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. 2021 Aug 17;4(8):e2121403. doi: 10.1001/jamanetworkopen.2021.21403

Estimated Cost-effectiveness of Endoscopic Screening for Upper Gastrointestinal Tract Cancer in High-Risk Areas in China

Ruyi Xia 1, Hongmei Zeng 2, Wenjun Liu 1, Li Xie 1, Mingwang Shen 1, Peng Li 1, He Li 2, Wenqiang Wei 2, Wanqing Chen 2,, Guihua Zhuang 1,
PMCID: PMC8371571  PMID: 34402889

This economic evaluation assesses the cost-effectiveness of endoscopic screening for esophageal and gastric cancers in a hypothetical cohort of individuals aged 40 to 69 years in areas of China where the risk of upper gastrointestinal tract cancer is high.

Key Points

Question

Is endoscopic screening for esophageal and gastric cancers cost-effective in areas of China where the risk of these cancers is high?

Findings

In this model-based economic evaluation of a hypothetical closed cohort of 100 000 individuals aged 40 to 69 years from areas of China where the risk of upper gastrointestinal tract cancer is high, 5 endoscopic screening strategies with different frequencies had an incremental cost-effectiveness ratio of less than the per capita gross domestic product in China for each quality-adjusted life-year gained compared with no screening. Screening every 2 years would be the most cost-effective strategy.

Meaning

These findings suggest that combined endoscopic screening for esophageal cancer and gastric cancer would be cost-effective in areas of China where the risk of these cancers is high and that screening every 2 years would be the optimal strategy.

Abstract

Importance

Upper gastrointestinal tract cancer, including esophageal and gastric cancers, in China accounts for 50% of the global burden. Endoscopic screening may be associated with a decreased incidence of and mortality from upper gastrointestinal tract cancer.

Objective

To evaluate the cost-effectiveness of endoscopic screening for esophageal and gastric cancers among people aged 40 to 69 years in areas of China where the risk of these cancers is high.

Design, Setting, and Participants

For this economic evaluation, a Markov model was constructed for initial screening at different ages from a health care system perspective, and 5 endoscopic screening strategies with different frequencies (once per lifetime and every 10 years, 5 years, 3 years, and 2 years) were evaluated. The study was conducted between January 1, 2019, and October 31, 2020. Model parameters were estimated based on this project, government documents, and published literature. For each initial screening age (40-44, 45-49, 50-54, 55-59, 60-64, and 65-69 years), a closed cohort of 100 000 participants was assumed to enter the model and follow the alternative strategies.

Main Outcomes and Measures

Cost-effectiveness was measured by calculating the incremental cost-effectiveness ratio (ICER), and the willingness-to-pay threshold was assumed to be 3 times the per capita gross domestic product in China (US $10 276). Univariate and probabilistic sensitivity analyses were conducted to assess the robustness of model findings.

Results

The study included a hypothetical cohort of 100 000 individuals aged 40 to 69 years. All 5 screening strategies were associated with improved effectiveness by 1087 to 10 362 quality-adjusted life-years (QALYs) and increased costs by US $3 299 000 to $22 826 000 compared with no screening over a lifetime, leading to ICERs of US $1343 to $3035 per QALY. Screening at a higher frequency was associated with an increase in QALYs and costs; ICERs for higher frequency screening compared with the next-lower frequency screening were between US $1087 and $4511 per QALY. Screening every 2 years would be the most cost-effective strategy, with probabilities of 90% to 98% at 3 times the per capita gross domestic product of China. The model was the most sensitive to utility scores of esophageal cancer– or gastric cancer–related health states and compliance with screening.

Conclusions and Relevance

The findings suggest that combined endoscopic screening for esophageal and gastric cancers may be cost-effective in areas of China where the risk of these cancers is high; screening every 2 years would be the optimal strategy. These data may be useful for development of policies targeting the prevention and control of upper gastrointestinal tract cancer in China.

Introduction

The incidence of upper gastrointestinal tract cancer (UGIC), including esophageal cancer (EC) and gastric cancer (GC), is high in China, with an estimated 802 930 new cases (324 422 cases of EC and 478 508 cases of GC) and 674 924 deaths (301 135 due to EC and 373 789 due to GC) in 2020, accounting for approximately 50% of the global burden.1 However, the geographic distribution of UGIC is uneven in China, mortality rates in some areas being 2- to 3-fold higher than the national average.2,3,4

The prognosis of UGIC depends mainly on the disease stage at the time of diagnosis. In China, the overall 5-year survival rates for patients with EC and GC are 30.3% and 35.1%, respectively.5 However, the rates would be 86% and 90%, respectively, if disease were detected at an early stage.6,7 This potential for increased survival has provided justification for early detection programs. A series of nationwide screening programs has been established in several East Asian countries where the incidence rates are high. In Japan, radiographic screening for GC was developed in the 1960s, and a national screening program was established in 1983; currently, endoscopic screening every 2 to 3 years is usually recommended.8 South Korea introduced both radiographic screening and endoscopic screening for GC into national screening programs in 2000 and currently recommends endoscopic screening every 2 years.9 Over approximately the past 20 years, endoscopic examination has become a major screening method for UGIC because of its high accuracy.10 Several economic evaluation studies11,12,13,14,15,16 from South Korea, Singapore, Portugal, the US, and China showed that endoscopic screening for EC or GC was cost-effective compared with no screening. Another study17 conducted in the US suggested that the cost-effectiveness of combined endoscopic screening for EC and GC was comparable to that of funded screening programs for other cancers when it was integrated into the current colonoscopy screening program.

