Predicting factors of central lymph node metastasis and BRAF^V600E mutation in Chinese population with papillary thyroid carcinoma

All PTC patients in the present study who underwent either total thyroidectomy or near-total thyroidectomy in Henan Provincial People’s Hospital between October 2014 and October 2016. The medical records of these patients were retrospectively analyzed. The histopathlogic examinations of all patient were performed by two experienced pathologists independently and a consensus was made blinded to BRAF^V600E status. Only conventional PTC that with papillae structure and PTC-type nuclei features were enrolled in the present study. In total, 943 patients were recruited for this study [men: 233, mean age(average ± standard deviation), 52.0 ± 11.6 years; women: 710, mean age, 45.4 ± 11.6 years]. None of these patients received radioactive iodine¹³¹ therapy before surgery. The preoperative levels of free triiothyronine, free thyroxine, thyroid-stimulating hormone, thyroglobulin antibodies, and thyroid peroxidase antibodies were detected by radioimmunoassay. Hashimoto’s thyroiditis (HT) was confirmed based on the postoperative pathologic findings and an elevated preoperative serum thyroid autoantibody level. Clinicopathologic staging was classified based on the 8th edition of the tumor-node-metastasis (TNM) staging published by the American Joint Committee on Cancer. The mean follow-up duration was 27 postoperative months (range = 11–44 months). At the time of follow-up, only one patient died of breast cancer.

Genomic DNA isolated from paraffin-embedded tissues of PTC patients. The paraffin-embedded tissue blocks of tumor tissue was sectioned for hematoxylin and eosin staining with the purpose of identifying pathological diagnosis. Regions with neoplastic compositions of 80% or greater were marked as tumor tissue under optical microscope. Depending on the size of the tissue, 3–4 pieces of 5-μm-thick sections of each block were manually microdissected using a needle and collected into 1.5 ml microtubes for DNA extraction. The Genomic DNA isolation process was performed using the Puregene Tissue Kit (Qiagen, Valencia, CA, USA), according to the manufacturer’s instructions. The absorbance of the DNA samples was measured using a spectrophotometer, and only the A260/A280 values between 1.8 and 2.0 were accepted for the next step. The extracted DNA was stored at – 80 °C for next procedure. The status of the BRAF^V600E mutation of each sample was examined by qRT-PCR using the AmoyDx BRAF^V600E Mutation Detection Kit (Amoy Diagnostics, Xiamen, China), and the presence of the mutation was evaluated following the manufacturer’s instructions. The sample was classified as mutation-positive when the cycle threshold (Ct) was ≤ 28 and as negative when Ct was > 28.

All statistical analyses in the present study were conducted using SPSS 21 (IBM Corporation, Waltham, NY, USA). Enumeration data were presented as frequencies and were compared utilizing the chi-squared or Fisher’s exact test. Measurement data were presented as means ± standard deviation and using the independent sample t test for variables for normal distribution and Mann-Whitney for non-normal distribution. The effects of the clinicopathologic factors on central lymph node metastasis (CLNM) and BRAF^V600E mutation were evaluated using univariate and multivariate logistic-regressions. For all test, a probability value of < 0.05 was considered statistically significant.

The clinical and pathological characteristics of the 943 patients are shown in Table 1. There were 233 (25%) male patients and 710 (75%) female patients, and the male-to-female ratio was 1:3.0. The age of the patients ranged from 15 to 77years, with an average age of 45.9 ± 11.3 years. The tumor size ranged from 1 to 50 mm, and the average size was 1.2 ± 0.9 mm. There were 688 patients with unifocality (73%) and 255 patients with multifocality (n ≥ 2) (27%). HT was rare among the PTC patients (5%, 50/943). CLNM was common among the PTC patients, with a frequency of 53% (504/943). The proportions of patients diagnosed with stage T1, T2, and T3 disease were 89% (838/924), 8% (80/943), and 3% (25/943), respectively. In total, there were 856 (91%) patients in TNM stage I and 87 (9%) patients in stage II. The BRAF^V600E mutation rate was 85% (806/943).

