Journal List > J Gynecol Oncol > v.29(1) > 1093911

Jiang, Xiang, Pei, He, Shen, Wu, and Yang: Mutational analysis of KRAS and its clinical implications in cervical cancer patients

Abstract

Objective

The predictive and prognostic role of KRAS mutations in cervical cancer remains inconclusive. The aim of this study was to explore the clinicopathological and prognostic relevance of KRAS mutations in invasive cervical cancers (ICC).

Methods

Reverse transcription polymerase chain reaction (PCR) and Sanger sequencing were employed to detect KRAS mutations in 876 ICC patients. Quantitative real-time PCR was used to detect human papillomavirus (HPV) 16 and HPV 18.

Results

Non-synonymous mutations of KRAS were identified in 30 (3.4%) patients. These mutations were more common in non-squamous cell carcinoma than in squamous cell carcinoma (SCC) (8.2% vs. 2.2%, respectively, p<0.001) and were associated with HPV 18 infection (p=0.003). The prevalence of mutations was highest (18.2%) in the uncommon histological subtypes followed by adenocarcinoma (AC, 7.3%) and adenosquamous carcinoma (ASC, 5.8%). During the median follow-up of 55 months, compared to patients with wild-type KRAS, a greater percentage of patients with mutant KRAS relapsed (20.0% vs. 42.9%, respectively, p=0.007). The 3-year relapse-free survival was poorer in patients with mutant KRAS than in patients without KRAS mutations (57.1% vs. 81.9%, respectively, p=0.001). Furthermore, the multivariate analysis showed that the presence of a KRAS mutation was an independent predictor for disease recurrence (hazard ratio [HR]=2.064; 95% confidence interval [CI]=1.125–3.787; p=0.019).

Conclusion

KRAS mutations were predominant in non-SCCs of the cervix and were associated with HPV 18 infection. A combination of KRAS mutation detection and HPV genotyping would be useful in identifying patient with poor prognosis for further interventions.

INTRODUCTION

In China, cervical cancer is the eighth leading cause of cancer-related death among women and is responsible for more than 20,000 deaths annually [1]. Despite improvements in cervical cancer screenings and treatments over the past 50 years, the incidence and mortality rates of cervical cancer in China have increased annually since 2000 [2]. Treatment of advanced or recurrent cervical cancer is still limited, resulting in poor survival [3]. Targeted therapy based on oncogenic mutations might be a potential approach to improve treatment outcomes.
The KRAS protein functions as a GTPase and plays a vital role in regulating cell differentiation, proliferation, and survival [45]. Somatic KRAS mutations can be detected in approximately 30% of all human cancers [6]. The three most common residues for KRAS mutations—G12, G13, and Q61—are responsible for intrinsic and GAP-induced GTP hydrolysis; point mutations at these residues can lead to the accumulation of cellular GTP-bound RAS, which activates downstream signaling pathways [6]. KRAS mutations have been confirmed as a promising prognostic marker in non-small cell lung cancer (NSCLC) and colorectal cancer (CRC) [789]. In a large cohort of patients with CRC, the multicenter Refractory Angina Spinal Cord stimulation and usuAL care (RASCAL) study demonstrated that the KRAS G12V mutation exerted more aggressive properties than other KRAS mutations regarding disease recurrence and death [1011]. In BRAF wild-type CRC, Imamura reported that a mutation at KRAS codon 12 but not at KRAS codon 13 was associated with reduced survival [12]. Thus, different KRAS mutations may have distinct clinical responses.
To date, RAS proteins have not yielded any successful targeted therapies and have been viewed as “undruggable” for many years. Some drugs have been designed to block pathways downstream of RAS, such as RAF, MAPK-MEK, and ERK; however, their efficacy has been generally disappointing [131415]. Nevertheless, the patient's KRAS mutation status has been confirmed to be a criterion for implementing treatment with anti-epidermal growth factor receptor (EGFR) antibodies [16], as this treatment modality is more successful in patients with RAS wild-type metastatic CRC than in patients with mutant RAS. The combination of a MEK inhibitor and a fibroblast growth factor receptor 1 (FGFR1) inhibitor leads to tumor cell death in KRAS-mutant lung cancer cells but not in corresponding KRAS wild-type cells [17]. Thus, detecting KRAS mutations has been shown to be useful in selecting patients who could benefit from some of the available targeted treatments.
KRAS mutation has been identified as the second common oncogenic mutation following PIK3CA in our previous comprehensive analysis of 16 targetable oncogenic mutations in 285 cervical cancers [18]. In this study, a larger cohort of patients with cervical cancer (876 patients) were enrolled to explore its association with clinicopathological characteristics and prognosis over a longer follow-up period as well as to determine the relevance of human papillomavirus (HPV) infection in the incidence of KRAS mutations.

