Overexpression of CDC7 in malignant salivary gland tumors correlates with tumor differentiation

Jaafari-Ashkavandi, Zohreh; Ashraf, Mohammad Javad; Abbaspoorfard, Ali Asghar

doi:10.1016/j.bjorl.2017.11.004

Abstract

Introduction:

Cell division cycle-7 protein is a serine/threonine kinase that has a basic role in cell cycle regulation and is a potential prognostic or therapeutic target in some human cancers.

Objectives:

This study investigated the expression of cell division cycle-7 protein in benign and malignant salivary gland tumors and also its correlation with clinicopathologic factors.

Methods:

Immunohistochemical expression of cell division cycle-7 was evaluated in 46 cases, including 15 adenoid cystic carcinoma, 12 mucoepidermoid carcinoma, 14 pleomorphic adenoma, and 5 normal salivary glands. Cell division cycle-7 expression rate and intensity were compared statistically.

Results:

The protein was expressed in almost all tumors. The intensity and mean of cell division cycle-7 expression were higher in malignant tumors in comparison with pleomorphic adenomas (p = 0.000). The protein expression was correlated with tumor grades (p = 0.000).

Conclusions:

The present study demonstrated cell division cycle-7 overexpression in malignant salivary gland tumors in comparison with pleomorphic adenomas, and also a correlation with tumor differentiation. Therefore, this protein might be a potential prognostic and therapeutic target for salivary gland tumors.

KEYWORDS
Salivary gland; CDC7; Adenoid cystic carcinoma; Mucoepidermoid carcinoma; Pleomorphic adenoma

Resumo

Introdução:

A cell division cycle-7 é uma serina/treonina quinase que tem um papel básico na regulação do ciclo celular e é um potencial marcador prognóstico ou terapêutico em alguns tipos de câncer humano.

Objetivos:

Este estudo investigou a expressão de cell division cycle-7 em tumores de glândulas salivares benignos e malignos e também sua correlação com fatores clínico-patológicos.

Método:

A expressão imuno-histoquímica de cell division cycle-7 foi avaliada em 46 casos, incluindo 15 carcinomas adenoide císticos, 12 carcinomas mucoepidermoides, 14 adenomas pleomórficos e 5 glândulas salivares normais. A taxa de expressão e a intensidade da proteína cell division cycle-7 foram comparadas estatisticamente.

Resultados:

A proteína foi expressa em quase todos os tumores. A intensidade e a média da expressão de cell division cycle-7 foram maiores em tumores malignos em comparação com adenoma pleomórfico (p = 0,000). A expressão da proteína foi correlacionada com os graus do tumor (p = 0,000).

Conclusões:

O presente estudo demonstrou a superexpressão de cell division cycle-7 em tumores malignos de glândulas salivares quando comparada com o adenoma pleomórfico, além de uma correlação com a diferenciação de tumores. Portanto, essa proteína pode ser um potencial marcador prognóstico e terapêutico para tumores de glândulas salivares.

PALAVRAS-CHAVE
Glândula salivar; CDC7; Carcinoma adenoide cístico; Carcinoma mucoepidermoide; Adenoma pleomórfico

Introduction

Salivary gland tumors (SGT) are relatively rare and diverse tumors which account for 3-6% of all head and neck neoplasms.¹1 Jaafari-Ashkavandi Z, Ashraf M, Afandak N. A clinico-pathologic study of 82 intraoral minor salivary gland tumors. I Red Crescent Med J. 2011;13:674-7. These tumors consist of different benign and malignant subtypes with a wide histopathologic spectrum which may overlap with each other; however, with a different clinical behavior and management, pleomorphic adenoma (PA), mucoepidermoid carcinoma (MEC) and adenoid cystic carcinoma (AdCC) are the most common benign and malignant SGTs. Surgery is the main treatment and in malignant tumors adjuvant chemo-radiotherapy may be required. Today, there is much promise in finding novel anti-cancer treatments to the basis of molecular target-therapy. The key molecules that participate in the cell growth and division are promising candidates for this goal. They may affect a broad range of various tumor types with a high proliferation rate.²2 Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25.