In China, several endoscopic screening programs for UGIC have been attempted in some areas with high incidence rates since 2005. Some observational studies18,19,20,21,22 have shown that endoscopic screening can reduce the incidence of and mortality associated with UGIC. To assess the feasibility and efficacy of endoscopic screening for EC and GC, a multicenter randomized controlled trial was launched in 2015, in which more than 140 000 persons aged 40 to 69 years were enrolled.23,24 A large amount of basic data has been obtained from this trial. The present study evaluated the cost-effectiveness of combined endoscopic screening for EC and GC in people aged 40 to 69 years in areas of China where the risk of these cancers is high. Furthermore, we evaluated the optimal initial age and frequency for screening.

Methods

This model-based economic evaluation was performed from the health care system perspective using TreeAge Pro (Healthcare Version) 2020 (TreeAge Software) and was conducted between January 1, 2019, and October 31, 2020. The project was registered with the Protocol Registration System in the Chinese Clinical Trial Registry and approved by the independent Ethics Committee of the National Cancer Center of China/Cancer Hospital, Chinese Academy of Medical Sciences. Because patient data were deidentified in the analysis, the requirement for informed consent was waived by the Ethics Committee of the National Cancer Center of China/Cancer Hospital, Chinese Academy of Medical Sciences. This evaluation followed the Consolidated Health Economic Evaluation Reporting Standards (CHEERS) reporting guideline.25

Markov Model

A Markov model was constructed for different initial screening ages (40-44, 45-49, 50-54, 55-59, 60-64, and 65-69 years) to simulate EC and GC progression and calculate related health and economic outcomes in a lifetime horizon. Five endoscopic screening strategies with different frequencies were considered, including once per lifetime and every 10 years, 5 years, 3 years, and 2 years. No screening was applied as a reference strategy. For each initial screening age, a closed cohort of 100 000 participants with a mean age of 42, 47, 52, 57, 62, or 67 years was assumed to enter the model and follow the alternative strategies.

The Markov model consisted of 26 health states. In addition to the normal and death states, series of EC and GC progression states were considered, and each progression state was divided into undetected and detected states. A posttreatment state was also considered separately from the states requiring medical treatment after diagnosis. Endoscopic screening, reexamination, and related treatment procedures followed the recommendations of the Chinese Expert Consensus on Screening and Endoscopic Diagnosis and Treatment of Early Esophageal Cancer/Gastric Cancer (2014 version).26,27 These recommendations were also followed in a randomized controlled trial by Chen et al.23 Details of the trial are given in the eMethods and eFigures 1 to 3 in the Supplement, details of the Markov model are given in eFigure 4 in the Supplement, and validation of the model is shown in eFigures 5 and 6 in the Supplement. Compliance with screening, reexamination, and treatment and complications associated with endoscopic screening were also considered in the model. The model was run with a 1-year cycle length and terminated when the mean age of the cohort reached 90 years. A half-cycle correction was applied.

Model Parameters

Compliance with endoscopic screening was determined to be 49% (range, 30%-80%) according to a pilot project concerning endoscopic screening for EC in several areas of China where the risk of EC is high (Table 1).18,28,29,30,31,32,33,34,35,36,37,38,39,40,41 Compliance with regular endoscopic reexamination among individuals who had mild esophageal dysplasia, moderate esophageal dysplasia, or low-grade gastric intraepithelial neoplasia detected on screening was assumed to be higher than compliance with endoscopic screening, which was 67% (range, 40%-90%) according to a previous report (Table 1).15 The model assumed that false-positive results would result in loss of quality of life but could be corrected with an endoscopic reexamination at an additional cost. The sensitivity and specificity of endoscopic examination for EC were 96% (range, 88%-99%) and 90% (range, 59%-100%), respectively, according to previous studies in areas in China where risk of EC is high.11,30,31 The sensitivity and specificity of endoscopic examination for GC were assumed to be 89% (range, 70%-98%) and 100% (range, 90%-100%), respectively, based on the published literature from other countries where risk for GC is high and other economic evaluation studies of GC8,12,32,33,34 because of the lack of available data in China. Clinically significant complications (eg, bleeding or perforation) are rare among individuals undergoing diagnostic endoscopic examination.42,43 The complication rate in the model was estimated to be 0.009% (range, 0%-0.2%) based on the trial by Chen et al23,24 and other published studies (Table 2).32,33,35

Table 1. Estimates of Parameters Used in the Model.