MATERIALS AND METHODS

1. Patient data

This study was approved by the Ethics Committee at the Fudan University Shanghai Cancer Center (FUSCC 050432-4-1212B) and was conducted in accordance with the approved guidelines. Patients with cervical cancer were enrolled between January 1, 2010 and December 30, 2012 if they satisfied the following conditions: pathologically determined primary cervical carcinomas, stages IB1–IIA2 disease according to the 2009 International Federation of Gynecology and Obstetrics (FIGO) staging system, and no prior neoadjuvant chemotherapy or radiation. Cervical tumor specimens were collected during either radical hysterectomy or trachelectomy procedures and stored at −80°C in RNAlater solution (Ambion; Thermo Fisher Scientific, Waltham, MA, USA). After the specimens were assessed by 2 independent pathologists (Xuxia Shen and Wentao Yang), those with either insufficient tumor material for a comprehensive mutational analysis or fewer than 50% malignant cells within the entire tissue sample were excluded. In total, 876 patients were eligible for this study. Among these, 553 patients received adjuvant therapy after surgery according to the guidelines, including 64 patients who received pelvic radiotherapy alone, 68 patients who received chemotherapy alone and 421 patients who received concurrent chemoradiation with or without subsequent systemic chemotherapy. The specific clinicopathological characteristics, including age, menopausal status, histological type, tumor size, depth of myometrial invasion, lymphovascular space involvement (LVSI), regional lymph node metastasis, parametrial involvement, and distant metastasis, were recorded. The patients were followed up for disease recurrence and survival duration either in the clinic or by telephone. All patients provided written informed consent for the analysis of their tumor specimens and the collection of clinical information.

2. Detection of KRAS mutations

Genomic DNA and total RNA were extracted from the tumor tissues using a DNA/RNA isolation kit (Tiangen Biotech, Beijing, China) according to the manufacturer's instructions. cDNA was obtained by reverse transcribing 2 μg of total RNA using an M-MLV Reverse Transcriptase kit (Invitrogen, Waltham, MA, USA) and was used for mutational analysis and HPV detection. Mutational analyses were conducted according to our previous protocol [18]. KRAS (exons 1–4) was amplified using KOD-Plus-Neo DNA polymerase (Toyobo, Tokyo, Japan) with the following primers: KRAS-F:CCATTTCGGACTGGGAGCGA, and KRAS-R: GGCATCATCAACACCCA GAT. The polymerase chain reaction (PCR) products were directly sequenced using the Sanger sequencing technique, and all mutations were confirmed by an additional independent PCR experiment.

3. Quantitative real-time PCR assay for the detection of HPV

A TaqMan quantitative real-time PCR assay was used to detect HPV 16 and HPV 18 [19] using the following primers: HPV 16 (F: 5'GAACCGAAACCGGTTAGTATAA 3', R: 5'ATGTATAGTTGTTTGCAGCTCTGT3') and HPV 18 (F: 5'GGACCGAAAACGGTGTATATAA 3', R: 5'CAGTGAAGTGTTCAGTTCGGT 3'). The probes for HPV 16 and HPV 18 were CATTTTATGCACCAAAAGAGAACTGCAATGTTTC and ATGTGAGAAACACACCACAATACTATGGCGCG, respectively. The PCR reaction (10 μL) comprised 5 μL of Premix Ex Taq™; 1 μL of Primer Mix (10 μM); 1 μL of Probe Mix (40 nM for HPV 16, 200 nM for HPV 18); 1 μL of sample cDNA and 2 μL of dH2O. The PCR was performed on an ABI 7500 instrument (Applied Biosystems, Foster City, CA, USA) as follows: denaturation step at 95°C for 30 seconds and 40 cycles of 5 seconds at 95°C, 10 seconds at 55°C, and 20 seconds at 72°C.

