同步和异步黑色素瘤转移中黑色素瘤分化抗原的一致性缺失:对免疫治疗的影响。
Concordant loss of melanoma differentiation antigens in synchronous and asynchronous melanoma metastases: implications for immunotherapy.
作者信息
Trefzer Uwe, Hofmann Maja, Reinke Susanne, Guo Ya-Jun, Audring Heike, Spagnoli Giulio, Sterry Wolfram
机构信息
Department of Dermatology and Allergy, Skin Cancer Centre, Charité-Universitätsmedizin Berlin, Berlin, Germany.
出版信息
Melanoma Res. 2006 Apr;16(2):137-45. doi: 10.1097/01.cmr.0000200489.55099.20.
Because of its known heterogeneity, the analysis of antigen expression is crucial prior to the initiation of antigen-specific immunotherapy for melanoma. The melanoma differentiation antigens gp100, MART-1 and tyrosinase are involved in a common pathway of melanin synthesis. Peptides derived from these melanoma differentiation antigens are used in the immunotherapy of melanoma and antibodies recognizing these antigens are commonly applied to detect melanocytic lesions. One hundred and ninety-one paraffin-embedded melanoma metastases from 28 patients with 2-19 lesions (mean, 6.8) developing synchronously (n = 67) or asynchronously (n = 124) were analysed by immunohistochemistry for the expression of the melanoma differentiation antigens, as well as cancer/testis antigens of the melanoma antigen-A (MAGE-A) family (monoclonal antibodies 77B and 57B), anti-S100 and SM5-1. The overall reactivities were 81.6% (gp100), 79.5% (MART-1), 59.6% (tyrosinase), 59.1% (77B), 60.7% (57B), 93.2% (S100) and 91.6% (SM5-1). Twenty-seven lesions (14.1%) were positive for all tumour-associated antigens, 75 lesions (39.2%) were negative for one antigen and 87 lesions (45.5%) were negative for several tumour-associated antigens. Co-ordinated loss was found for lesions negative for gp100 and MART-1 (9.4%, P < 0.0005), gp100 and tyrosinase (11.0%, P = 0.009), MART-1 and tyrosinase (15.2%, P < 0.0005) and gp100, MART-1 and tyrosinase (8.9%, P < 0.0005), which is up to six times higher than the expected calculated loss. This co-ordinated loss of melanoma differentiation antigens in melanoma did not include cancer testis antigens and S100 or SM5-1. On average, the melanoma differentiation antigens stained 50-65% of cells within a lesion, and 10-39% of synchronous clusters were heterogeneous for melanoma differentiation antigen expression. In conclusion, broader polypeptide vaccines should be used for melanoma immunotherapy.
由于黑色素瘤具有已知的异质性,因此在启动黑色素瘤抗原特异性免疫治疗之前,分析抗原表达至关重要。黑色素瘤分化抗原gp100、MART-1和酪氨酸酶参与黑色素合成的共同途径。源自这些黑色素瘤分化抗原的肽被用于黑色素瘤的免疫治疗,识别这些抗原的抗体通常用于检测黑素细胞病变。通过免疫组织化学分析了28例患者的191个石蜡包埋的黑色素瘤转移灶,这些转移灶有2 - 19个病变(平均6.8个),病变同步发生(n = 67)或异步发生(n = 124),检测黑色素瘤分化抗原以及黑色素瘤抗原-A(MAGE-A)家族的癌胚抗原(单克隆抗体77B和57B)、抗S100和SM5-1的表达。总体反应率分别为81.6%(gp100)、79.5%(MART-1)、59.6%(酪氨酸酶)、59.1%(77B)、60.7%(57B)、93.2%(S100)和91.6%(SM5-1)。27个病变(14.1%)对所有肿瘤相关抗原呈阳性,75个病变(39.2%)对一种抗原呈阴性,87个病变(45.5%)对几种肿瘤相关抗原呈阴性。发现gp100和MART-1阴性的病变(9.4%,P < 0.0005)、gp100和酪氨酸酶阴性的病变(11.0%,P = 0.009)、MART-1和酪氨酸酶阴性的病变(15.2%,P < 0.0005)以及gp100、MART-1和酪氨酸酶阴性的病变(8.9%,P < 0.0005)存在协同缺失,这比预期计算的缺失高出多达六倍。黑色素瘤中黑色素瘤分化抗原的这种协同缺失不包括癌胚抗原以及S100或SM5-1。平均而言,黑色素瘤分化抗原在一个病变内染色50 - 65%的细胞,10 - 39%的同步簇在黑色素瘤分化抗原表达方面存在异质性。总之,应使用更广泛的多肽疫苗进行黑色素瘤免疫治疗。
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