新型基于血液或粪便的分子结直肠癌筛查检测的预期影响和成本效益

Projected Impact and Cost-Effectiveness of Novel Molecular Blood-Based or Stool-Based Screening Tests for Colorectal Cancer.

作者信息

Ladabaum Uri, Mannalithara Ajitha, Schoen Robert E, Dominitz Jason A, Lieberman David

机构信息

Division of Gastroenterology and Hepatology and Department of Medicine, Stanford University School of Medicine, Stanford, California (U.L., A.M.).

Division of Gastroenterology, Hepatology and Nutrition, and Department of Epidemiology, University of Pittsburgh, Pittsburgh, Pennsylvania (R.E.S.).

出版信息

Ann Intern Med. 2024 Dec;177(12):1610-1620. doi: 10.7326/ANNALS-24-00910. Epub 2024 Oct 29.

DOI:10.7326/ANNALS-24-00910

PMID:39467291

Abstract

BACKGROUND

Cell-free DNA blood tests (cf-bDNA) and next-generation stool tests could change colorectal cancer (CRC) screening.

OBJECTIVE

To estimate the clinical and economic impacts of novel CRC screening tests.

DESIGN

Cost-effectiveness analysis using MOSAIC (Model of Screening and Surveillance for Colorectal Cancer).

DATA SOURCES

Published data.

TARGET POPULATION

Average-risk persons.

TIME HORIZON

Ages 45 to 100 years.

PERSPECTIVE

Health sector.

INTERVENTION

Novel versus established CRC screening tests.

OUTCOME MEASURES

Incidence and mortality of CRC, quality-adjusted life-years (QALYs), costs.

RESULTS OF BASE-CASE ANALYSIS: For colonoscopy every 10 years, annual fecal immunochemical test (FIT), and triennial next-generation multitarget stool DNA, FIT-RNA, cf-bDNA (Guardant Shield), or cf-bDNA (Freenome), the relative rates (RRs) and 95% uncertainty intervals (UIs) versus no screening for CRC incidence were 0.21 (0.19 to 0.22), 0.29 (0.27 to 0.31), 0.33 (0.32 to 0.36), 0.32 (0.30 to 0.34), 0.58 (0.55 to 0.61) and 0.58 (0.55 to 0.60), respectively; the RRs for CRC death were 0.19 (0.17 to 0.20), 0.25 (0.23 to 0.27), 0.28 (0.27 to 0.30), 0.28 (0.26 to 0.30), 0.44 (0.42 to 0.47), and 0.46 (0.44 to 0.49), respectively. The cf-bDNA test (Shield; list price $1495) cost $89 600 ($74 800 to $102 300) per QALY gained versus no screening; alternatives were less costly and more effective.

RESULTS OF SENSITIVITY ANALYSIS

Incremental costs exceeded incremental benefits when novel test intervals were shortened to 2 or 1 years. The cf-bDNA test matched FIT's impact on CRC mortality at 1.35 (1.30 to 1.40)-fold FIT's uptake rate, assuming equal colonoscopy follow-up. If persons who accept colonoscopy or stool tests shifted to cf-bDNA, CRC deaths increased. This adverse effect was overcome if every 3 such substitutions were counterbalanced by cf-bDNA uptake by 2 or more persons refusing alternatives, assuming equal colonoscopy follow-up.

LIMITATION

Longitudinal test-specific participation patterns are unknown.

CONCLUSION

First-generation cf-bDNA tests may deliver net benefit or harm, depending on the balance between achieving screening in persons who decline alternatives versus substituting cf-bDNA for more effective alternatives.

PRIMARY FUNDING SOURCE

The Gorrindo Family Fund.

摘要

背景

游离DNA血液检测（cf-bDNA）和新一代粪便检测可能会改变结直肠癌（CRC）筛查。

目的

评估新型CRC筛查检测的临床和经济影响。

设计

使用MOSAIC（结直肠癌筛查与监测模型）进行成本效益分析。

数据来源

已发表的数据。

目标人群

平均风险人群。

时间范围

45至100岁。

视角

卫生部门。

干预措施

新型与既定的CRC筛查检测。

结果指标

CRC的发病率和死亡率、质量调整生命年（QALY）、成本。

基础病例分析结果

对于每10年进行一次结肠镜检查、每年进行粪便免疫化学检测（FIT）以及每三年进行一次新一代多靶点粪便DNA、FIT-RNA、cf-bDNA（Guardant Shield）或cf-bDNA（Freenome）检测，与未进行CRC筛查相比，CRC发病率的相对率（RRs）及95%不确定性区间（UIs）分别为0.21（0.19至0.22）、0.29（0.27至0.31）、0.33（0.32至0.36）、0.32（0.30至0.34）、0.58（0.55至0.61）和0.58（0.55至0.60）；CRC死亡的RRs分别为0.19（0.17至0.20）、0.25（可0.23至0.27）、0.28（0.27至0.30）、0.28（0.26至0.30）、0.44（0.42至0.47）和0.46（0.44至0.49）。与未进行筛查相比，cf-bDNA检测（Shield；标价1495美元）每获得一个QALY的成本为89600美元（74800美元至102300美元）；其他检测成本更低且更有效。

敏感性分析结果

当新型检测间隔缩短至2年或1年时，增量成本超过增量效益。假设结肠镜检查随访相同，cf-bDNA检测在FIT采用率为1.35（1.30至1.40）倍时，对CRC死亡率的影响与FIT相当。如果接受结肠镜检查或粪便检测的人转而采用cf-bDNA检测，CRC死亡人数会增加。假设结肠镜检查随访相同，如果每3次这样的替代由2个或更多拒绝其他检测方法的人采用cf-bDNA检测来平衡，这种不利影响可以克服。