4. Statistical analysis

All statistical analyses were performed using IBM SPSS statistics software, version19 (IBM Corporation, New York, NY, USA). Either the χ2 test or Fisher's exact test was used to analyze the association between KRAS mutations and the patients' clinicopathological characteristics. Relapse-free survival (RFS) was defined as the period from the completion of surgery to the date of documented evidence of disease recurrence. The end of the observation period was March 31, 2016, and patients without disease recurrence were censored at their last follow-up visit. Survival curves were calculated using the Kaplan-Meier method, and differences between the groups were tested using the log-rank test. The Cox proportional hazards model was used for multivariate survival analysis. Statistical significance was set at p<0.050.

RESULTS

1. Characterization of KRAS mutation in cervical cancers

Among 876 patients, 30 non-synonymous mutations of KRAS were identified (3.4%), the majority (86.7%, 26/30) of which were found on exon 2. Ten percent (3/30) of the mutations were located on exon 3, and only one (3.3%) mutation existed on exon 4. The detailed mutation and clinicopathological information were provided in Supplementary Table 2. Fig. 1 demonstrated the distribution of the mutation sites in KRAS-mutant carcinomas. The G12 residue on KRAS was the most frequently mutated (17/30, 56.7%) followed by G13 (4/30, 13.3%). KRAS G12 mutations are predominant in non-squamous cell carcinomas (SCCs) (73.3%), and the rates of KRAS G12 & G13 mutations in SCC were 40% and 20%, respectively. A mutation of residue Q61 was only found in one patient in this cohort despite its status as a common mutation of KRAS in other human cancers [6]. In addition, 3 novel KRAS mutations (G15C, S39Y, and F156Y), which have not been previously described in cervical cancer according to the Catalogue of Somatic Mutations in Cancer (COSMIC) database (http://cancer.sanger.ac.uk/cancergenome/projects/cosmic; Jun 8, 2017), were identified in our patient cohort.
Fig. 1
Identification of KRAS mutation hotspots in cervical cancers. (A) KRAS mutations identified in 30 cervical cancers. (B) KRAS mutations identified in 15 non-SCCs. (C) KRAS mutations identified in 15 SCCs.
SCC, squamous cell carcinoma.
jgo-29-e4-g001

2. Clinicopathological association of KRAS mutations

Table 1 summarizes the association between KRAS mutations and the patients' clinicopathological characteristics. KRAS mutations were more common in non-SCC than in SCC (8.2% vs. 2.2%, p<0.001). The highest prevalence of mutations (18.2%) occurred in uncommon histological subtypes (neuroendocrine carcinoma, clear cell carcinoma, carcinosarcoma, and poorly differentiated carcinoma) followed by adenocarcinoma (AC; 7.3%), adenosquamous carcinoma (ASC; 5.8%), and SCC (2.2%) (p<0.001, Table 1).
Table 1

Association between KRAS mutations and clinicopathological parameters

jgo-29-e4-i001
Variables Cases KRAS mutation status p-value (χ2 test)
Wild-type (n=846) Mutant (n=30)
Age (yr) 0.664
<47 404 389 15
≥47 472 457 15
Menopausal status 0.688
Premenopausal 556 538 18
Postmenopausal 320 308 12
HPV infectious* 0.003
HPV 16 487 477 10
HPV 18 136 125 11
HPV 16 & 18 8 8 0
Negative 245 236 9
Histological subtypes <0.001
SCC 693 678 15
AC 109 101 8
ASC 52 49 3
Others 22 18 4
FIGO stage 0.673
IB 434 418 16
IIA 442 428 14
Node status 0.525
Negative 629 609 20
Positive 247 237 10
Tumor sizes (cm) 0.698
>4 264 254 10
≤4 612 592 20
Depth of myometrial invasion 0.745
Whole thickness 279 268 11
>1/2 349 339 10
≤1/2 248 239 9
LVSI 0.097
Yes 331 324 7
No 545 522 23
Parametrial involvement 0.081
Yes 49 45 4
No 827 801 26
AC, adenocarcinoma; ASC, adenosquamous carcinoma; FIGO, International Federation of Gynecology and Obstetrics; HPV, human papillomavirus; LVSI, lymphovascular space involvement; SCC, squamous cell carcinoma.
*Eight Cases positive for both HPV 16 & 18 were excluded in χ2 test. All the 8 cases were negative for mutations. Others include neuroendocrine carcinoma (16), clear cell carcinoma (2), carcinosarcoma (2), and poorly differentiated carcinoma. Fisher's exact test was used.
Either HPV 16 or HPV 18 was detected in 631 patients (71.9%), with 487 (55.6%) patients positive for HPV 16, 136 (15.5%) patients positive for HPV 18, and 8 (0.9%) patients positive for both. HPV 18 positive patients were more likely to harbor a KRAS mutation than either HPV 16 positive or negative patients (8.1% vs. 2.1% vs. 3.7%, respectively, p=0.003, Table 1). KRAS mutations were not found to correlate with other clinicopathological characteristics such as lymph node metastasis, larger tumor size, deep myometrial invasion and the presence of LVSI.