Parameter Base-case value Range Distribution Source
Compliance with screening 0.49 0.30-0.80 Triangular (0.30, 0.49, 0.80) Wei et al,18 2015; Feng et al,28 2015; Wang et al,29 2015
Compliance with reexamination 0.67 0.40-0.90 Triangular (0.40, 0.67, 0.90) Yang et al,15 2015
Endoscopic examination characteristics
Sensitivity for EC 0.96 0.88-0.99 Triangular (0.88, 0.96, 0.99) Chang et al,11 2012; Dawsey et al,30 1998; Nagami et al,31 2014
Specificity for EC 0.90 0.59-1.00 Triangular (0.59, 0.90, 1.00) Chang et al,11 2012; Dawsey et al,30 1998; Nagami et al,31 2014
Sensitivity for GC 0.89 0.70-0.98 Triangular (0.70, 0.89, 0.98) Zhou et al,12 2013; Hamashima et al,8 2018; Yeh et al,32 2016; Lee et al,33 2007; Hamashima et al,34 2013
Specificity for GC 1.00 0.90-1.00 Triangular (0.90, 1.00, 1.00) Zhou et al,12 2013; Hamashima et al,8 2018; Yeh et al,32 2016; Lee et al,33 2007; Hamashima et al,34 2013
Endoscopic examination complications 0.00009 0-0.002 Triangular (0, 0.00009, 0.002) Zeng et al,24 2020; Yeh et al,32 2016; Lee et al,33 2007; Espino et al,35 2012
Annual self-initiated examination
Severe esophageal dysplasia and CIS or HGIN and CIS 0.01 0.005-0.02 Triangular (0.005, 0.01, 0.02) Chang et al,11 2012
Early EC or GC 0.20 0.10-0.40 Triangular (0.10, 0.20, 0.40) Chang et al,11 2012
Advanced EC or GC 0.70 0.56-0.90 Triangular (0.56, 0.70, 0.90) Chang et al,11 2012
Compliance with treatment
Severe esophageal dysplasia or CIS 0.7458 0.5625-0.9654 β (31.72, 10.81) Chen et al,23 2017
Early EC 0.9405 0.7149-1.0000 β (8.17, 0.52) Chen et al,23 2017
Advanced EC 0.9643 0.8393-1.0000 β (16.99, 0.63) Chen et al,23 2017
HGIN or CIS 0.5455 0.4425-0.7746 β (92.43, 77.01) Chen et al,23 2017
Early GC 0.9000 0.6792-1.0000 β (12.41, 1.38) Chen et al,23 2017
Advanced GC 0.9643 0.8393-1.0000 β (16.99, 0.63) Chen et al,23 2017
Costs, $
Screening mobilization and administration per capita 1.05 ±50% γ (0.16, 0.15) Chen et al,23 2017
Endoscopic examination 47.87 ±50% γ (46.57, 0.97) Chen et al,23 2017
Treatment for endoscopic complications 113.68 ±50% γ (5.82, 0.05) Chen et al,23 2017
Initial treatment
Severe esophageal dysplasia or CIS 1604 ±50% γ (3.33, 0.002) Yang et al,36 2018
Early EC 7732 ±50% γ (2.33, 3.01) Yang et al,36 2018
Advanced EC 7320 ±50% γ (3.33, 4.55) Yang et al,36 2018
HGIN or CIS 1423 ±50% γ (1.41, 9.88) Yang et al,36 2018
Early GC 7548 ±50% γ (4.61, 6.11) Yang et al,36 2018
Advanced GC 7086 ±50% γ (5.96, 8.41) Yang et al,36 2018
Annual health care
Severe esophageal dysplasia or CIS 216 ±50% γ (1.22, 0.006) Yang et al,36 2018
Early EC 367 ±50% γ (1.23, 0.003) Yang et al,36 2018
Advanced EC 342 ±50% γ (2.05, 0.006) Yang et al,36 2018
HGIN or CIS 243 ±50% γ (1.24, 0.005) Yang et al,36 2018
Early GC 409 ±50% γ (1.18, 0.003) Yang et al,36 2018
Advanced GC 435 ±50% γ (1.19, 0.003) Yang et al,36 2018
Utility scores
Mild esophageal dysplasia 1.00 0.98-1.00 Triangular (0.98, 1.00, 1.00) Sharaiha et al,37 2014; Inadomi et al,38 2009
Moderate esophageal dysplasia 1.00 0.98-1.00 Triangular (0.98, 1.00, 1.00) Sharaiha et al,37 2014; Inadomi et al,38 2009
Severe esophageal dysplasia or CIS 0.84 0.79-0.89 β (3.57, 0.68) Liu et al,39 2018
Early EC 0.70 0.66-0.74 β (2.63, 1.13) Liu et al,39 2018
Advanced EC 0.61 0.56-0.66 β (1.12, 0.71) Liu et al,39 2018
LGIN 1.00 0.98-1.00 Triangular (0.98, 1.00, 1.00) Sharaiha et al,37 2014; Inadomi et al,38 2009
HGIN or CIS 0.92 0.86-0.99 β (2.53, 0.22) Xia et al,40 2020
Early GC 0.75 0.71-0.78 β (3.15, 1.05) Xia et al,40 2020
Advanced GC 0.57 0.53-0.62 β (1.35, 1.02) Xia et al,40 2020
Discount rate 0.05 0-0.08 NA Weinstein et al,41 1996
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Abbreviations: CIS, carcinoma in situ; EC, esophageal cancer; GC, gastric cancer; HGIN, high-grade intraepithelial neoplasia; LGIN, low-grade intraepithelial neoplasia; NA, not applicable.

