J Cancer Prev 2024; 29(4): 148-156
Published online December 30, 2024
https://doi.org/10.15430/JCP.24.024
© Korean Society of Cancer Prevention
Yonghoon Choi1,2 , Nayoung Kim1,2,3 , Seon Hee Lim4 , Ji Hyun Park3 , Jeong Hwan Lee1 , Yeejin Kim1 , Hyemin Jo1 , Ho-Kyoung Lee1 , Jinju Choi1 , Yu Kyung Jun1 , Hyuk Yoon1 , Cheol Min Shin1 , Young Soo Park1 , Dong Ho Lee1,2,3
1Department of Internal Medicine, 2Research Center for Sex- and Gender-Specific Medicine, Seoul National University Bundang Hospital, Seongnam, 3Department of Internal Medicine and Liver Research Institute, Seoul National University College of Medicine, 4Department of Internal Medicine, Seoul National University Healthcare System Gangnam Center, and Healthcare Research Institute, Seoul, Korea
Correspondence to :
Nayoung Kim, E-mail: nakim49@snu.ac.kr, https://orcid.org/0000-0002-9397-0406
This is an Open Access article distrBifidobacterium longum, Irritable bowel syndrome, Rats, Probioticsibuted under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted noncommercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
Serological tests for Helicobacter pylori needs local validation as the diagnostic accuracy may vary depending on the prevalence of H. pylori. This study examined the diagnostic performance of two ELISA, GastroPanel® (GastroPanel ELISA; Biohit Oyj) and GENEDIA ® (GENEDIA® H. pylori ELISA, Green Cross Co.) in Korean population. One thousand seventy seven patients who visited for esophagogastroduodenoscopy between 2013 and 2023 were prospectively enrolled, and serum samples from the subjects were tested using both GastroPanel® and GENEDIA®. The two tests were compared for their diagnostic accuracy in detecting atrophic gastritis (AG), intestinal metaplasia (IM), gastric adenoma (GA), and gastric cancer (GC), and the positivity rates by age and sex were observed. There was substantial correlation (Pearson coefficient [r] = 0.512, P < 0.001) and agreement (Cohen’s Kappa coefficient [κ] = 0.723, P < 0.001) between the results obtained using GastroPanel® and GENEDIA®. The test results from the two kits did not match perfectly with a discrepancy observed in approximately 16% of cases, that 67 subjects were positive only on GENEDIA ® while 75 subjects were positive only on GastroPanel®. The area under receiver operating characteristic curve for AG, IM, GA, and GC using GastroPanel® were 0.666, 0.635, 0.540, and 0.575, while the results tested using GENEDIA® were 0.649, 0.604, 0.553, and 0.555, respectively, without significant difference between the two results. GastroPanel® and GENEDIA® showed similar performance in terms of diagnostic accuracy; but the test results did not match perfectly. A large-scale validation study in Koreans is needed.
Keywords: Helicobacter pylori, Serology, Enzyme-linked immunosorbent assay, Diagnosis
Serological tests for diagnosing
In South Korea, serological tests include bacterial agglutination, complement fixation, indirect immunofluorescence test, and immunoassay, depending on the antibody measurement method [2], and among immunoassay techniques, enzyme immunoassay, ELISA, radioimmunoassay, and chemiluminescent immunoassay are commonly used, with ELISA being the most widely utilized method [2,5,6]. GENEDIA®
Recently, GastroPanel®, an ELISA-based biomarker assay panel, was introduced in Europe [9]. The test kit is composed of ELISA of pepsinogen I (PG I), PG II and gastrin-17 combined with an ELISA assay of HpIgG, all being measured from the same serum/plasma sample [10]. GastroPanel® has been introduced as a method to quickly and accurately diagnose the condition of the gastric mucosa and the presence of
Considering this, we aimed to compare the diagnostic accuracy of
A total of 1,077 patients who visited for upper endoscopy between June 2013 and May 2023 were prospectively enrolled. The medical histories of the participants were reviewed using electronic medical record, and subjects with postgastrectomy status, those requiring continuous medication due to chronic conditions, or those have taken acid-suppressing drugs such as proton-pump inhibitors within the last six months were excluded.
The study protocol was reviewed and approved by the Institutional Review Board of the Seoul National University Bundang Hospital (B-2403-889-303), and written informed consent was obtained from all the participants (B-0602-030-001, B-0903-071-001, B-1012-117-013, and B-1103-123-004). There were no potential conflicts of interest regarding the use of commercial kits, and the study design, data collection, analysis, and manuscript preparation were conducted entirely at the authors’ discretion.