3. The association between KRAS mutation and treatment outcome

A total of 767 (87.6%) patients were included in the survival analysis with a median follow-up duration of 55 months (range: 1–75 months). Disease recurrence was documented in 160 patients (20.9%) during the follow-up intervals, with 12 (42.9%) of 28 patients with mutant KRAS experiencing recurrence during follow-up; this rate was significantly higher than rate of patients with wild-type KRAS (20.0%, 148/739, p=0.007; Fisher's exact test). Detailed recurrence information was available for 759 patients. Distant metastasis outside of the pelvis was documented in 113 (14.9%) patients, and pelvic recurrence was documented in 39 patients (5.1%). In patients with a KRAS mutation, distant metastasis and pelvic recurrence within the surgical or radiation area were documented in 29.6% and 11.1% of the patients, respectively; these rates were significantly higher than those in patients with wild-type KRAS (14.3% and 4.9%, respectively, p=0.023). Furthermore, a significant relation was found between KRAS mutation and distant metastasis (p=0.016), but not for local recurrence (p=0.101) (Supplementary Table 1).
KRAS mutations were confirmed to be associated with patient survival in both univariate and multivariate analyses. The 3-year RFS of patients with mutant KRAS was significantly poorer than that of patients with wild-type KRAS (57.1% vs. 81.9%, respectively, p=0.001) (Fig. 2A). The multivariate analyses revealed that KRAS mutations were an independent predictor for worse RFS (hazard ratio [HR]=2.064; 95% confidence interval [CI]=1.125–3.787; p=0.019) (Table 2).
Fig. 2
Kaplan-Meier curve of RFS. (A) Kaplan-Meier curve of RFS of the 767 cervical cancer patients. (B) Kaplan-Meier curve of RFS of the 166 patients with non-SCCs. (C) Kaplan-Meier curve of RFS of the 118 patients with HPV 18 infections.
HPV, human papillomavirus; RFS, relapse-free survival; SCC, squamous cell carcinoma.
jgo-29-e4-g002
Table 2

Identification of predictors for disease-relapse survival by univariate and multivariate analysis in 767 patients with cervical cancer

jgo-29-e4-i002
Variables Univariate analyses Multivariate analyses
HR 95% CI p-value HR 95% CI p-value
Age (≥47 yr vs. <47 yr) 1.148 0.840–1.570 0.387
Postmenopause (yes vs. no) 1.187 0.866–1.627 0.287
HPV 16/18 infection (no vs. yes) 0.970 0.687–1.369 0.862
Histological subtypes (non-SCC vs. SCC) 1.766 1.261–2.473 0.001 1.983 1.401–2.808 <0.001
Tumor size (>4 cm vs. ≤4 cm) 1.521 1.103–2.097 0.010 1.175 0.847–1.631 0.334
FIGO stage (IIA vs. IB) 1.779 1.293–2.448 <0.001 1.307 0.935–1.827 0.117
Node status (yes vs. no) 3.569 2.615–4.870 <0.001 1.881 1.293–2.737 0.001
Depth of myometrial invasion (whole thickness vs. >1/2 vs. ≤1/2) 2.308 1.842–2.893 <0.001 1.628 1.257–2.108 <0.001
Parametrial involvement (yes vs. no) 4.252 2.809–6.438 <0.001 1.822 1.167–2.844 0.008
LVSI (yes vs. no) 2.835 2.058–3.905 <0.001 1.543 1.056–2.254 0.025
KRAS mutation (yes vs. no) 2.577 1.430–4.642 0.002 2.064 1.125–3.787 0.019
CI, confidence interval; FIGO, International Federation of Gynecology and Obstetrics; HPV, human papillomavirus; HR, hazard ratio; LVSI, lymphovascular space involvement; SCC, squamous cell carcinoma.
Furthermore, survival analysis was performed in patients with SCC or non-SCC. Among the 166 patients with non-SCC, the 3-year RFS was significantly poorer in patients with a KRAS mutation than in those with wild-type KRAS (46.7% vs. 75.5%, p=0.013) (Fig. 2B); however, this finding was not replicated in patients with SCC (Supplementary Fig. 1).
Among patients positive for HPV 18, those with a KRAS mutation had a shorter survival than patients with wild-type KRAS (3-year RFS: 40.0% vs. 85.2%, respectively, p=0.001). However, an association between KRAS mutations and RFS was not observed in patients positive for HPV 16 (p=0.478) (Fig. 2C).
In addition, the 3-year RFS was compared among 4 patients with KRAS G13 mutations and 17 patients with KRAS G12 mutations. A worse survival trend was revealed in patients harboring G13 mutations than in patients with KRAS G12 mutations (25.0% vs. 70.6%); however, due to the limited number of cases (21 cases), this difference was not statistically significant (p=0.153) (Supplementary Fig. 2).

