肢端型黑色素瘤组织中MITF的表达及其与临床、病理学特征及预后的相关性研究

doi:10.19401/j.cnki.1007-3639.2025.09.006

摘要/Abstract

摘要：

背景与目的： 小眼畸形相关转录因子（microphthalmia-associated transcription factor，MITF）在黑色素瘤的发生、发展过程中发挥着复杂的多层次调控作用。已有大量关于MITF的研究在皮肤型黑色素瘤（cutaneous melanoma，CM）中进行，但MITF在肢端型黑色素瘤（acral melanoma，AM）中的研究却十分有限。本研究回顾性分析AM患者的MITF表达情况与临床、病理学特征及预后的相关性，为患者的预后评估和个体化治疗方案制订提供依据。方法： 本研究纳入2008年3月—2022年2月在复旦大学附属肿瘤医院进行原发灶切除，术后病理学检查诊断为恶性黑色素瘤的患者，取得患者手术切除标本制成组织芯片（tissue microarray，TMA）。本研究获复旦大学附属肿瘤医院医学伦理委员会批准（伦理编号：2203-ZZK-69-3）。从复旦大学附属肿瘤医院电子数据库中查阅患者的基本信息、临床、病理学特征，整理出与组织芯片孔位逐一对应的患者信息总表。切取完整的组织芯片进行免疫组织化学（immunohistochemistry，IHC）染色，由3名病理科医师独立在显微镜下进行阅片，评估MITF的表达情况。依据MITF表达水平对患者进行分层，统计分析两组患者的临床、病理学特征及预后的差异。结果： 共纳入137例AM患者。MITF表达水平与T分期、N分期、美国癌症联合会（American Joint Committee on Cancer，AJCC）分期、Clark分级、前哨淋巴结、溃疡有关。调整混杂因素后进行多因素分析，结果显示，N分期和溃疡是MITF高表达的独立危险因素。生存分析显示，MITF高表达或更高的T分期预示着更短的无病生存期（disease-free survival，DFS）。MITF高表达患者的总生存期（overall survival，OS）在术后观察或细胞因子治疗组与辅助免疫检查点抑制剂（immune checkpoint inhibitor，ICI）治疗组间并无显著差异，而MITF低表达的患者能够从辅助ICI治疗中显著获益。结论： 较高的N分期或合并溃疡预示着AM患者的肿瘤细胞内MITF呈高表达，而高表达MITF是疾病早期出现复发、转移甚至死亡的危险信号。此外，MITF低表达的患者可以从术后辅助ICI治疗中获益。MITF不仅可以辅助黑色素瘤的诊断，还能够为临床预后评估和个体化治疗方案的制订提供依据。

关键词: 肢端型黑色素瘤, 组织芯片, 小眼畸形相关转录因子, 临床、病理学特征, 预后, 治疗

Abstract:

Background and purpose: The microphthalmia-associated transcription factor (MITF) plays a complex role in melanoma pathogenesis and progression. It is known to regulate multiple processes both in melanocytes and melanoma cells. While numerous studies have explored MITF in cutaneous melanoma (CM), research in acral melanoma (AM) is still limited. This study retrospectively analyzed the correlation between MITF expression and clinical, pathological characteristics and prognosis in AM patients, providing a basis for prognosis evaluation and personalized treatment plan formulation for patients. Methods: Patients who underwent primary resection of AM at Fudan University Shanghai Cancer Center from March 2008 to February 2022 were included. All surgical samples were diagnosed by clinical histopathology and used to construct the tissue microarray (TMA). This study was approved by the medical ethics committee of Fudan University Shanghai Cancer Center (approval number: 2203-ZZK-69-3). Cutting complete tissue microarray and evaluating MITF expression levels by immunohistochemistry (IHC) staining were carried out. The results were independently assessed and scored by three pathologists. Clinical and pathological data were collected from the hospital’s electronic medical record system, and each patient’s data was matched to their corresponding tissue sample on the chip. Patients were stratified into two groups based on MITF expression levels. Statistical analyses were performed to assess differences in clinical, pathological characteristics and survival outcomes between these two groups. Results: A total of 137 AM patients were included. MITF expression was significantly associated with T stage, N stage, American Joint Committee on Cancer (AJCC) stage, clark level, sentinel lymph node status, and presence of ulceration. Among these, N stage and ulceration were independent risk factors for high expression of MITF after adjusting for confounding factors. Survival analysis showed that AM patients with high MITF expression or higher T stage were associated with shorter disease-free survival (DFS). Patients with high MITF expression showed no significant difference in overall survival (OS) between observation or cytokine therapy and adjuvant immune checkpoint inhibitor (ICI) therapy, whereas those with low MITF expression derived significant survival benefits from ICI treatment. Conclusion: A higher N stage or the presence of ulceration indicates high MITF expression in tumor cells, with high MITF levels serving as a warning signal for early recurrence, metastasis, and even death. Patients with low MITF expression could receive improved OS with early adjuvant ICI therapy. MITF could not only serve as an auxiliary diagnostic marker for melanoma but also provide a basis for clinical prognosis assessment and the formulation of personalized treatment plans.