An existing study by our team was referred to for the acquisition of blood and tissue samples and measurement methods [14]. Briefly, fasting serum samples were collected from all the participants at the time of enrollment. The samples were centrifuged immediately at 4°C and stored at –80°C until required. Serum HpIgG was measured using GENEDIA® (GENEDIA
To diagnose
As mentioned, the primary outcome of this study was the comparison of diagnostic accuracy for
All statistical analyses were performed using SPSS software (version 25.0; IBM Corp.). Student’s
Baseline characteristics of the enrolled patients are shown in Table 1. There were 652 (60.5%) males and 425 (39.5%) females, with an average age of 58.01 years. The study participants included 552 (51.3%) normal controls without dysplastic lesions, and 166 (15.4%) and 359 (33.3%) with histologically confirmed GA or GC, respectively. In the
Table 1 . Basic characteristics of study subjects
Variable | Total (n = 1,077) | (n = 651) | H. pylori seronegative by GENEDIA® (n = 426) | |
---|---|---|---|---|
Sex | < 0.001 | |||
Male | 652 (60.5) | 428 (65.7) | 224 (52.6) | |
Female | 425 (39.5) | 223 (34.3) | 202 (47.4) | |
Age (yr) | 58.01 ± 13.25 | 58.25 ± 12.38 | 57.68 ± 14.50 | 0.500 |
Smoking | 0.022 | |||
Never | 476 (44.6) | 267 (41.5) | 209 (49.4) | |
Ex-smoker | 221 (20.7) | 147 (22.8) | 74 (17.5) | |
Current smoker | 370 (34.7) | 230 (35.7) | 140 (33.1) | |
Alcohol drinking | 0.009 | |||
Never | 588 (55.2) | 336 (52.3) | 252 (59.7) | |
Ex-drinker | 316 (29.7) | 213 (33.1) | 103 (24.4) | |
Current drinker | 161 (15.1) | 94 (14.6) | 67 (15.9) | |
Previous | 0.106 | |||
No | 886 (85.2) | 550 (86.6) | 336 (83.0) | |
Yes | 154 (14.8) | 85 (13.4) | 69 (17.0) | |
Endoscopic findings | < 0.001 | |||
Normal control | 327 (30.4) | 137 (21.1) | 190 (44.6) | |
Duodenal ulcer | 87 (8.1) | 64 (9.8) | 23 (5.4) | |
Gastric ulcer | 138 (12.8) | 92 (14.1) | 46 (10.8) | |
Gastric adenoma | 166 (15.4) | 119 (18.3) | 47 (11.0) | |
Gastric cancer | 359 (33.3) | 239 (36.7) | 120 (28.2) | |
< 0.001 | ||||
Negative | 418 (38.8) | 67 (10.3) | 351 (82.4) | |
Positive | 659 (61.2) | 584 (89.7) | 75 (17.6) |
Values are presented as number (%) or mean ± SD. Values are measured using. GENEDIA® (GENEDIA
When analyzing the concordance and correlation between the results of the two kits, the Cohen’s Kappa coefficient was 0.723 (
HpIgG titer on GENEDIA® and GastroPanel® according to clinicopathological factors was compared (Table 2). As results, the HpIgG levels were statistically significantly higher in individuals with AG, IM, and gastric ulcers compared to those without these conditions on both GENEDIA® and GastroPanel®. In contrast, HpIgG levels were significantly higher in individuals with duodenal ulcers compared to those without in the case of GENEDIA®, whereas no such difference was observed with GastroPanel®. In individuals with gastric dysplastic lesions, HpIgG levels were higher in those with GA or GC compared to the control group, and there was no significant difference between the GA group and the GC group when tested with GENEDIA®. On the other hand, there was a tendency for HpIgG levels to increase in the order of control, GA, and GC group when measured with GastroPanel®. When analyzed by age, both kits showed the highest HpIgG levels in the 40 to 69 age group. When analyzed by sex, GENEDIA® showed a tendency for higher levels in males, but this was not statistically significant, whereas HpIgG levels were significantly higher in males on GastroPanel®.