Cell division cycle-7 protein (CDC7) is a serine-threonine kinase, originally introduced in budding yeast, and plays a key role in DNA replication, principally by activating MCM complex, and regulation of S-phase check point in the cell cycle.³3 Dally RD, Woods TA. CDC7 Inhibitors. Google Patents; 2014.^,⁴4 Montagnoli A, Moll J, Colotta F. Targeting cell division cycle 7 kinase: a new approach for cancer therapy. Clin Cancer Res. 2010;16:4503-8. The regulator subunit of CDC7 is Dbf4/activator of S-phases.⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31. CDC7 overexpression was also correlated with P53 inactivation⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31. and has been found in many human tumor cell lines and tissues, including breast, colon and lung cancers, melanoma and oral squamous cell carcinoma (OSCC), but this protein has very low or undetectable expression in normal tissues.²2 Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25.^,⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31.

6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65.

7 Barkley LR, Santocanale C. MicroRNA-29a regulates the benzo[a]pyrene dihydrodiol epoxide-induced DNA damage response through Cdc7 kinase in lung cancer cells. Oncogenesis. 2013;2:e57.

8 Clarke LE, Fountaine TJ, Hennessy J, Bruggeman RD, Clarke JT, Mauger DT, et al. Cdc7 expression in melanomas, Spitz tumors and melanocytic nevi. J Cutan Pathol. 2009;36:433-8.

9 Cheng AN, Jiang SS, Fan CC, Lo YK, Kuo CY, Chen CH, et al. Increased Cdc7 expression is a marker of oral squamous cell carcinoma and overexpression of Cdc7 contributes to the resistance to DNA-damaging agents. Cancer Lett. 2013;337:218-25.^-¹⁰10 Chen H-J, Zhu Z, Wang X-L, Feng Q-L, Wu Q, Xu Z-P, et al. Expression of huCdc7 in colorectal cancer. World J Gastroenterol. 2013;19:3130-3.

It has been shown that CDC7 overexpression was correlated with poor prognosis in patients with B-cell lymphoma.¹¹11 Hou Y, Wang HQ, Ba Y. High expression of cell division cycle 7 protein correlates with poor prognosis in patients with diffuse large B-cell lymphoma. Med Oncol. 2012;29:3498-503. Also, it contributed to the resistance to DNA damaging agents and increasing survival in OSCC cancer cell line.⁹9 Cheng AN, Jiang SS, Fan CC, Lo YK, Kuo CY, Chen CH, et al. Increased Cdc7 expression is a marker of oral squamous cell carcinoma and overexpression of Cdc7 contributes to the resistance to DNA-damaging agents. Cancer Lett. 2013;337:218-25. CDC7 was a therapeutic target in ovarian carcinoma.¹²12 Kulkarni AA, Kingsbury SR, Tudzarova S, Hong H-K, Loddo M, Rashid M, et al. Cdc7 kinase is a predictor of survival and a novel therapeutic target in epithelial ovarian carcinoma. Clin Cancer Res. 2009;15:2417-25. Therefore, CDC7 is a promising and potent candidate target for cell-growth inhibition because it points DNA replication before it starts.⁴4 Montagnoli A, Moll J, Colotta F. Targeting cell division cycle 7 kinase: a new approach for cancer therapy. Clin Cancer Res. 2010;16:4503-8.^,⁶6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65.^,¹³13 Ito S, Taniyami C, Arai N, Masai H. Cdc7 as a potential new target for cancer therapy. Drug News Perspect. 2008;21:481-8. Therefore, evaluation of CDC7 function in any specific tumor is suggested. To the best of our knowledge, there is no research focused on CDC7 expression and its significance in SGTs. This study aimed to evaluate CDC7 expression rate and its correlation with clinicopathologic parameters of the most common benign and malignant SGTs.

Methods

Tissue samples

In this cross-sectional retrospective study, 46 cases consisting of 14 PA, 15 AdCC, 12 MEC and 5 normal salivary glands (NSG) were included. The cases obtained from archive of Pathology Department from 2009 to 2014. All cases had definitive diagnosis and adequate epithelial tissue. Severe inflamed cases were excluded. The baseline data including patient's age and gender, as well as tumor site, size, grade and stage were recorded, using the patient's medical files.

Immunohistochemistry

4 µm tissue sections were provided from formalin-fixed and paraffin-embedded blocks. After deparaffinization and rehydration, antigen retrieval was performed by Tris-buffer in PH = 8 at 121 °C for 20 min. Endogenous peroxidase activity was blocked using 3% hydrogen peroxide for 30 min. Then, the sections were incubated by primary antibody (anti-CDC7 polyclonal antibody, 1:50, Genetex Company, USA) for 60 min. Envision system was applied as secondary antibody and the section were washed in PBS. The chromogen solution was 3,3′-diaminobenzidine tetrahydrochloride (DAB). Finally, the slides were counterstained with Mayer's hematoxylin. A section of normal lymph node was used as positive control and the same section by omitting primary antibody as the negative control.