Key words: Acral melanoma, Tissue microarray, Microphthalmia-associated transcription factor, Clinical, pathological characteristics, Prognosis, Treatment

中图分类号:

R739.5

王彤, 孙伟, 徐宇, 胡涂, 刘琬琳, 郑琼丹, 邹孜瑊, 董子瑞, 马文杰, 陈勇. 肢端型黑色素瘤组织中MITF的表达及其与临床、病理学特征及预后的相关性研究[J]. 中国癌症杂志, 2025, 35(9): 859-866.

WANG Tong, SUN Wei, XU Yu, HU Tu, LIU Wanlin, ZHENG Qiongdan, ZOU Zijian, DONG Zirui, MA Wenjie, CHEN Yong. MITF expression in acral melanoma tissues and its association with clinical, pathological characteristics and prognosis[J]. China Oncology, 2025, 35(9): 859-866.

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Characteristic	MITF-low (n=82)	MITF-high (n=55)	Pearson χ²	P value	Characteristic	MITF-low (n=82)	MITF-high (n=55)	Pearson χ²	P value
Gender			0.029	0.864	Ⅳ	52 (63.41)	27 (49.09)
Male	45 (54.88)	31 (56.36)			Ⅴ	13 (15.85)	21 (38.18)
Female	37 (45.12)	24 (43.64)			Unknown	5 (6.10)	3 (5.45)
Age at diagnosis/year			3.387	0.066	SLN			10.793	0.001
≤60	26 (31.71)	26 (47.27)			Positive	16 (19.51)	20 (36.36)
>60	56 (68.29)	29 (52.73)			Negative	50 (60.98)	15 (27.27)
T stage			9.459	0.024	Unknown	16 (19.51)	20 (36.36)
T1	11 (13.41)	1 (1.82)			Ulceration			7.583	0.006
T2	14 (17.07)	5 (9.09)			Positive	34 (41.46)	36 (65.45)
T3	27 (32.93)	18 (32.73)			Negative	48 (58.54)	19 (34.55)
T4	30 (36.59)	31 (56.36)			Location			0.532	0.466
N stage			21.937	<0.001	Upper extremity	6 (7.32)	6 (10.91)
N0	55 (67.07)	16 (29.09)			Lower extremity	76 (92.68)	49 (89.09)
N1	13 (15.85)	14 (25.45)			Histology			2.198	0.532
N2	10 (12.20)	12 (21.82)			ALM	52 (63.41)	34 (61.82)
N3	4 (4.88)	13 (23.64)			NM	3 (3.66)	4 (7.27)
AJCC Stage			21.42	<0.001	SSM	2 (2.44)	0 (0.00)
Ⅰ	20 (24.39)	2 (3.64)			Unknown	25 (30.49)	17 (30.91)
Ⅱ	35 (42.68)	14 (25.45)			Adjuvant therapy			12.463	0.006
Ⅲ	27 (32.93)	39 (70.91)			PD-1 inhibitors	22 (26.83)	27 (49.09)
Clark level			12.531	0.006	Cytokines	29 (35.37)	6 (10.91)
Ⅱ	7 (8.54)	0 (0.00)			Observation	24 (29.27)	18 (32.73)
Ⅲ	5 (6.10)	4 (7.27)			Unknown	7 (8.54)	4 (7.27)

Characteristic	Univariate analysis			Multivariate analysis
Characteristic	OR	95% CI	P value	OR	95% CI	P value
Gender	1.062	0.534-2.113	0.864
Age at diagnosis	0.518	0.256-1.048	0.067
T stage	1.872	1.234-2.841	0.003	1.116	0.618-2.018	0.716
N stage	2.168	1.520-3.096	<0.001	1.893	1.281-2.795	0.001
AJCC Stage	4.183	2.040-6.746	<0.001
Clark level	2.418	1.336-4.380	0.004	1.473	0.703-3.083	0.305
SLN	4.166	1.737-9.994	0.001
Ulceration	2.901	1.420-5.930	0.003	2.907	1.239-6.814	0.014

Characteristic	Univariate analysis			Multivariate analysis
Characteristic	HR	95% CI	P value	HR	95% CI	P value
MITF by IHC	1.844	1.048-3.246	0.034	2.415	1.093-5.337	0.029
Gender	1.991	1.120-3.539	0.019	1.750	0.773-3.961	0.179
Age at diagnosis	0.784	0.453-1.358	0.389
T stage	1.777	1.237-2.553	0.002	1.974	1.083-3.599	0.026
N stage	1.195	0.930-1.534	0.163
Clark level	1.416	0.886-2.264	0.146	0.854	0.403-1.807	0.679
SLN	1.390	0.713-2.710	0.333	1.503	0.700-3.226	0.296
Ulceration	0.630	0.663-1.972	0.630
Adjuvant therapy	1.261	0.704-2.261	0.436	1.253	0.565-2.776	0.579