DISCUSSION

The features of KRAS mutations in lung and colon cancer have become increasing clear, whereas the clinicopathological and prognostic characteristics of KRAS mutations in cervical cancer remain inconclusive. There are some uncertainties regarding the predictive and prognostic role of KRAS mutations in previous studies due to their relatively small sample sizes. In this study, with a large cohort of 876 patients with cervical cancer, KRAS mutations were found to be more associated with non-SCC and a positive HPV 18 infection status. In these specific subtypes of cervical cancer, patients with a KRAS mutation have a worse prognosis.
The development of a KRAS mutation is a rare event in SCCs of the cervix. According to the COSMIC database (http://cancer.sanger.ac.uk/cancergenome/projects/cosmic; Jun 8, 2017), the prevalence of KRAS mutations in SCC is approximately 2%, which was confirmed in our patient cohort (2.2%). In comparison, KRAS mutations were predominant in non-squamous cell cervical carcinomas, including AC, ASC, and other uncommon subtypes. Spaans et al. [20] demonstrated that KRAS mutations occurred more frequently in AC than in SCC (24% vs. 3%, p<0.001), and Wright et al. [21] indicated that KRAS mutations were detected only in AC but not in SCC (17.5% vs. 0%, p=0.010). In our cohort of patients with AC, the KRAS mutation rate of was 7.3% (8/110), which is similar to the results observed by Ojesina et al. [22] using whole exome sequencing of 24 patients with AC (2/24, 8%). Regarding neuroendocrine carcinomas, Frumovitz et al. [23] reported that the prevalence of KRAS mutations was 14% (6/44), which is lower than observed in this study (4/16, 25%). Due to its small sample size, both studies may have some bias. Thus, the reported prevalence of KRAS mutations in non-SCC is highly variable.
In the present study, KRAS mutations were detected in 3.4% (30/876) of Chinese patients with cervical carcinoma, which was relatively low compared with data from other studies. According to the COSMIC database, the frequency of KRAS mutations in cervical cancer is 5.83% (http://cancer.sanger.ac.uk/cancergenome/projects/cosmic; Jun 8, 2017). As the data above indicated, the distribution of the different histological subtypes accounts for the variance of the mutation rate among the studies [21]. In addition, the disease stage might also contribute to the low frequency of KRAS mutations in our cohort of cervical cancer patients. Wegman et al. [24] reported that KRAS mutations were more commonly found in patients with advanced stage disease (FIGO stages III–IV) than in those with early stage disease (FIGO stages I–II) (35.3% vs. 5.6%, respectively, p<0.001); however, all our patients were diagnosed with FIGO stages IB–IIA disease.
In accordance with the result of most studies, we confirmed that the 3-year RFS in patients with KRAS mutations was significantly lower than that in patients without KRAS mutations in our large patient cohort [182124]. Wegman et al. [24] found that among patients treated with definitive chemoradiation, those harboring mutant KRAS had significantly worse recurrence-free survival than those with wild-type KRAS (p=0.030). Our cohort of patients underwent surgery-based multimodal treatment, and disease recurrence outside of the pelvis was the primary recurrence pattern. Wegman et al. [24] reported that there was a significant association between KRAS mutation and distant metastases but not local recurrence, which is consistent with our previous findings. In clinic, the finding of the association between KRAS mutation and worse 3-year RFS suggests that detection of KRAS mutation could be used as a prognostic marker. Close follow-up is needed in those patients with KRAS mutation for early detection of recurrence. In addition to conventional adjuvant therapy, such as concurrent chemoradiation and systemic chemotherapy, further management might be considered in patients with KRAS mutation to prevent from recurrence. Novel therapy is needed to be identified including KRAS-targeted therapy.