The stained tissues evaluated by light microscopy and the cells with brown nuclei were considered as positive. In each case, at least 1000 cells were counted in 3 microscopic fields and the percentage of positive cells was noted. The intensity of staining was assessed and scored as 1 - mild or 2 - moderate/severe, in comparison with the positive control. The mean of CDC7 expression was scored as: (1) positive cells < 5%, (2) 5-10% and (3) >10%. The final score was obtained by multiplying the intensity and percentage scores. Data were analyzed by Kruskal-Wallis, Tukey and Dunn tests and Spearman's correlation. p < 0.05 was considered as significant.

Results

The patients were 18 males and 28 females with a mean age of 49.4 ± 15. The baseline data related to all study groups are illustrates in Table 1.

Thumbnail

Table 1
Basic information of all study groups.

In NSGs, two specimens exhibited a limited nuclear staining in acinar and ductal cells, with weak to moderate intensity. Almost all tumors, except one MEC, showed positive nuclear CDC7 expression.

PAs showed CDC7 expression in the epithelial and ductal cells (Fig. 1A and B) with a mean of 2.3 ± 1.2. 71% of the cases revealed weak staining.

Figure 1
Nuclear, weak CDC7 expression in pleomorphic adenoma (A, ×200 and B, ×400).

The epidermoid cells of MEC showed CDC7 staining (Fig. 2A and B) and most of the cases (74%) had moderate/severe expression with a mean of 32.1 ± 14.3. Mucous and clear cells were not stained. All cases of AdCC exhibited moderate/severe CDC7 expression with a mean of 9.7 ± 3 (Fig. 3A and B).

Figure 2
Severe nuclear CDC7 expression in epidermoid cells of high-grade mucoepidermoid carcinoma (A, ×200; B, ×400).

Figure 3
Severe nuclear CDC7 expression in adenoid cystic carcinoma (A, ×200; B, ×400).

Details about mean expression of CDC7, intensity of staining and final scores are shown in Table 2. Kruskal-Wallis test showed a significant difference among groups in CDC7 expression (p = 0.000). Dunn test showed this difference between PA and MEC, as well as PA and AdCC (p = 0.000 and p = 0.004). However, there was not any significant difference between MEC and AdCC groups. Also, final scores of the groups were significantly different, according to Kruskal-Wallis test (p = 0.000).

Thumbnail

Table 2
Scores of intensity and CDC7 mean expression in all study groups.

PA showed significant lower scores of CDC7 mean, in comparison with MEC and also with AdCC groups, using Dunn test (p = 0.000 and p = 0.02, respectively). However, MEC and AdCC groups were statistically similar (Dunn test, p = 0.26).

Final scores were also different among the groups according to the results of Kruskal- Wallis test (p = 0.000) (Table 3). Dunn test showed that finals scores of the PA group was significantly lower than both malignant tumors (p = 0.000); however, MEC and AdCC were not different (p = 1).

Thumbnail

Table 3
Final scores of all study groups (Intensity × Mean scores).

High-grade tumors showed a significant increased CDC7 expression in comparison with low and intermediate grades. Spearman's correlation test showed that CDC7 expression was correlated with tumor grades (p = 0.000), but not with tumor stage or patient's age and gender (p > 0.05).

