Could Galectin 3 Be a Good Prognostic Factor in Endometrial Cancer?
Abstract
:1. Introduction
2. Material and Methods
- 55 had two-component HRT—estrogen/progesterone
- 3 patients were taking tibolone—estrogen/progesterone/androgen
3. Results
3.1. Characteristics of Patients in Terms of Endometrial Cancer Risk Factors
3.2. Comparative Analysis of Galectin 3 Concentrations Depending on the Stage and the Grade of Cancer
3.3. The Analysis to Confirm the Applicability of Galectin 3 as a Good Diagnostic Test
3.4. DFS and OS
- median baseline galectin 3 level
- 75th percentile of baseline galectin 3 levels
- 95th percentile of baseline galectin 3 levels
- baseline galectin 3 level cutoff level.
3.5. Univariate and Multivariate Logistic Regression Analysis
4. Discussion
5. Conclusions
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
References
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Characteristic | Median | 95% CI | |
---|---|---|---|
144 | Age | 56.2 | (48.2–61.3) |
36 | Nullipara | 17.1 | (14.0–26.2) |
81 | Never smoking | 16.3 | (15.1–23.8) |
63 | Current smoker | 17.2 | (14.9–19.6) |
71 | Diabetic (yes) | 21.1 | (16.3–22.8) |
73 | Diabetic (no) | 16.8 | (14.2–17.1) |
86 | Hormonal replacement therapy (never) | 17.2 | (15.5–19.9) |
58 | Hormonal replacement therapy | 18.4 | (16.7–21.8) |
89 | Hypertension (yes) | 19.1 | (16.3–23.0) |
55 | Hypertension (no) | 17.2 | (15.5–20.7) |
67 | Obesity (yes) | 21.6 | (18.0–24.6) |
77 | Obesity (no) | 16.4 | (16.2–18.1) |
65 | CRP < 5 | 14.9 | (13.2–19.1) |
79 | CRP > 5 | 18.6 | (16.3–22.5) |
Subgroups | Distribution | Numbers |
---|---|---|
The histopathological type | Endometrial endometrioid adenocarcinoma | 64 |
Nonendometrioid adenocarcinoma | 18 | |
Histopathological grade of the tumor | G1 | 26 |
G2 | 35 | |
G3 | 21 | |
Clinical stage of the tumor | FIGO I and II | 61 |
FIGO III and IV | 21 | |
Lymphovascular space (LVSI) invasion | Yes | 45 |
No | 39 | |
Lymph node metastases | With lymph node metastases | 33 |
Without lymph node metastases | 51 |
Median <17.8 | Median >=17.8 | Cutoff <16.2 | Cutoff >=16.2 | |
---|---|---|---|---|
36 months | n = 52 | n = 14 | n = 55 | n = 11 |
5 years | n = 45 | n = 8 | n = 46 | n = 7 |
Mean survival | 57.1 months | 50.3 months | 58.4 months | 48.2 months |
n Patients | Pathological Stage | Pathological Findings | Median (95%CI) [ng/mL] |
---|---|---|---|
7 | IA | LVSI (−), G1 | 15.7 (13.1–16.0) |
5 | IA | LVSI (+), G1 | 15.6 (14.4–19.2) |
9 | IA | LVSI (+), G2-G3 | 16.8 (16.5–18.9) |
3 | IB | LVSI (−), G1 | 17.2 (16.1–19.5) |
2 | IB | LVSI (+), G1 | 16.5 (15.0–17.1) |
8 | IB | LVSI (−), G2-G3 | 17.9 (17.8–19.2) |
9 | IB | LVSI (+), G2-G3 | 18.4 (17.2–20.3) |
2 | IIA | LVSI (−), G1 | 18.1 (17.2–20.6) |
2 | IIA | LVSI (−), G2-G3 | 19.4 (15.8–21.0) |
3 | IIA | LVSI (+), G1 | 18.6 (17.1–20.9) |
3 | IIA | LVSI (+), G2-G3 | 20.2 (19.4–23.1) |