An association between KRAS mutations and HPV infection has not been confirmed in the literature, as Wright et al. [21] did not observe an association between HPV infection and KRAS mutations in a cohort of 80 patients with cervical cancer. In our study, we demonstrated that KRAS mutations were associated with HPV 18 infection but not HPV 16 infection. Moreover, KRAS mutations were a predictor of poor disease-free survival (DFS) only in patients with HPV 18 infection. This result is consistent with the finding that an association between KRAS mutations and disease recurrence was only observed in patients with non-SCC but not with SCC. Epidemiological studies have confirmed that HPV 18 infection accounts for majority of cervical ACs. In this study, we found that HPV 18 infection was predominantly present in ACs (19.9%), ASCs (23.5%), and uncommon histological subtypes (8.1%) at significantly higher rates than HPV 16 infection (6.0%, 2.5%, and 0.4%, respectively, p<0.001). Compared to SCC, these specific histologic subtypes present poorer survival. Thus, a combination of KRAS mutation detection and HPV genotyping might be useful in identifying patient with poor prognosis for further interventions.
According to the literature, KRAS mutations at residues G12 and G13 have different risks of tumor progression in lung cancer and CRC [7892526]. The mechanism of different KRAS mutations on tumor progression has not been completely elucidated. It has been revealed that different amino acid changes result in the involvement of different signaling pathways [272829]. In this study, patients with mutant KRAS at codon 13 are more likely to have a shorter DFS than patients with mutant KRAS at codon 12, although this difference was not statistically significant. More cases are required to confirm these results. Functional studies of those KRAS mutations warrant further studies, especially for the newly identified mutants in cervical cancer.
There are some limitations in our study. First, eligible patients did not include those with advanced cervical cancer, and the frequency, clinicopathological features and prognostic relevance of KRAS mutations were obtained from patients with relatively early stage disease, which could lead to an incomplete analysis of KRAS mutations in cervical cancer. Second, the presence of concurrent mutations may also influence the clinical phenotype and prognostic outcomes. Our other study discovered a subset of cervical cancer patients with concurrent ERBB2, PIK3CA, and/or KRAS mutations (sent to publication). A study of a large patient cohort based on whole-genome sequencing is required to fully analyze oncogenic mutations in cervical cancer. Third, the detection of HPV was just limited in HPV 16 and HPV 18. Finally, because a small group of people died of cervical cancer, overall survival was not analyzed in our study.
In summary, KRAS mutations were predominant in non-SCC of the cervix and are associated with HPV 18 infection. These mutations were an independent predictor for disease recurrence in patients with cervical cancer who received surgery-based multimodal treatment. Further intervention might be necessary in patients with KRAS mutations because of their increased risk for recurrence and distant metastasis. A combination of KRAS mutation detection and HPV genotyping would be useful in identifying patient with poor prognosis for further interventions.

ACKNOWLEDGMENTS

The authors thank Wentao Yang for the contribution in histopathological diagnosis.

Notes

Funding The study was supported by grants from National Natural Science Foundation of China (81572803/81502236) and Key research project of Shanghai Municipal Commission of Health and Family Planning (201640010).

Conflict of Interest No potential conflict of interest relevant to this article was reported.

Author Contributions

  • Conceptualization: J.W., X.L., W.X., Y.H.

  • Data curation: J.W., X.L., P.X., H.T., S.X., Y.H.

  • Formal analysis: J.W., X.L., Y.H.

  • Funding acquisition: Y.H., X.L.

  • Investigation: J.W., Y.H.

  • Methodology: J.W., X.L., S.X., H.T., P.X.