Discussion

In the present study, we described CDC7 expression in PA, MEC and AdCC, and also its overexpression in malignant SGTs in comparison with benign ones and normal glands. Various studies have previously revealed that CDC7 has a basic role in cell proliferation, tumorogenesis and malignant progression⁶6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65. by activating DNA replication.⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31.^,⁸8 Clarke LE, Fountaine TJ, Hennessy J, Bruggeman RD, Clarke JT, Mauger DT, et al. Cdc7 expression in melanomas, Spitz tumors and melanocytic nevi. J Cutan Pathol. 2009;36:433-8. Our findings support previous studies in various human cancer cell lines and tissues. Melling et al. demonstrated overexpression of CDC7 protein in colorectal cancer in association with P53 overexpression and as a favorable prognostic marker.²2 Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25. Bonte et al. also showed that CDC7 is very low or undetectable in normal tissue, but it was over-expressed in the human breast, colon and lung cancer cell lines.⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31. One study showed increased CDC7 mRNA level in malignant transformed breast cancer cell line and also in hyper-proliferating cells in a lesser degree in comparison with primary normal cells.⁶6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65. Increased CDC7 expression has been a marker of OSCC and has contributed to the resistance to DNA-damaging material.⁹9 Cheng AN, Jiang SS, Fan CC, Lo YK, Kuo CY, Chen CH, et al. Increased Cdc7 expression is a marker of oral squamous cell carcinoma and overexpression of Cdc7 contributes to the resistance to DNA-damaging agents. Cancer Lett. 2013;337:218-25. CDC7 and bf4 subunit form a complex that acts as an active protein kinase in all organisms.¹⁴14 Miller CT, Gabrielse C, Chen YC, Weinreich M. Cdc7p-Dbf4p regulates mitotic exit by inhibiting Polo kinase. PLoS Genet. 2009;5:e1000498. The main target of that complex activity is the MCM complex. The strong MCM positive cells indicate a high CDC7 activity.¹¹11 Hou Y, Wang HQ, Ba Y. High expression of cell division cycle 7 protein correlates with poor prognosis in patients with diffuse large B-cell lymphoma. Med Oncol. 2012;29:3498-503. MCM2-7 have considered as replication initiation factors and, as a novel diagnostic and prognostic biomarker for several human cancers. MCM expression has been reported in the tumors that showed CDC7 overexpression such as OSCC, breast cancer cell line and tissue and also SGTs.¹⁵15 Jurikova M, Danihel L, Polak S, Varga I. Ki67, PCNA, and MCM proteins: markers of proliferation in the diagnosis of breast cancer. Acta Histochem. 2016;118:544-52.

16 Razavi SM, Jafari M, Heidarpoor M, Khalesi S. Minichromosome maintenance-2 (MCM2) expression differentiates oral squamous cell carcinoma from pre-cancerous lesions. Malays J Pathol. 2015;37:253-8.

17 Vargas PA, Cheng Y, Barrett AW, Craig GT, Speight PM. Expression of Mcm-2, Ki-67 and geminin in benign and malignant salivary gland tumours. J Oral Pathol Med. 2008;37:309-18.^-¹⁸18 Jaafari-Ashkavandi Z, Najvani AD, Tadbir AA, Pardis S, Ranjbar MA, Ashraf MJ. MCM3 as a novel diagnostic marker in benign and malignant salivary gland tumors. Asian Pac J Cancer Prev. 2013;14:3479-82. MCM2 and MCM3 represented an overexpression in malignant SGTs in comparison with benign ones¹⁷17 Vargas PA, Cheng Y, Barrett AW, Craig GT, Speight PM. Expression of Mcm-2, Ki-67 and geminin in benign and malignant salivary gland tumours. J Oral Pathol Med. 2008;37:309-18.^,¹⁸18 Jaafari-Ashkavandi Z, Najvani AD, Tadbir AA, Pardis S, Ranjbar MA, Ashraf MJ. MCM3 as a novel diagnostic marker in benign and malignant salivary gland tumors. Asian Pac J Cancer Prev. 2013;14:3479-82. which indirectly support the overexpression of CDC7 in our samples.

It has also been demonstrated that CDC7 overexpression was correlated with TP53 gene mutation. CDC7 inhibition can induce cell death via a P53-dependent pathway.¹⁹19 Vanotti E, Amici R, Bargiotti A, Berthelsen J, Bosotti R, Ciavolella A, et al. Cdc7 kinase inhibitors: pyrrolopyridinones as potential antitumor agents. 1. Synthesis and structure-activity relationships. J Med Chem. 2008;51:487-501. Bonte et al. found a correlation between P53 loss, and CDC7 overexpression in some cancer cell line.⁵5 Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31. Also, in another study CDC7 expression was linked to P53 positivity in colorectal cancer.²2 Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25. CDC7 was a therapeutic target for P53 mutant breast cancer.⁶6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65. Previous studies on SGTs showed a higher expression of P53 in malignant SGTs in comparison with PA, which indirectly support our findings.²⁰20 Al-Rawi NH, Omer H, Al Kawas S. Immunohistochemical analysis of P(53) and bcl-2 in benign and malignant salivary glands tumors. J Oral Pathol Med. 2010;39:48-55.