Table 2. Base-Case Cost-effectiveness Results Compared Among Different Strategies by Initial Screening Age Among 100 000 Cohort Membersa.

Initial screening age, strategy QALYs Incremental QALYs Cost ($, thousand) Incremental cost ($, thousand) ICER ($/QALY)
Vs no screening Vs the next most effective strategyb Vs no screening Vs the next most effective strategyb Vs no screening Vs the next most effective strategyb
40-44 y
No screening 1 659 260 NA NA 25 035 NA NA NA NA
Screening once per lifetime 1 660 347 1087 1087 28 334 3299 3299 3035 3035
Screening every 10 y 1 663 677 4417 3330 31 954 6919 3620 1566 1087
Screening every 5 y 1 666 345 7085 2668 36 707 11 672 4753 1647 1781
Screening every 3 y 1 668 371 9111 2026 42 218 17 183 5511 1886 2720
Screening every 2 y 1 669 622 10 362 1251 47 861 22 826 5643 2203 4511
45-49 y
No screening 1 572 532 NA NA 26 817 NA NA NA NA
Screening once per lifetime 1 574 161 1629 1629 30 347 3530 3530 2167 2167
Screening every 10 y 1 576 941 4409 2780 33 961 7144 3614 1620 1300
Screening every 5 y 1 579 145 6613 2204 37 745 10 928 3784 1653 1717
Screening every 3 y 1 580 974 8442 1829 42 531 15 714 4786 1861 2617
Screening every 2 y 1 582 334 9802 1360 48 190 21 373 5659 2180 4161
50-54 y
No screening 1 468 506 NA NA 30 229 NA NA NA NA
Screening once per lifetime 1 470 890 2384 2384 34 142 3913 3913 1641 1641
Screening every 10 y 1 472 583 4077 1693 36 373 6144 2231 1507 1318
Screening every 5 y 1 474 773 6267 2190 40 356 10 127 3983 1616 1819
Screening every 3 y 1 476 325 7819 1552 44 120 13 891 3764 1777 2425
Screening every 2 y 1 477 651 9145 1326 49 010 18 781 4890 2054 3688
55-59 y
No screening 1 342 830 NA NA 36 095 NA NA NA NA
Screening once per lifetime 1 346 031 3201 3201 40 491 4396 4396 1373 1373
Screening every 10 y 1 347 264 4434 1233 42 811 6716 2320 1515 1882
Screening every 5 y 1 348 747 5917 1483 45 240 9145 2429 1546 1638
Screening every 3 y 1 350 365 7535 1618 49 171 13 076 3931 1735 2430
Screening every 2 y 1 351 491 8661 1126 52 843 16 748 3672 1934 3261
60-64 y
No screening 1 195 742 NA NA 45 876 NA NA NA NA
Screening once per lifetime 1 199 618 3876 3876 51 081 5205 5205 1343 1343
Screening every 5 y 1 201 091 5349 1473 53 970 8094 2889 1513 1961
Screening every 3 y 1 202 293 6551 1202 56 498 10 622 2528 1621 2103
Screening every 2 y 1 203 210 7468 917 58 779 12 903 2281 1728 2487
65-69 y
No screening 1 025 119 NA NA 60 442 NA NA NA NA
Screening once per lifetime 1 029 058 3939 3939 67 233 6791 6791 1724 1724
Screening every 2 y 1 030 594 5475 1536 70 810 10 368 3577 1894 2329
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Abbreviations: ICER, incremental cost-effectiveness ratio; NA, not applicable; QALY, quality-adjusted life-year.

a

QALYs, costs, and ICERs are expressed as the values in 2019.

b

Compared with the next most effective strategy at the same initial screening age.