Table 2 . Comparison of titer of GENEDIA® and GastroPanel® on prediction for specific factors
Variable | HpIgG titer on GENEDIA® (OD) | HpIgG titer on GastroPanel® (EIU) | ||
---|---|---|---|---|
Atrophic gastritis | < 0.001 | < 0.001 | ||
Present | 1.34 ± 1.01 | 212.29 ± 405.36 | ||
Absent | 0.86 ± 1.00 | 107.13 ± 302.80 | ||
Intestinal metaplasia | < 0.001 | < 0.001 | ||
Present | 1.26 ± 1.01 | 201.96 ± 408.76 | ||
Absent | 0.96 ± 1.03 | 113.05 ± 290.91 | ||
Gastric ulcer | 0.044 | 0.033 | ||
Present | 1.29 ± 1.08 | 226.27 ± 419.69 | ||
Absent | 1.09 ± 1.06 | 145.64 ± 350.09 | ||
Duodenal ulcer | 0.003 | 0.708 | ||
Present | 1.43 ± 1.02 | 145.20 ± 270.02 | ||
Absent | 1.08 ± 1.06 | 156.93 ± 367.55 | ||
Gastric dysplastic lesion | 0.005 | 0.029 | ||
Control | 1.01 ± 1.07 | 129.93 ± 313.03 | ||
Adenoma | 1.22 ± 1.01 | 157.72 ± 336.97 | ||
Cancer | 1.22 ± 1.06 | 194.84 ± 429.78 | ||
Age (yr) | 0.008 | 0.093 | ||
< 40 | 0.91 ± 1.05 | 96.43 ± 249.67 | ||
40-69 | 1.18 ± 1.06 | 170.08 ± 389.41 | ||
≥ 70 | 0.99 ± 1.07 | 137.04 ± 294.39 | ||
Sex | 0.156 | < 0.001 | ||
Male | 1.15 ± 1.02 | 192.95 ± 413.16 | ||
Female | 1.05 ± 1.13 | 98.93 ± 249.38 |
Values are presented as mean ± SD. Values are measured using GENEDIA® (GENEDIA
The diagnostic accuracy of GENEDIA® and GastroPanel® in gastric lesions was compared using ROC curve (Fig. 1, Table 3). The areas under the curve (AUCs) for GENEDIA® in diagnosing AG, IM, GA, and GC were 0.649, 0.604, 0.553, and 0.555, respectively, with the optimal cutoff values being 0.46, 0.30, 0.40, and 0.21. For GastroPanel®, the AUCs for diagnosing AG, IM, GA, and GC were 0.666, 0.634, 0.541, and 0.575, respectively, with the optimal cutoff values being 18.31, 17.53, 18.35, and 19.33. When comparing the two kits, there was no statistically significant difference, but GastroPanel® showed slightly higher sensitivity and specificity than GENEDIA®.
Table 3 . Comparison of GENEDIA® and GastroPanel® in the diagnosis of gastric diseases
Variable | GENEDIA® | GastroPanel® |
---|---|---|
Atrophic gastritis | ||
AUC | 0.649 | 0.666 |
< 0.001 | < 0.001 | |
HpIgG cutoffa | 0.46 | 18.31 |
Sensitivity (%) | 72 | 74 |
Specificity (%) | 57 | 55 |
Intestinal metaplasia | ||
AUC | 0.604 | 0.634 |
< 0.001 | < 0.001 | |
HpIgG cutoffa | 0.30 | 17.53 |
Sensitivity (%) | 75 | 74 |
Specificity (%) | 46 | 48 |
Gastric adenoma | ||
AUC | 0.553 | 0.541 |
0.030 | 0.097 | |
HpIgG cutoffa | 0.40 | 18.35 |
Sensitivity (%) | 71 | 70 |
Specificity (%) | 41 | 43 |
Gastric cancer | ||
AUC | 0.555 | 0.575 |
0.003 | < 0.001 | |
HpIgG cutoffa | 0.21 | 19.33 |
Sensitivity (%) | 74 | 66 |
Specificity (%) | 36 | 48 |
Values are measured using GENEDIA® (GENEDIA
The HpIgG positivity rates by age and sex were analyzed (Table 4). The results showed that males had higher HpIgG positivity rates compared to females across all age groups in both kits, and the highest positivity rates were observed in the 40 to 69 age group for both sexes. The results from the two kits were similar for individuals under 40 and those aged 40 to 69, while some differences were observed between the two kits in males aged 70 and above, that the HpIgG positivity rate was higher with GastroPanel® compared to GENEDIA® in the group of males aged 70 and older.