Of the 943 PTC patients, there were 373 (40%) patients with PTC > 10 mm and 570 (60%) PTMC patients (Table 1). The average tumor sizes were 2.0 ± 1.0 mm and 0.6 ± 0.2 mm, respectively (P < 0.001). The univariate analysis revealed that there were more male patients (P = 0.02), more patients with CLNM (P < 0.001), and higher TNM stages (P < 0.001) in the PTC > 10 mm group than in the PTMC group. The multivariate analysis revealed that only CLNM was significantly correlated with PTC > 10 mm [P < 0.001, odds ratio (OR) = 4.10, 95% confidence interval (95% CI) 3.04–5.53]. Even though the frequency of the BRAF^V600E mutation was slightly higher in the PTMC group (87%) than in the PTC > 10 mm group (83%), there was no statistically significant difference (P = 0.074). No difference was found in age, tumor size, or HT between the two groups.

The relationships between CLNM and the clinicopathological characteristics of the PTC patients are shown in Table 2. Both univariate and multivariate analyses revealed that the risk for CLNM was significantly associated with male, younger age, and larger tumor size among PTC patients, regardless of the tumor size (P < 0.05). In addition, in both the overall and PTC > 10 mm groups, the positive rate of CLNM was significantly decreased in PTC patients with coexistent HT compared with patients without HT, which suggested that coexistent HT might be a protective factor against CLNM in the PTC patients (P = 0.002). Furthermore, advanced T stage was also a risk factor for CLNM in the PTC patients (P < 0.001, OR = 4.94, 95% CI 2.84–8.59).

Since both age and tumor size were the predictive factors of CLNM in PTC patients, it is necessary to try to find out the precise boundary that associated with CLNM. The relationship between CLNM and both patient age and tumor size was further analyzed using 10 years as an increment for age and 5 mm as an increment for tumor size (Table 3). It is interesting that all patients ≤ 30 years of age in the PTC > 10 mm group were positive for CLNM (100%, 51/51), and although the positivity rate decreased as age increased, it remained high at 60% (P < S0.001). In the PTMC group, the frequency of CLNM was 66% (29/44) in patients ≤ 30 years of age; however, it decreased dramatically with increasing age (P = 0.001). Regarding tumor size, the frequency of CLNM was only 31% (78/248) when the tumor size was ≤ 5 mm, and it increased with increasing tumor size. When the tumor size was > 20 mm, the rate of CLNM was greater than 80% (P < 0.001).

The relationship between the BRAF^V600E mutation and the clinicopathological characteristics of the PTC patients are detailed in Table 4. In the overall PTC group, the incidence of BRAF^V600E mutation was statistically correlated with older age (P = 0.03), tumor size (P = 0.04), coexistent HT (P = 0.002), and early T stage (P = 0.02) but not with gender, multifocality, CLNM, or TNM stage. Multivariate analysis found that only age (P < 0.001, OR = 1.04, 95% CI 1.02–1.06) and coexistent HT (P = 0.005, OR = 0.35, 95% CI 0.17–0.73) were independent predictive factors of BRAF^V600E mutation status. In addition, both univariate and multivariate analyses uncovered that age (P = 0.004, OR = 1.03, 95% CI = 1.01–1.06) was a risk factor for BRAF^V600E mutation in the PTC > 10 mm group. Moreover, in the PTMC group, the BRAF^V600E mutation was significantly correlated with tumor size (P < 0.001, OR = 8.19, 95% CI = 2.73–24.57) and coexistent HT (P = 0.03, OR = 0.42, 95% CI = 0.19–0.92) by both univariate and multivariate analyses.

The relationships between the BRAF^V600E mutation among age and tumor size were also further analyzed using 10 years as an increment for age and 5 mm as an increment for tumor size (Table 5). The BRAF^V600E mutation rate was maintained above 85% in the PTMC group, regardless of age. However, in the PTC > 10 mm group, the BRAF^V600E mutation rate was only 65% in patients ≤ 30 years of age (P = 0.003), and it rapidly increased to more than 85% in patients > 30 years of age. Furthermore, compared with tumor size ≤ 5 mm, the frequency of BRAF^V600E mutation was significantly higher (91%, 294/322) when the tumor size was in the 5–10 mm range (P < 0.001). The frequency of the BRAF^V600E mutation remained relatively high when the tumor size was > 10 mm.

The relationships among CLNM, tumor size, and BRAF^V600E mutation status are shown in Table 6. When the tumor size was ≤ 5 mm, the incidence of CLNM was significantly higher in BRAF^V600E mutation-positive patients than in mutation-negative patients (P = 0.009). When the tumor size was > 5 mm, there was no significant difference in CLNM rates between BRAF^V600E mutation-positive patients and mutation-negative patients.