The prevalence rates of EC- and GC-related health states were estimated based on baseline screening reports from the trial by Chen et al23 in areas where the risk of these cancers is high (eTable 1 in the Supplement); these reports were used to determine initial distributions of cohort members across health states in the model. A wide range was set for each rate to cover the values reported in these areas by referring to previous studies from China.29,44,45,46 The annual transition probabilities were derived from published observational studies concerning the natural history of EC and GC and economic evaluation studies of EC and GC (eTable 2 in the Supplement).15,47,48,49

The model assumed that in the absence of active screening, individuals with severe esophageal dysplasia and carcinoma in situ, high-grade gastric intraepithelial neoplasia and carcinoma in situ, or EC or GC would receive a diagnosis on the basis of self-initiated examinations according to state-specific probabilities (Table 1).11 Individuals with these diagnoses would receive state-specific treatments, whereas individuals who did not receive these diagnoses would remain untreated. The rates of state-specific compliance with treatment were calculated for the proportion of screened patients who actually completed the entire treatment procedure in areas where the risk of UGIC is high in the trial by Chen et al23 (eTable 3 in the Supplement). The state-specific probabilities of recurrence after treatment and cancer-related mortality rates for advanced EC and GC were estimated based on the survival rates among patients with EC and GC (eTable 2 in the Supplement),15 whereas age-specific natural background death rates were obtained from the China Population & Employment Statistics Yearbook, 2019.50

Costs were converted from Chinese renminbi to 2019 US dollars (US $1 = ¥6.8968 in 2019). The cost of screening included screening mobilization and administration costs, endoscopic examination costs, and costs of treatment for endoscopic complications, all of which were obtained from the 7 study centers that participated in the trial by Chen et al23 (eTable 4 in the Supplement). The cost of EC- and GC-related treatment included the initial treatment cost after detection of the cancer and the subsequent annual health care cost after treatment, both of which were obtained from the survey included in the trial by Chen et al23 that was administered to assess the economic burden of UGIC in China.36 Calculation details are shown in eTable 5 in the Supplement.

The health outcome was utility-weighted life expectancy expressed as quality-adjusted life-years (QALYs). Utility scores of EC- and GC-related health states were obtained from the survey included in the trial by Chen et al23 that was administered to assess the quality of life of patients with UGIC in China (eTable 6 in the Supplement).39,40 Considering that patients diagnosed with mild esophageal dysplasia, moderate esophageal dysplasia, and low-grade gastric intraepithelial neoplasia do not have symptoms, we used a utility score of 1 in the base-case analysis and set a range of 0.98 to 1 in the sensitivity analyses.37,38 We assumed a discount rate of 5% (range, 0%-8%) for both QALYs and costs.41 The choice of distribution for all parameters was based on consideration of the properties of the parameters and the data informing the parameters.

Statistical Analysis

Effectiveness and Cost-effectiveness Evaluation

Expected QALYs and costs of each strategy were obtained from the model. We evaluated the cost-effectiveness of screening strategies at different initial screening ages with 2 approaches. First, we calculated the incremental cost-effectiveness ratio (ICER), defined as incremental costs per QALY gained of each screening strategy compared with no screening. Second, we calculated the ICER of each screening strategy compared with the next most effective screening strategy to identify the optimal strategy at each initial screening age. Because of the lack of data regarding the willingness to pay in the population of China, we adopted the cost-effectiveness definition used by the World Health Organization. Highly cost-effective was defined as an ICER less than 1 time the per capita gross domestic product (GDP) in China; cost-effective, an ICER of 1 to 3 times the per capita GDP; and not cost-effective, and an ICER greater than 3 times the per capita GDP.51 The per capita GDP in China in 2019 was US $10 276.

Uncertainty and Sensitivity Analyses

Univariate sensitivity analyses of all parameters within their respective ranges were performed to identify the main sensitivity parameters. Probabilistic sensitivity analyses were further conducted to determine the probability of each screening strategy being cost-effective compared with no screening and the probability of each strategy being optimal compared with all other strategies.

Results

Base-Case Results

The study included a hypothetical sample of 100 000 individuals aged 40 to 69 years. All 5 screening strategies increased QALYs and costs compared with no screening at the same initial screening age (Table 2) by 1087 to 10 362 QALYs and US $3 299 000 to $22 826 000 for a cohort of 100 000 participants over a lifetime, and the corresponding ICERs were US $1343 to $3035 per QALY, which were lower than the per capita GDP ($10 276). Therefore, all screening strategies would be more cost-effective than no screening.

Further comparisons of the screening strategies were performed, and more frequent screening would be associated with a gain of more QALYs but with higher costs (Table 2). When a screening strategy was compared with the next most effective screening strategy in the cohort with the same initial screening age, 917 to 3939 QALYs would be gained and an additional cost of US $2 231 000 to $6 791 000 gained for a cohort of 100 000 participants over a lifetime; the corresponding ICERs were US $1087 to $4511 per QALY, which was lower than the per capita GDP. Therefore, the high-frequency screening strategy would be more cost-effective than the low-frequency screening strategy, and screening every 2 years would be the optimal strategy at each initial screening age. Screening every 2 years and screening once per lifetime had the most incremental QALYs at the initial screening ages of 40 to 44 years and 65 to 69 years, respectively.