Table 4 . Anti-
Variable | Total population | Male | Female | ||||||
---|---|---|---|---|---|---|---|---|---|
Positive | Negative | Positive | Negative | Positive | Negative | ||||
GENEDIA® | Total | 651 (60.4) | 426 (39.6) | 428 (65.6) | 224 (34.4) | 223 (52.5) | 202 (47.5) | ||
Age (yr) | |||||||||
< 40 | 50 (45.5) | 60 (54.5) | 31 (58.5) | 22 (41.5) | 19 (33.3) | 38 (66.7) | |||
40-69 | 483 (64.2) | 270 (35.8) | 318 (69.3) | 142 (30.7) | 165 (56.3) | 128 (43.7) | |||
≥ 70 | 118 (55.1) | 96 (44.9) | 79 (56.8) | 60 (43.2) | 39 (52.0) | 36 (48.0) | |||
GastroPanel® | Total | 659 (61.2) | 418 (38.8) | 442 (67.8) | 210 (32.2) | 217 (51.1) | 208 (48.9) | ||
Age (yr) | |||||||||
< 40 | 49 (44.5) | 61 (55.5) | 30 (56.6) | 23 (43.4) | 19 (33.3) | 38 (66.7) | |||
40-69 | 479 (63.7) | 274 (36.3) | 321 (69.9) | 139 (30.1) | 158 (53.9) | 135 (46.1) | |||
≥ 70 | 131 (63.7) | 83 (38.8) | 91 (65.5) | 48 (34.5) | 40 (53.3) | 35 (46.7) |
Values are presented as number (%). Values are measured using GENEDIA® (GENEDIA
As previously mentioned, a total of 142 discrepancy cases were observed: 67 cases were positive only in the GENEDIA® test, while 75 cases were positive only in the GastroPanel® test (Table 5). An analysis of such discrepancy between the two kits revealed that individuals in the discrepant group were more likely to have a history of prior
Table 5 . Subgroup analysis of discrepancy cases
Variable | ||||||
---|---|---|---|---|---|---|
(n = 584) | (n = 67) | (n = 75) | (n = 350) | |||
Age (yr) | 58.15 ± 12.43 | 59.01 ± 11.97 | 62.09 ± 12.63 | 56.72 ± 14.70 | 0.012 | |
Sex | < 0.001 | |||||
Male | 389 (66.6) | 39 (58.2) | 53 (70.7) | 171 (48.7) | ||
Female | 195 (33.4) | 28 (41.8) | 22 (29.3) | 179 (51.3) | ||
Atrophic gastritis | < 0.001 | |||||
Present | 314 (65.4) | 25 (52.1) | 30 (51.7) | 85 (31.5) | ||
Absent | 166 (34.6) | 23 (47.9) | 28 (48.3) | 185 (68.5) | ||
Intestinal metaplasia | < 0.001 | |||||
Present | 337 (63.8) | 26 (48.1) | 32 (53.3) | 114 (39.2) | ||
Absent | 191 (36.2) | 28 (51.9) | 28 (46.7) | 177 (60.8) | ||
Gastric adenoma | 0.010 | |||||
Present | 107 (18.3) | 12 (17.9) | 11 (14.7) | 36 (10.3) | ||
Absent | 477 (81.7) | 55 (82.1) | 64 (85.3) | 315 (89.7) | ||
Gastric cancer | 0.002 | |||||
Present | 222 (38.0) | 17 (25.4) | 26 (34.7) | 94 (26.8) | ||
Absent | 362 (62.0) | 50 (74.6) | 49 (65.3) | 257 (73.2) | ||
Previous history of | < 0.001 | |||||
Present | 68 (11.9) | 17 (27.0) | 19 (27.1) | 50 (14.9) | ||
Absent | 504 (88.1) | 46 (73.0) | 51 (72.9) | 285 (85.1) | ||
HpIgG titer on GENEDIA® (OD) | 1.88 ± 0.84 | 0.80 ± 0.52 | 0.19 ± 0.11 | 0.09 ± 0.09 | < 0.001 | |
HpIgG titer on GastroPanel® (EIU) | 272.60 ± 458.09 | 16.41 ± 0.82 | 27.42 ± 20.17 | 15.65 ± 0.73 | < 0.001 |
Values are presented as number (%) or mean ± SD. Values are measured using GENEDIA® (GENEDIA
In this study, we compared the diagnostic accuracy of
As mentioned earlier, HpIgG titer testing can be used to assess the density of colonized
It should be noted that the test results from the two kits were not entirely consistent. As mentioned, the rate of discrepancies was higher in individuals without AG or IM, and with a prior history of
An analysis of the 142 cases with discrepant results between the two kits revealed that individuals in the discrepant group were more likely to have a history of prior
In the analysis by age and sex, both kits showed the highest HpIgG positivity rate in the 40 to 69 age group, and the positivity rate was significantly higher in males compared to females across all age ranges. In a recent nationwide multicenter study in Korea, the
Our present study has several limitations. First, in comparing the GastroPanel®, the GENEDIA® kit was used instead of histology, as endoscopic biopsy for
In conclusion, GastroPanel® and GENEDIA® showed similar performance in terms of diagnostic accuracy though the test results from the two kits did not match perfectly. A large-scale validation study in Koreans is needed.
This work was supported by Seoul National University Bundang Hospital Research fund (06-2024-0143). In addition, the clinical study was supported by Dow Biomedica. The funders had no role in study design, data collection and analysis, decision to publish or preparation of the manuscript.
No potential conflicts of interest were disclosed.
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