过与肿瘤坏死因子和CD40配体的额外培养而被激活。每月间隔共接种8种疫苗。第一名患者于2002年12月和2003年11月获得。截至2006年1月，有14例患者在12个月时还活着，有9例患者在24个月时还活着，有8例患者还活着。估计的总生存期中位数为22.5个月2至35.5个月。接种疫苗是安全且可以忍受的。他们在2名先前治疗失败的患者中诱发了持久的客观临床反应，分别持续18个月和23个月的1次完全消退（CR）和1次部分消退（PR）。在13位分析的患者中，有3位显示T细胞对自体T细胞（MART-1）组织分化抗原识别的黑色素瘤抗原具有免疫力。 3名患者中有2名在接种疫苗后表现出免疫功能改善，这是由于对MART-1衍生肽的应答增加了干扰素（IFN）-γ或T细胞的分泌所致。在其中一名患者中，接种疫苗可引发对源自MART-1抗原的新型肽特异的CD8 T细胞免疫，这表明DC疫苗已发生交叉引发/呈递黑色素瘤抗原。因此，本结果证明进行较大规模的随访研究的设计是合理的，以评估转移性黑素瘤患者对负载灭活的同种异体肿瘤细胞的DC疫苗的临床反应。

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来源
《Journal of immunotherapy 》 |2006年第5期| 共13页
作者
Palucka AK; Ueno H; Connolly J; Kerneis Norvell F; Blanck JP; Johnston DA; Fay J; Banchereau J;
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正文语种 eng
中图分类治疗学 ;
关键词
T-Lymphocytes; allogeneic; month; Melanoma; T淋巴细胞; 黑色素瘤;

机译：T-Lymphocytes;allogeneic;month;Melanoma;T淋巴细胞;黑色素瘤;

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专利

1. Dendritic cells loaded with killed allogeneic melanoma cells can induce objective clinical responses and MART-1 specific CD8+ T-cell immunity. [J] . Palucka AK, Ueno H, Connolly J, Journal of immunotherapy . 2006 ,第5期

机译：负载有杀死的异源黑色素瘤细胞的树突状细胞可以诱导客观的临床反应和MART-1特异性CD8 + T细胞免疫。
2. Cross-priming of cyclin B1, MUC-1 and survivin-specific CD8+ T cells by dendritic cells loaded with killed allogeneic breast cancer cells [J] . Hiroaki Saito, Peter Dubsky, Carole Dantin, Breast Cancer Research . 2006 ,第6期

机译：载有被杀死的同种异体乳腺癌细胞的树突状细胞对细胞周期蛋白B1，MUC-1和survivin特异性CD8 + T细胞的交叉引发
3. CD8+ T-cells suppress antigen-specific and allogeneic CD4+ T-cell responses to herpes simplex virus type 2-infected human dendritic cells. [J] . Nordstrom I, Nurkkala M, Collins LV, Viral immunology . 2005 ,第4期

机译：CD8 + T细胞抑制抗原特异性和同种异体CD4 + T细胞对单纯疱疹病毒2型感染的人树突状细胞的应答。
4. Mechanisms of Inhibition of Human Allergic Th2 Immune Responses by Regulatory T-Cells Induced by Interleukln 10-Treated Dendritic Cells and Transforming Growth Factor beta [C] . I. Bellinghausen, B. Konig, I. Bottcher, Collegium Internationale Allergologicum . 2007

机译：通过白细胞uck10-处理的树突细胞和转化生长因子β诱导的调节T细胞抑制人过敏Th2免疫应答的机制，转化生长因子β
5. The role of CD8+ T cells in the regulation of recipient immune responses induced by allogeneic platelet transfusions [D] . Sterling, Katherine. 2004

机译：CD8 + T细胞在同种异体血小板输注诱导的受体免疫应答调节中的作用
6. Monocyte-derived dendritic cells loaded with a mixture of apoptoticecrotic melanoma cells efficiently cross-present gp100 and MART-1 antigens to specific CD8+ T lymphocytes [O] . Erika M von Euw, María M Barrio, David Furman, 2007

机译：单核细胞衍生的树突状细胞载有凋亡/坏死性黑色素瘤细胞混合物可有效地将gp100和MART-1抗原交叉呈递至特定CD8 + T淋巴细胞
7. Monocyte-derived dendritic cells loaded with a mixture of apoptotic/necrotic melanoma cells efficiently cross-present gp100 and MART-1 antigens to specific CD8+ T lymphocytes [O] . Erika M von Euw, María M Barrio, David Furman, 2007

机译：单核细胞衍生的树突状细胞载有凋亡/坏死性黑色素瘤细胞混合物，可有效地将gp100和MART-1抗原交叉呈递至特定CD8 + T淋巴细胞

Dendritic cells loaded with killed allogeneic melanoma cells can induce objective clinical responses and MART-1 specific CD8+ T-cell immunity.

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