Natali P G, Hamby C V, Felding-Habermann B, Liang B, Nicotra M R, Di Filippo F, Giannarelli D, Temponi M, Ferrone S
Department of Immunology, Regina Elena Cancer Institute, Rome, Italy.
Cancer Res. 1997 Apr 15;57(8):1554-60.
Several lines of experimental evidence in in vitro and animal model systems suggest that the integrin alpha(v)beta3 plays a role in the tumorigenicity of human melanoma cells and that the blocking of alpha(v)beta3 ligand binding can inhibit tumor progression. However, there is only scanty information about the role of alpha(v)beta3 in malignant melanoma in a clinical setting. Therefore, in the present study, we have analyzed the distribution in lesions of melanocyte origin and in normal tissues of the alpha(v) integrin subunit and of the alpha(v)beta3 complex and their association with histopathological and clinical parameters of malignant melanoma. We have used as probes the monoclonal antibodies (mAbs) TP36.1 and VF27.263.15, which we have shown with a combination of serological and immunochemical assays to be specific for the alpha(v) subunit and for the alpha(v)beta3 complex, respectively. In immunohistochemical assays, mAb TP36.1 stained both benign and malignant lesions of melanocyte origin. In contrast, the reactivity of mAb VF27.263.15 was restricted to malignant lesions. Both mAbs displayed differential reactivity with primary melanoma lesions of different histotypes because they stained about 50% of acral lentiginous melanoma and superficial spreading melanoma lesions, at least 80% of nodular melanoma lesions, and none of the uveal melanoma lesions tested. Both mAbs TP36.1 and VF27.263.15 stained about 60% of lymph node metastases and 80% of cutaneous metastases. Expression of the alpha(v)beta3 complex in melanocytic lesions resembles that of intercellular adhesion molecule-1 (ICAM-1) in several respects: (a) both are expressed in a significantly (P < 0.004) larger proportion of malignant than of benign lesions; (b) expression of both molecules in primary melanoma lesions is significantly (P < 0.05) associated with lesion thickness; and (c) expression of both molecules in primary lesions from patients with stage I melanoma is significantly (P < 0.05) associated with an increased probability of disease recurrence following surgical excision. alpha(v)beta3 and ICAM-1 in primary melanoma lesions complement each other in predicting the outcome of the disease, because the association with prognosis was enhanced when primary lesions were stained by both anti-alpha(v)beta3 mAb VF27.263.15 and anti-ICAM-1 mAb CL203.4 or by neither mAb. Because alpha(v)beta3 has been suggested as a potential target of immunotherapy, its distribution in normal tissues was investigated. alpha(v)beta3 expression is restricted because it was only detected in ductal epithelium of parotid glands, thyrocytes, basal glands of the stomach, colonic and rectal epithelium glomeruli, Bowman's capsules and proximal and distal tubules of kidneys, and endometrial epithelium. These findings suggest that renal function will be a critical clinical parameter to monitor in therapies of malignant diseases relying on systemic administration of anti-alpha(v)beta3 mAb.
体外实验证据以及动物模型系统中的多项实验证据表明,整合素α(v)β3在人类黑色素瘤细胞的致瘤性中发挥作用,并且阻断α(v)β3配体结合可抑制肿瘤进展。然而,关于α(v)β3在临床环境中恶性黑色素瘤中的作用,仅有少量信息。因此,在本研究中,我们分析了α(v)整合素亚基和α(v)β3复合物在黑素细胞起源的病变以及正常组织中的分布情况,及其与恶性黑色素瘤的组织病理学和临床参数的关联。我们使用单克隆抗体(mAb)TP36.1和VF27.263.15作为探针,通过血清学和免疫化学分析相结合的方法,我们已证明它们分别对α(v)亚基和α(v)β3复合物具有特异性。在免疫组织化学分析中,mAb TP36.1对黑素细胞起源的良性和恶性病变均有染色。相比之下,mAb VF27.263.15的反应性仅限于恶性病变。两种单克隆抗体对不同组织学类型的原发性黑色素瘤病变表现出不同的反应性,因为它们对约50%的肢端雀斑样痣黑色素瘤和浅表扩散性黑色素瘤病变、至少80%的结节性黑色素瘤病变进行了染色,而对所检测的葡萄膜黑色素瘤病变均未染色。mAb TP36.1和VF27.263.15均对约60%的淋巴结转移灶和80%的皮肤转移灶进行了染色。黑素细胞病变中α(v)β3复合物的表达在几个方面类似于细胞间黏附分子-1(ICAM-1):(a)两者在恶性病变中表达的比例均显著(P < 0.004)高于良性病变;(b)两种分子在原发性黑色素瘤病变中的表达均与病变厚度显著(P < 0.05)相关;(c)I期黑色素瘤患者原发性病变中两种分子的表达均与手术切除后疾病复发概率增加显著(P < 0.05)相关。原发性黑色素瘤病变中的α(v)β3和ICAM-1在预测疾病转归方面相互补充,因为当原发性病变同时用抗α(v)β3单克隆抗体VF27.263.15和抗ICAM-1单克隆抗体CL203.4染色或均未用这两种单克隆抗体染色时,与预后的关联会增强。由于α(v)β3已被认为是免疫治疗的潜在靶点,因此对其在正常组织中的分布进行了研究。α(v)β3的表达受限,因为仅在腮腺导管上皮、甲状腺细胞、胃底腺、结肠和直肠上皮、肾小球、鲍曼囊以及肾近端和远端小管以及子宫内膜上皮中检测到。这些发现表明,在依赖抗α(v)β3单克隆抗体全身给药的恶性疾病治疗中,肾功能将是一个关键的临床监测参数。
