Cox Charlotte, Brown Susan, Walpole Euan, Roy Edwige, Dousset Lea, Ladwa Rahul, Khosrotehrani Kiarash
Dermatology Research Centre, Frazer Institute, Experimental Dermatology Group, University of Queensland, Brisbane, Australia.
Department of Dermatology, Princess Alexandra Hospital, Brisbane, Australia.
JAMA Dermatol. 2025 Apr 1;161(4):383-390. doi: 10.1001/jamadermatol.2024.5750.
Therapies for individual keratinocyte carcinomas (KCs) do not prevent the onset of new KCs in a field of sun damage, and therefore the KC burden remains unchanged.
To investigate the association of immune checkpoint inhibitors (ICIs) with changes in field cancerization evaluated by the number of actinic keratoses (AKs) and KCs at baseline compared with 12 months after starting ICI therapy.
DESIGN, SETTING, AND PARTICIPANTS: This prospective cohort study was performed at the outpatient oncology clinic of a single tertiary public hospital in Brisbane, Australia, from April 1, 2022, to November 30, 2023. Consecutive immunocompetent adults starting therapy with an inhibitor for programmed cell death 1 (PD-1) or programmed cell death ligand 1 (PDL-1) for any active cancer, with a planned treatment duration of at least 6 months, and who exhibited clinical AKs on their forearms were eligible. Those with immunosuppression, concurrent chemotherapy or radiotherapy, or recent topical fluorouracil use were excluded.
Intravenous ICI therapy, either PD-1 or PDL-1 inhibitors with or without a cytotoxic T-lymphocyte-associated protein 4 inhibitor, with therapy duration determined by the treating oncologist.
Clinical AKs were counted and photographed before and 3, 6, and 12 months after starting ICI therapy. KC numbers were evaluated based on histopathology reports of all skin lesions excised 12 months before and after starting ICI therapy. Participants' medical history, primary cancer tumor response using Response Evaluation Criteria in Solid Tumors, and adverse events were recorded.
A total of 23 participants were recruited, of whom 17 (73.9%) were male, with a mean (SD) age of 69.7 (9.6) years. No participants withdrew; however, 4 died during the study due to disease progression. The mean (SD) AK number significantly decreased from 47.2 (33.8) at baseline to 14.3 (12.0) at 12 months (P < .001). Younger patients (8 of 12 [66.7%] vs 4 of 12 [33.3%]; P = .007) and those with a history of blistering sunburn (12 of 12 [100%] vs 0; P = .005) were more likely to reduce their AK numbers by 65% or greater. KC total numbers decreased from 42 in the 12 months before starting ICI therapy to 17 in the 12 months after. The number of cutaneous squamous cell carcinomas decreased from 16 to 5 in the same period.
This pilot cohort study found that ICIs used for any cancer were associated with a significant reduction of AKs, suggesting potential as an immunopreventive strategy for high-risk individuals. Given the known effects of other chemopreventive agents on KCs, further investigation into ICIs managing field cancerization is required, especially considering toxicity and cost.
针对单个角质形成细胞癌(KC)的治疗并不能预防日光损伤区域中新的KC的发生,因此KC负担保持不变。
研究免疫检查点抑制剂(ICI)与起始ICI治疗12个月后相比,通过基线时光化性角化病(AK)和KC数量评估的场癌化变化之间的关联。
设计、设置和参与者:这项前瞻性队列研究于2022年4月1日至2023年11月30日在澳大利亚布里斯班一家单一的三级公立医院的门诊肿瘤诊所进行。连续的免疫功能正常的成年人,开始使用程序性细胞死亡蛋白1(PD - 1)或程序性细胞死亡配体1(PDL - 1)抑制剂治疗任何活动性癌症,计划治疗持续时间至少6个月,且前臂有临床AK的患者符合条件。排除有免疫抑制、同时进行化疗或放疗或近期使用局部氟尿嘧啶的患者。
静脉注射ICI治疗,即PD - 1或PDL - 1抑制剂,有或没有细胞毒性T淋巴细胞相关蛋白4抑制剂,治疗持续时间由主治肿瘤学家确定。
在开始ICI治疗前以及治疗后3、6和12个月对临床AK进行计数和拍照。根据开始ICI治疗前后12个月切除的所有皮肤病变的组织病理学报告评估KC数量。记录参与者的病史、使用实体瘤疗效评价标准评估的原发性癌症肿瘤反应以及不良事件。
共招募了23名参与者,其中17名(73.9%)为男性,平均(标准差)年龄为69.7(9.6)岁。没有参与者退出;然而,4名参与者在研究期间因疾病进展死亡。AK的平均(标准差)数量从基线时的47.2(33.8)显著降至12个月时的14.3(12.0)(P <.001)。年龄较小的患者(12名中的8名[66.7%]对12名中的4名[33.3%];P = 0.007)和有晒伤起泡病史的患者(12名中的12名[100%]对0名;P = 0.005)更有可能将其AK数量减少65%或更多。KC总数从开始ICI治疗前的12个月内切除的42个降至治疗后的12个月内的17个。同期皮肤鳞状细胞癌的数量从16个降至5个。
这项初步队列研究发现,用于任何癌症的ICI与AK的显著减少相关,这表明其作为高危个体免疫预防策略的潜力。鉴于其他化学预防剂对KC的已知作用,需要进一步研究ICI对场癌化的管理,特别是考虑到毒性和成本。
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