Castelli C, Storkus W J, Maeurer M J, Martin D M, Huang E C, Pramanik B N, Nagabhushan T L, Parmiani G, Lotze M T
Istituto Nazionale Tumori, Milan, Italy.
J Exp Med. 1995 Jan 1;181(1):363-8. doi: 10.1084/jem.181.1.363.
We and others have previously reported that melanoma-specific, cytotoxic T lymphocytes (CTL) define a minimum of six class I-presented peptide epitopes common to most HLA-A2+ melanomas. Here we show that three of these peptide epitopes are coordinately recognized by a CTL clone obtained by limiting dilution from the peripheral blood of an HLA-A2+ melanoma patient. Tandem mass spectrometry was used to characterize and sequence one of these three naturally processed melanoma peptides. One of the potential forms of the deduced peptide sequence (XXTVXXGVX, X = I or L) matches positions 32-40 of the recently identified melanoma gene MART-1/Melan-A. This peptide (p939; ILTVILGVL) binds to HLA-A2 with an intermediate-to-low affinity and is capable of sensitizing the HLA-A2+ T2 cell line to lysis by CTL lines and clones derived from five different melanoma patients. A relative high frequency of anti-p939-specific effector cells appear to be present in situ in HLA-A2+ melanoma patients, since p939 is also recognized by freshly isolated tumor infiltrating lymphocytes. p939 represents a good candidate for the development of peptide-based immunotherapies for the treatment of patients with melanoma.
我们和其他研究人员之前曾报道,黑色素瘤特异性细胞毒性T淋巴细胞(CTL)至少可识别大多数HLA - A2 +黑色素瘤共有的6种I类呈递肽表位。在此我们表明,通过对一名HLA - A2 +黑色素瘤患者外周血进行有限稀释获得的一个CTL克隆可协同识别其中三种肽表位。采用串联质谱对这三种天然加工的黑色素瘤肽之一进行表征和测序。推导的肽序列的一种潜在形式(XXTVXXGVX,X = I或L)与最近鉴定的黑色素瘤基因MART - 1 / Melan - A的第32 - 40位氨基酸匹配。该肽(p939;ILTVILGVL)以中低亲和力与HLA - A2结合,并且能够使HLA - A2 + T2细胞系对来自五名不同黑色素瘤患者的CTL系和克隆介导的裂解敏感。由于新鲜分离的肿瘤浸润淋巴细胞也能识别p939,因此在HLA - A2 +黑色素瘤患者体内似乎存在相对高频的抗p939特异性效应细胞。p939是开发用于治疗黑色素瘤患者的基于肽的免疫疗法的良好候选物。