2 | IIB | LVSI (−), G1 | 19.9 (18.7–21.6) |
2 | IIB | LVSI (+), G1 | 20.7 (19.5–22.1) |
2 | IIB | LVSI (−), G2-G3 | 21.5 (19.8–22.3) |
12 | IIIA | LVSI (+), G2-G3 | 22.2 (19.7–23.1) |
6 | IIIB | LVSI (+), G2-G3 | 22.6 (18.9–22.8) |
3 | IVA | LVSI (+), G2-G3 | 25.2 (21.6–24.8) |
Univariate Analysis (Cox Regression Model) | ||||||
PFS | OS | |||||
HR | 95% CI | p | HR | 95% CI | p | |
Age | 2.11 | (1.6–2.4) | 0.003 | 1.38 | (1.20–1.53) | 0.0367 |
Stage III, IV vs. I, II | 3.63 | (3.0–3.86) | 0.002 | 3.04 | (2.78–3.21) | 0.0113 |
Grade 3 vs. 1 | 2.09 | (1.71–2.61) | 0.021 | 1.94 | (1.69–2.09) | 0.0062 |
Galectin 75th percentile | 1.62 | (1.38–1.68) | 0.0042 | 1.38 | (1.16–1.41) | 0.0562 |
Galectin 95th percentile | 1.71 | (1.55–1.82) | 0.0031 | 1.30 | (1.22–1.49) | 0.0076 |
Galectin median | 1.41 | (1.31–1.66) | 0.003 | 1.22 | (1.06–1.37) | 0.026 |
Galectin cutoff | 1.54 | (1.43–1.61) | 0.0004 | 1.48 | (1.24–1.62) | 0.0091 |
Multivariate Analysis (Cox Regression Model) | ||||||
DFS | OS | |||||
HR | 95% CI | p | HR | 95% CI | p | |
Galectin median | 1.18 | (0.96–1.32) | 0.026 | 1.21 | (1.08–1.3) | 0.0216 |
Galectin 75th percentile | 1.23 | (1.12–1.39) | 0.612 | 1.12 | (1.04–1.34) | 0.1542 |
Galectin 95th percentile | 1.08 | (0.99–1.21) | 0.054 | 1.29 | (1.12–1.46) | 0.048 |
Galectin cutoff | 1.63 | (1.41–1.80) | 0.008 | 1.46 | (1.20–1.55) | 0.022 |
Laparoscopy | Laparotomy | p | ||||
---|---|---|---|---|---|---|
G1 n = 20 | G2 n = 22 | G3 n = 5 | G1 n = 6 | G2 n = 13 | G3 n = 16 | – |
FIGO 1 + 2 n = 41 | FIGO 3 + 4 n = 6 | FIGO 1 + 2 n = 20 | FIGO 3 + 4 n = 15 | – | ||
Lymph nodes invasion YES n = 11 | Lymph nodes invasion NO n = 36 | Lymph nodes invasion YES n = 22 | Lymph nodes invasion NO n = 15 | – | ||
DFS n = 27.6 | DFS n = 28.1 | 0.0612 | ||||
OS n = 49.3 | OS n = 52.6 | 0.0508 |
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Cymbaluk-Płoska, A.; Gargulińska, P.; Kwiatkowski, S.; Pius-Sadowska, E.; Machaliński, B. Could Galectin 3 Be a Good Prognostic Factor in Endometrial Cancer? Diagnostics 2020, 10, 635. https://doi.org/10.3390/diagnostics10090635
Cymbaluk-Płoska A, Gargulińska P, Kwiatkowski S, Pius-Sadowska E, Machaliński B. Could Galectin 3 Be a Good Prognostic Factor in Endometrial Cancer? Diagnostics. 2020; 10(9):635. https://doi.org/10.3390/diagnostics10090635
Chicago/Turabian StyleCymbaluk-Płoska, Aneta, Paula Gargulińska, Sebastian Kwiatkowski, Ewa Pius-Sadowska, and Bogusław Machaliński. 2020. "Could Galectin 3 Be a Good Prognostic Factor in Endometrial Cancer?" Diagnostics 10, no. 9: 635. https://doi.org/10.3390/diagnostics10090635
APA StyleCymbaluk-Płoska, A., Gargulińska, P., Kwiatkowski, S., Pius-Sadowska, E., & Machaliński, B. (2020). Could Galectin 3 Be a Good Prognostic Factor in Endometrial Cancer? Diagnostics, 10(9), 635. https://doi.org/10.3390/diagnostics10090635