Sensitivity Analysis Results

Univariate sensitivity analyses revealed that the results remained largely unchanged over the plausible range of each parameter. The ICER upper limits of the most sensitive parameters of each screening strategy at different initial screening ages are shown in Table 3. When a screening strategy was compared with no screening, only varying utility scores of EC- and GC-related health states resulted in ICERs exceeding the per capita GDP at initial screening ages of 40 to 44 years and 65 to 69 years. When a screening strategy was compared with the next most effective screening strategy, varying utility scores of EC- and GC-related health states resulted in ICERs at some initial screening ages exceeding 3 times the per capita GDP, and varying compliance with screening resulted in ICERs of screening every 2 years vs screening every 3 years exceeding the per capita GDP. Univariate sensitivity analyses demonstrated the stability of the cost-effectiveness and ranking of the cost-effectiveness of the screening strategies.

Table 3. Upper Limits of Incremental Cost-effectiveness Ratio for Each Screening Strategy in Univariate Sensitivity Analyses by Initial Screening Agea.

Initial screening age and screening strategy Utility scoresb Compliance with screening Discount rate Prevalences of EC- and GC-related health statesb Costs of screeningc Annual transition probability from severe esophageal dysplasia or CIS to early EC
Vs no screening Vs the next most effective strategy Vs no screening Vs the next most effective strategy Vs no screening Vs the next most effective strategy Vs no screening Vs the next most effective strategy Vs no screening Vs the next most effective strategy Vs no screening Vs the next most effective strategy
40-44 y
Screening once per lifetime 11 778d 11 778d 4016 4016 6671 6671 4711 4711 4422 4422 4592 4592
Screening every 10 y 4498 2877 1883 1271 3440 2144 1737 1129 2272 1570 2186 1658
Screening every 5 y 5116 6395 1845 2277 3467 3513 1811 1927 2397 2603 2308 2513
Screening every 3 y 6202 11 273d 2085 5204 3871 5260 2082 3003 2758 4022 2609 3659
Screening every 2 y 7452 19 296d 2619 13 156d 4480 8663 2451 5127 3240 6747 2996 5740
45-49
Screening once per lifetime 6153 6153 2760 2760 4486 4486 3448 3448 3092 3092 2677 2677
Screening every 10 y 5236 4571 1912 1473 3248 2358 1934 1389 2304 1842 2259 1986
Screening every 5 y 5310 5455 1853 2155 3246 3241 1949 1979 2370 2502 2284 2333
Screening every 3 y 6217 10 190 2020 4874 3583 4782 2206 3090 2687 3830 2539 3455
Screening every 2 y 7678 22 118d 2552 10 504d 4128 7457 2605 5002 3163 6125 2936 5387
50-54 y
Screening once per lifetime 3976 3976 1674 1974 3216 3216 2609 2609 2296 2296 2134 2134
Screening every 10 y 4253 4844 1564 1409 2897 2367 2010 1479 2122 1876 2069 1972
Screening every 5 y 5210 7982 1850 2752 2998 3197 2091 2219 2292 2609 2238 2560
Screening every 3 y 5803 8366 2233 6715 3252 4255 2320 3550 2542 3197 2424 3161
Screening every 2 y 7025 17 484d 2821 12 807d 3695 6278 2710 4887 2956 5401 2768 4787
55-59 y
Screening once per lifetime 3271 3271 1394 1394 2601 2601 2127 2127 1882 1882 1920 1920
Screening every 10 y 4841 52 896e 1527 2043 2746 3194 2151 2191 2084 2608 2194 2954
Screening every 5 y 5026 5620 1680 2573 2777 2868 2186 2277 2155 2366 2210 2258
Screening every 3 y 6162 13 002d 2076 5658 3046 4045 2476 3421 2443 3496 2455 3346
Screening every 2 y 6920 12 320d 2523 13 669d 3357 5377 2814 5008 2745 4770 2694 4255
60-64 y
Screening once per lifetime 3635 3635 1360 1360 2476 2476 1995 1995 1794 1794 2054 2054
Screening every 5 y 5310 31 253e 1566 2611 2697 3324 2235 2736 2055 2741 2324 3033
Screening every 3 y 6082 11 374d 1805 4871 2847 3515 2448 3321 2228 3001 2459 3044
Screening every 2 y 6492 9464 2076 11 769d 3011 4159 2683 4334 2399 3621 2586 3459
65-69 y
Screening once per lifetime 8653 8653 1741 1741 3128 3128 2375 2375 2185 2185 3053 3053
Screening every 2 y 14 302d 25 436d 2019 4801 3372 4011 2747 3644 2456 3153 3313 3959
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Abbreviations: CIS, carcinoma in situ; EC, esophageal cancer; GC, gastric cancer; ICER, incremental cost-effectiveness ratio.

a

Only main sensitive parameters are shown; ICERs are expressed as the value in 2019.

b

As a set of parameters, all the parameters changed simultaneously with a positive correlation in univariate sensitivity analyses.

c

Including screening mobilization and administration costs, endoscopic examination costs, and treatment costs for endoscopic complications. The 3 parameters changed simultaneously with a positive correlation in univariate sensitivity analyses.

d

The upper limit of ICER was higher than the per capita GDP but lower than 3 times the per capita GDP.

e

The upper limit of ICER was higher than 3 times the per capita GDP.