  • Project administration: Y.H., X.L.

  • Resources: W.X., Y.H.

  • Software: J.W., P.X.

  • Supervision: Y.H., W.X.

  • Validation: W.X., Y.H.

  • Visualization: J.W., X.L., H.T., S.X.

  • Writing - original draft: J.W.

  • Writing - review & editing: Y.H., X.L.

References

1. Chen W, Zheng R, Zeng H, Zhang S, He J. Annual report on status of cancer in China, 2011. Chin J Cancer Res. 2015; 27:2–12.
2. Chen W, Zheng R, Baade PD, Zhang S, Zeng H, Bray F, et al. Cancer statistics in China, 2015. CA Cancer J Clin. 2016; 66:115–132.
crossref
3. Kitagawa R, Katsumata N, Shibata T, Kamura T, Kasamatsu T, Nakanishi T, et al. Paclitaxel plus carboplatin versus paclitaxel plus cisplatin in metastatic or recurrent cervical cancer: the open-label randomized phase III trial JCOG0505. J Clin Oncol. 2015; 33:2129–2135.
crossref
4. Wennerberg K, Rossman KL, Der CJ. The Ras superfamily at a glance. J Cell Sci. 2005; 118:843–846.
crossref
5. Adjei AA. Blocking oncogenic Ras signaling for cancer therapy. J Natl Cancer Inst. 2001; 93:1062–1074.
crossref
6. Pylayeva-Gupta Y, Grabocka E, Bar-Sagi D. RAS oncogenes: weaving a tumorigenic web. Nat Rev Cancer. 2011; 11:761–774.
crossref
7. Hutchins G, Southward K, Handley K, Magill L, Beaumont C, Stahlschmidt J, et al. Value of mismatch repair, KRAS, and BRAF mutations in predicting recurrence and benefits from chemotherapy in colorectal cancer. J Clin Oncol. 2011; 29:1261–1270.
8. Blons H, Emile JF, Le Malicot K, Julié C, Zaanan A, Tabernero J, et al. Prognostic value of KRAS mutations in stage III colon cancer: post hoc analysis of the PETACC8 phase III trial dataset. Ann Oncol. 2014; 25:2378–2385.
9. Kadota K, Sima CS, Arcila ME, Hedvat C, Kris MG, Jones DR, et al. KRAS mutation is a significant prognostic factor in early-stage lung adenocarcinoma. Am J Surg Pathol. 2016; 40:1579–1590.
10. Andreyev HJ, Norman AR, Cunningham D, Oates J, Dix BR, Iacopetta BJ, et al. Kirsten ras mutations in patients with colorectal cancer: the ‘RASCAL II’ study. Br J Cancer. 2001; 85:692–696.
11. Andreyev HJ, Norman AR, Cunningham D, Oates JR, Clarke PA. Kirsten ras mutations in patients with colorectal cancer: the multicenter “RASCAL” study. J Natl Cancer Inst. 1998; 90:675–684.
crossref
12. Imamura Y, Morikawa T, Liao X, Lochhead P, Kuchiba A, Yamauchi M, et al. Specific mutations in KRAS codons 12 and 13, and patient prognosis in 1075 BRAF wild-type colorectal cancers. Clin Cancer Res. 2012; 18:4753–4763.
13. Holderfield M, Deuker MM, McCormick F, McMahon M. Targeting RAF kinases for cancer therapy: BRAF-mutated melanoma and beyond. Nat Rev Cancer. 2014; 14:455–467.
14. Friday BB, Adjei AA. Advances in targeting the Ras/Raf/MEK/Erk mitogen-activated protein kinase cascade with MEK inhibitors for cancer therapy. Clin Cancer Res. 2008; 14:342–346.
crossref
15. Lito P, Saborowski A, Yue J, Solomon M, Joseph E, Gadal S, et al. Disruption of CRAF-mediated MEK activation is required for effective MEK inhibition in KRAS mutant tumors. Cancer Cell. 2014; 25:697–710.
16. Adelstein BA, Dobbins TA, Harris CA, Marschner IC, Ward RL. A systematic review and meta-analysis of KRAS status as the determinant of response to anti-EGFR antibodies and the impact of partner chemotherapy in metastatic colorectal cancer. Eur J Cancer. 2011; 47:1343–1354.
