摘要PO034:一项长期随访的前瞻性II期临床研究:左炔诺孕酮宫内节育器非手术治疗复杂不典型增生和早期子宫内膜癌

Mikayla Waters, N. Pal, M. Woodall, J. Gallegos, S. Westin, M. Yates
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Further, we propose that estrogen-regulated gene expression biomarkers in the endometrium could reflect differences in estrogen signaling that drive later outcomes. Methods: This study was conducted under an approved IRB protocol at MD Anderson Cancer Center. Follow-up data for complete responders (those without evidence of hyperplasia or cancer following 12 months of LIUD) were abstracted from the medical record to determine long-term outcomes and relapse status (presence of CAH or grade 1 EEC). Estrogen-regulated gene expression biomarkers (PR, EIG121, IGF1, IGF2, RALDH2, survivin) were measured by real-time PCR from baseline endometrial biopsies and compared by relapse status. Results: Follow-up data were available for 30 of 39 participants that experienced complete response with 12 months of treatment with LIUD (median follow-up was 40 months). Eleven of 30 patients (36.7%) with complete response at the end of the 12-month LIUD treatment went on to experience relapse (6/23 with initial diagnosis of CAH and 5/7 g1 EEC). Median time to relapse after complete response was 14.3 months. Relapse occurred in patients with LIUD still in place (n=6) and LIUD removed (n=5). Of 11 cases with relapse, 5 subsequently responded to LIUD (including 3 cases with LIUD previously removed) and 6 went on to have hysterectomy. Two out of 30 (6.7%) complete responders showed progression of their initial g1 EEC lesions following the study: one patient progressed to grade 2 EEC and one patient progressed to grade 2 mixed EEC/clear cell carcinoma. Ten of 30 later had hysterectomy (equally from CAH and g1 EEC cohorts). Finally, although 13/30 patients indicated desired future fertility at baseline, only 3 attempted to conceive, and 1 achieved pregnancy and live birth. 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引用次数: 0