The results of the probabilistic sensitivity analyses of each screening strategy compared with no screening are shown in Figure 1. The probability of each screening strategy being cost-effective increased as the willingness-to-pay threshold increased and reached 91% to 98% even at a willingness-to-pay threshold of the per capita GDP. The results of the probabilistic sensitivity analyses conducted for each strategy compared with all other strategies are shown in Figure 2. Screening every 2 years maintained its dominance from a willingness-to-pay threshold of less than the per capita GDP to a willingness-to-pay threshold equal to 3 times the per capita GDP at each initial screening age, with probabilities of 82% to 93% and 90% to 98% for being optimal at 1 and 3 times per capita GDP, respectively. Therefore, all screening strategies would be more cost-effective than no screening, and screening every 2 years would be the optimal strategy at a willingness-to-pay threshold of 3 times the per capita GDP.

Figure 1. Cost-effectiveness Acceptability Curves of All Screening Strategies Compared With No Screening by Initial Screening Age.

Figure 1.

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Dashed vertical blue lines represent per capita gross domestic product (GDP); dashed vertical black lines represent 3 times per capita GDP. QALY indicates quality-adjusted life-year.

Figure 2. Cost-effectiveness Acceptability Curves of All Strategies Competing With Each Other by Initial Screening Age.

Figure 2.

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Dashed vertical blue lines represent per capita gross domestic product (GDP); dashed vertical black lines represent 3 times per capita GDP. QALY indicates quality-adjusted life-year.

Discussion

Upper gastrointestinal tract cancer continues to be a major public health burden in areas in China where incidence and mortality rate for this cancer are higher than those in other areas. The present study targeted local residents aged 40 to 69 years in areas where the risk of UGIC is high who were most likely to benefit from endoscopic screening according to the age characteristics of UGIC incidence and life expectancy in China, and this population accounts for a large proportion of patients with UGIC in China. Our base-case results suggest that combined endoscopic screening for EC and GC would be more cost-effective than no screening regardless of the initial screening age or screening frequency; this finding is consistent with the conclusion reported in a systematic review.52 Screening every 2 years would be the optimal strategy, and an initial screening age of 40 to 44 years was associated with the most health benefits. A screening frequency of 1 to 5 years has been previously proposed,53 with the optimal interval being less than 3 years.54 Most cases of early UGIC that were missed at the first endoscopic examination and subsequently identified in the second screening within 3 years were still amenable to curative surgery,55 which could theoretically increase the sensitivity of endoscopic examination after 2 consecutive screenings.13 The optimal strategy in this study was similar to the guidelines recommended in Japan and South Korea,8,9 where the incidence rates are as high as those in China. Areas in China where the risk of UGIC is high are usually rural and have limited health resources and an underdeveloped economy.56,57 Policy makers should consider the cost and effectiveness of the screening strategy, local economic level, and disease burden of UGIC when choosing appropriate screening strategies. If screening once per lifetime, which was the least expensive screening strategy, is preferable, the optimal initial screening age suggested by this study is 65 to 69 years.

Univariate sensitivity analyses revealed that utility scores of EC- and GC-related health states and compliance with screening were the 2 main sensitivity parameters. In this study, because most patients diagnosed with mild esophageal dysplasia, moderate esophageal dysplasia, or low-grade gastric intraepithelial neoplasia did not have symptoms, we used a utility score of 1 in the base-case analysis and a range of 0.98 to 1 in the sensitivity analyses according to other reports.37,38 Whether any decrements in the quality of life could be present in patients diagnosed with mild esophageal dysplasia, moderate esophageal dysplasia, or low-grade intraepithelial neoplasia if they were asymptomatic and received education regarding their true cancer risk is unknown.17 Although previous studies have found that patients with precancerous lesions have a poorer quality of life than the general population,58,59 whether the decrement in the quality of life is caused by coexisting symptoms (eg, esophagitis, gastric ulcers) or the patient’s perception of cancer risk remains unknown.60 Future studies should focus on the effect on the quality of life among those diagnosed with precancerous lesions. Compliance with screening affected whether the optimal strategy was screening every 2 years or screening every 3 years at a willingness-to-pay threshold of the per capita GDP. Endoscopic screening may be associated with reduced incidence and mortality of UGIC, and improving compliance among the target population is critical for achieving prevention effectiveness. The compliance with screening in this study was only 49%, which was derived from the areas with the highest incidence of UGIC in China18; these areas have the most longstanding promotion times and the most abundant experience with endoscopic screening and have residents with the highest cognitive understanding of endoscopic screening. Endoscopic screening is relatively expensive and slightly invasive, resulting in discomfort when individuals are examined. In addition, most of the target population, aged 40 to 69 years (especially men), in areas where there is high risk of UGIC are the primary sources of family income and migrate elsewhere for work. Therefore, compliance with endoscopic screening for UGIC is still low in China, and further popularization and promotion of endoscopic screening are needed to improve compliance.