17. Manchado E, Weissmueller S, Morris JP 4th, Chen CC, Wullenkord R, Lujambio A, et al. A combinatorial strategy for treating KRAS-mutant lung cancer. Nature. 2016; 534:647–651.
18. Xiang L, Li J, Jiang W, Shen X, Yang W, Wu X, et al. Comprehensive analysis of targetable oncogenic mutations in chinese cervical cancers. Oncotarget. 2015; 6:4968–4975.
crossref
19. Schmitz M, Scheungraber C, Herrmann J, Teller K, Gajda M, Runnebaum IB, et al. Quantitative multiplex PCR assay for the detection of the seven clinically most relevant high-risk HPV types. J Clin Virol. 2009; 44:302–307.
crossref
20. Spaans VM, Trietsch MD, Peters AA, Osse M, Ter Haar N, Fleuren GJ, et al. Precise classification of cervical carcinomas combined with somatic mutation profiling contributes to predicting disease outcome. PLoS One. 2015; 10:e0133670.
crossref
21. Wright AA, Howitt BE, Myers AP, Dahlberg SE, Palescandolo E, Van Hummelen P, et al. Oncogenic mutations in cervical cancer: genomic differences between adenocarcinomas and squamous cell carcinomas of the cervix. Cancer. 2013; 119:3776–3783.
22. Ojesina AI, Lichtenstein L, Freeman SS, Pedamallu CS, Imaz-Rosshandler I, Pugh TJ, et al. Landscape of genomic alterations in cervical carcinomas. Nature. 2014; 506:371–375.
23. Frumovitz M, Burzawa JK, Byers LA, Lyons YA, Ramalingam P, Coleman RL, et al. Sequencing of mutational hotspots in cancer-related genes in small cell neuroendocrine cervical cancer. Gynecol Oncol. 2016; 141:588–591.
crossref
24. Wegman P, Ahlin C, Sorbe B. Genetic alterations in the K-Ras gene influence the prognosis in patients with cervical cancer treated by radiotherapy. Int J Gynecol Cancer. 2011; 21:86–91.
crossref
25. Ohnishi T, Tomita N, Monden T, Ohue M, Yana I, Takami K, et al. A detailed analysis of the role of K-ras gene mutation in the progression of colorectal adenoma. Br J Cancer. 1997; 75:341–347.
crossref
26. Alamo P, Gallardo A, Di Nicolantonio F, Pavón MA, Casanova I, Trias M, et al. Higher metastatic efficiency of KRas G12V than KRas G13D in a colorectal cancer model. FASEB J. 2015; 29:464–476.
crossref
27. Ihle NT, Byers LA, Kim ES, Saintigny P, Lee JJ, Blumenschein GR, et al. Effect of KRAS oncogene substitutions on protein behavior: implications for signaling and clinical outcome. J Natl Cancer Inst. 2012; 104:228–239.
28. Lito P, Saborowski A, Yue J, Solomon M, Joseph E, Gadal S, et al. Disruption of CRAF-mediated MEK activation is required for effective MEK inhibition in KRAS mutant tumors. Cancer Cell. 2014; 25:697–710.
29. Friday BB, Adjei AA. Advances in targeting the Ras/Raf/MEK/Erk mitogen-activated protein kinase cascade with MEK inhibitors for cancer therapy. Clin Cancer Res. 2008; 14:342–346.
crossref

Supplementary Materials

Supplementary Table 1

The association between KRAS mutation and disease recurrence

Supplementary Table 2

Detailed mutation and clinicopathological information

Supplementary Fig. 1

Kaplan-Meier curves of RFS for 601 patients with SCCs.

Supplementary Fig. 2

Kaplan-Meier curves of RFS for patients with KRAS G12 and G13 mutations.
TOOLS
ORCID iDs

Wei Jiang
https://orcid.org/0000-0001-7683-5811

Libing Xiang
https://orcid.org/0000-0001-8009-6521

Xuan Pei
https://orcid.org/0000-0002-4654-2222

Tiancong He
https://orcid.org/0000-0002-5736-3617

Xuxia Shen
https://orcid.org/0000-0003-2302-7188

Xiaohua Wu
https://orcid.org/0000-0002-6889-3541

Huijuan Yang
https://orcid.org/0000-0003-4569-6454

Similar articles