摘要

背景:复杂非典型增生(CAH)和早期子宫内膜样子宫内膜癌(EEC)的发病率正在上升。虽然CAH和EEC的标准前期治疗是子宫切除术,但由于医学合并症或期望的未来生育能力,越来越多的人无法接受子宫切除术,因此需要非手术治疗。我们最近发表的左炔诺孕酮宫内节育器(LIUD) II期试验显示,对CAH或1 (g1)级EEC患者有显著的疗效,在LIUD治疗12个月时总有效率为83%。然而,复发率在大规模前瞻性临床试验人群中尚未得到明确定义。此外,我们提出子宫内膜中雌激素调节的基因表达生物标志物可以反映雌激素信号的差异,从而驱动后期结果。方法:本研究在MD安德森癌症中心按照批准的IRB协议进行。从医疗记录中提取完全应答者(LIUD 12个月后无增生或癌症证据)的随访数据,以确定长期结果和复发状态(CAH或1级EEC的存在)。通过实时荧光定量PCR检测基线子宫内膜活检的雌激素调节基因表达生物标志物(PR、EIG121、IGF1、IGF2、RALDH2、survivin),并与复发状态进行比较。结果:39名参与者中有30名在12个月的LIUD治疗后获得了完全缓解的随访数据(中位随访为40个月)。在12个月的LIUD治疗结束时完全缓解的30例患者中有11例(36.7%)复发(6/23初始诊断为CAH, 5/7初始诊断为EEC)。完全缓解后到复发的中位时间为14.3个月。复发发生在LIUD仍然存在(n=6)和LIUD切除(n=5)的患者中。在11例复发病例中,5例随后对LIUD有反应(其中3例先前已移除LIUD), 6例继续进行子宫切除术。30名完全缓解者中有2名(6.7%)在研究后显示其初始g1级EEC病变进展:1名患者进展为2级EEC, 1名患者进展为2级混合EEC/透明细胞癌。30例中有10例后来进行了子宫切除术(CAH组和EEC组各占1例)。最后,虽然13/30的患者在基线时表示希望将来生育,但只有3人试图怀孕,1人成功怀孕并活产。当比较雌激素调节的基因表达时,表现出复发的参与者的治疗前IGF1低于未复发的参与者(p=0.028)。然而,其他生物标志物在复发状态上没有显著差异。结论:这些发现表明,尽管许多CAH或1级EEC患者最初对LIUD有反应,但这种反应可能不会持久。需要进一步的研究来评估生物标志物,以预测复发风险,并确定改进治疗策略的候选靶点。引文格式:Mikayla Waters, Navdeep Pal, Misty Woodall, Jessica Gallegos, Shannon Westin, Melinda Yates。左炔诺孕酮宫内节育器非手术治疗复杂不典型增生及早期子宫内膜癌的远期随访研究[摘要]。AACR虚拟特别会议论文集:子宫内膜癌:新生物学驱动研究和治疗;2020年11月9-10日。费城(PA): AACR;临床肿瘤杂志,2021;27(3 -增刊):摘要nr PO034。
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Abstract PO034: Long-term follow-up for a prospective phase II trial of levonorgestrel intrauterine device as non-surgical treatment for complex atypical hyperplasia and early endometrial cancer
Background: The incidence of complex atypical hyperplasia (CAH) and early stage endometrioid endometrial cancer (EEC) is increasing. While standard upfront treatment for CAH and EEC is hysterectomy, non-surgical options are needed for the increasing population unable to undergo hysterectomy due to medical comorbidities precluding surgery or desired future fertility. Our recently published phase II trial of levonorgestrel intrauterine device (LIUD) showed substantial response for patients with CAH or grade 1 (g1) EEC, with 83% overall response rate at 12 months of LIUD treatment. Yet, relapse rates have not been well-defined in a large prospective clinical trial population. Further, we propose that estrogen-regulated gene expression biomarkers in the endometrium could reflect differences in estrogen signaling that drive later outcomes. Methods: This study was conducted under an approved IRB protocol at MD Anderson Cancer Center. Follow-up data for complete responders (those without evidence of hyperplasia or cancer following 12 months of LIUD) were abstracted from the medical record to determine long-term outcomes and relapse status (presence of CAH or grade 1 EEC). Estrogen-regulated gene expression biomarkers (PR, EIG121, IGF1, IGF2, RALDH2, survivin) were measured by real-time PCR from baseline endometrial biopsies and compared by relapse status. Results: Follow-up data were available for 30 of 39 participants that experienced complete response with 12 months of treatment with LIUD (median follow-up was 40 months). Eleven of 30 patients (36.7%) with complete response at the end of the 12-month LIUD treatment went on to experience relapse (6/23 with initial diagnosis of CAH and 5/7 g1 EEC). Median time to relapse after complete response was 14.3 months. Relapse occurred in patients with LIUD still in place (n=6) and LIUD removed (n=5). Of 11 cases with relapse, 5 subsequently responded to LIUD (including 3 cases with LIUD previously removed) and 6 went on to have hysterectomy. Two out of 30 (6.7%) complete responders showed progression of their initial g1 EEC lesions following the study: one patient progressed to grade 2 EEC and one patient progressed to grade 2 mixed EEC/clear cell carcinoma. Ten of 30 later had hysterectomy (equally from CAH and g1 EEC cohorts). Finally, although 13/30 patients indicated desired future fertility at baseline, only 3 attempted to conceive, and 1 achieved pregnancy and live birth. When comparing estrogen-regulated gene expression, participants that exhibited relapse had lower pre-treatment IGF1 than those that did not relapse (p=0.028). However, other biomarkers were not significantly different by relapse status. Conclusions: These findings show that although many patients with CAH or grade 1 EEC are initially responsive to LIUD, the response may not be durable. Additional studies are needed to evaluate biomarkers to predict risk of relapse and identify candidate targets for improved therapeutic strategies. Citation Format: Mikayla Waters, Navdeep Pal, Misty Woodall, Jessica Gallegos, Shannon Westin, Melinda Yates. Long-term follow-up for a prospective phase II trial of levonorgestrel intrauterine device as non-surgical treatment for complex atypical hyperplasia and early endometrial cancer [abstract]. In: Proceedings of the AACR Virtual Special Conference: Endometrial Cancer: New Biology Driving Research and Treatment; 2020 Nov 9-10. Philadelphia (PA): AACR; Clin Cancer Res 2021;27(3_Suppl):Abstract nr PO034.
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