Limitations

This study has limitations. The accuracy of the model depends on the accuracy of parameter estimates. First, base-case initial probabilities of EC- and GC-related health states were derived from the study by Chen et al.23 Residents of areas where there is high risk of UGIC enrolled in the project may have had a higher incidence of this cancer; thus, the estimated parameters may not represent the status of the entire region. Second, annual progression or regression transition probabilities of health states should increase or decrease with age in the real world. However, those between specific precancerous lesion states were fixed owing to the lack of relevant observational data. As a result, the cost-effectiveness of screening strategies may be overestimated in younger age groups and underestimated in older age groups. Third, compliance with different screening frequencies was assumed to be consistent in the model. In the real world, a higher screening frequency may be associated with a reduction in compliance because of patients’ concerns about pain and sedation and competing life demands.61,62 Fourth, annual screening was not considered as an alternative strategy in this study because it has not been recommended in any country until now. In addition, the burden may be difficult to address in countries with low GDP.

Conclusions

To our knowledge, this is the first comprehensive cost-effectiveness analysis of endoscopic screening for both EC and GC in China. The findings from the present study suggest that from the perspective of the health care system, combined endoscopic screening for EC and GC would be highly cost-effective for people aged 40 to 69 years in areas of China where there is a high risk of UGIC; screening every 2 years would be the optimal strategy. The findings provide important evidence for policies targeting the prevention and control of UGIC in China.

Supplement.

eMethods.

eFigure 1. Flowchart of the Overall Participants in the Multicenter Randomized Trial Project

eFigure 2. Flowchart of the Participants in the High-Risk Areas

eFigure 3. Flowchart of the Screening and Reexamination

eFigure 4. Markov Model of Upper Gastrointestinal Tract Cancer (Including Esophageal Cancer and Gastric Cancer) Progression

eFigure 5. Model Projected Age-Specific GC Incidence and Mortality Rates Compared to 2 Folds of Observed National GC Incidence and Mortality Rates in 2015

eFigure 6. Model Projected Age-Specific EC Incidence and Mortality Rates Compared to 2 Folds of Observed National EC Incidence and Mortality Rates in 2015

eTable 1. Prevalence Rates (%) of EC/GC-Related Health States Used in the Model, by Initial Screening Age

eTable 2. Annual Transition Probabilities Used in the Model

eTable 3. State-Specific Compliances with Treatment Estimated Based on Our Project

eTable 4. Costs of Screening Estimated Based on Our Project

eTable 5. Costs of EC/GC-Related Treatment in Different Disease Progression Stages Based on the Survey Included in Our Project (US$)

eTable 6. Utility Scores of EC/GC-Related Health States Based on the Survey Included in Our Project

eReferences.

Click here for additional data file. (1MB, pdf)

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Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

Supplement.

eMethods.

eFigure 1. Flowchart of the Overall Participants in the Multicenter Randomized Trial Project

eFigure 2. Flowchart of the Participants in the High-Risk Areas

eFigure 3. Flowchart of the Screening and Reexamination

eFigure 4. Markov Model of Upper Gastrointestinal Tract Cancer (Including Esophageal Cancer and Gastric Cancer) Progression

eFigure 5. Model Projected Age-Specific GC Incidence and Mortality Rates Compared to 2 Folds of Observed National GC Incidence and Mortality Rates in 2015

eFigure 6. Model Projected Age-Specific EC Incidence and Mortality Rates Compared to 2 Folds of Observed National EC Incidence and Mortality Rates in 2015

eTable 1. Prevalence Rates (%) of EC/GC-Related Health States Used in the Model, by Initial Screening Age

eTable 2. Annual Transition Probabilities Used in the Model

eTable 3. State-Specific Compliances with Treatment Estimated Based on Our Project

eTable 4. Costs of Screening Estimated Based on Our Project

eTable 5. Costs of EC/GC-Related Treatment in Different Disease Progression Stages Based on the Survey Included in Our Project (US$)

eTable 6. Utility Scores of EC/GC-Related Health States Based on the Survey Included in Our Project

eReferences.

Click here for additional data file. (1MB, pdf)

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