The present study showed a positive correlation between CDC7 expression and tumor grades. However, our data did not show a significant difference between AdCC and MEC in CDC7 expression. Although AdCC is a high-grade tumor with more aggressive behavior in comparison with MEC, in our samples most of the MEC specimens were high-grade tumors. In agreement with our results, increased CDC7 expression was linked to loss of tumor differentiation, genomic instability and development of aggressive phenotype in breast cancer.⁶6 Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65. Also, high grade colorectal and ovarian cancers showed higher CDC7 expression.²2 Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25.^,¹²12 Kulkarni AA, Kingsbury SR, Tudzarova S, Hong H-K, Loddo M, Rashid M, et al. Cdc7 kinase is a predictor of survival and a novel therapeutic target in epithelial ovarian carcinoma. Clin Cancer Res. 2009;15:2417-25. This association of CDC7 expression with differentiation makes this protein a potential suitable target for therapeutic and prognostic approaches. However, in contrast to these researches, our limited cases with complete data about clinical stage did not show any significant correlation with protein expression.

The present study revealed nuclear staining of CDC7 in all positive specimens which reinforced CDC7 function in DNA replication. Previous studies have demonstrated protein accumulation in the cell nuclei during G1 phase.²¹21 Sato N, Sato M, Nakayama M, Saitoh R, Arai K, Masai H. Cell cycle regulation of chromatin binding and nuclear localization of human Cdc7-ASK kinase complex. Genes Cells. 2003;8:451-63.

Conclusion

The present findings showed CDC7 expression in the most common benign and malignant SGTs and its overexpression in malignant ones. Positive correlation of this protein with tumoral differentiation may represent it as a potential prognostic and therapeutic target.

Peer Review under the responsibility of Associação Brasileira de Otorrinolaringologia e Cirurgia Cérvico-Facial.
☆
Please cite this article as: Jaafari-Ashkavandi Z, Ashraf MJ, Abbaspoorfard AA. Overexpression of CDC7 in malignant salivary gland tumors correlates with tumor differentiation. Braz J Otorhinolaryngol. 2019;85:144-9.

Acknowledgment

The authors would like to thank the Vice-Chancellery of Shiraz University of Medical Science for supporting this research (Grant #10052), the Research Consultation Center (RCC) of Shiraz University of Medical Sciences for their invaluable assistant in editing this article. The authors also would like to thank Dr Salehi from the Dental Research Development Centre, for the statistical analysis. This manuscript is related to undergraduate thesis of Aliasghar Abbaspoorfard.

References

¹
Jaafari-Ashkavandi Z, Ashraf M, Afandak N. A clinico-pathologic study of 82 intraoral minor salivary gland tumors. I Red Crescent Med J. 2011;13:674-7.
²
Melling N, Muth J, Simon R, Bokemeyer C, Terracciano L, Sauter G, et al. Cdc7 overexpression is an independent prognostic marker and a potential therapeutic target in colorectal cancer. Diagn Pathol. 2015;10:25.
³
Dally RD, Woods TA. CDC7 Inhibitors. Google Patents; 2014.
⁴
Montagnoli A, Moll J, Colotta F. Targeting cell division cycle 7 kinase: a new approach for cancer therapy. Clin Cancer Res. 2010;16:4503-8.
⁵
Bonte D, Lindvall C, Liu H, Dykema K, Furge K, Weinreich M. Cdc7-Dbf4 kinase overexpression in multiple cancers and tumor cell lines is correlated with p53 inactivation. Neoplasia. 2008;10:920-31.
⁶
Choschzick M, Lebeau A, Marx AH, Tharun L, Terracciano L, Heilenkötter U, et al. Overexpression of cell division cycle 7 homolog is associated with gene amplification frequency in breast cancer. Hum Pathol. 2010;41:358-65.
⁷
Barkley LR, Santocanale C. MicroRNA-29a regulates the benzo[a]pyrene dihydrodiol epoxide-induced DNA damage response through Cdc7 kinase in lung cancer cells. Oncogenesis. 2013;2:e57.
⁸
Clarke LE, Fountaine TJ, Hennessy J, Bruggeman RD, Clarke JT, Mauger DT, et al. Cdc7 expression in melanomas, Spitz tumors and melanocytic nevi. J Cutan Pathol. 2009;36:433-8.
⁹
Cheng AN, Jiang SS, Fan CC, Lo YK, Kuo CY, Chen CH, et al. Increased Cdc7 expression is a marker of oral squamous cell carcinoma and overexpression of Cdc7 contributes to the resistance to DNA-damaging agents. Cancer Lett. 2013;337:218-25.
¹⁰
Chen H-J, Zhu Z, Wang X-L, Feng Q-L, Wu Q, Xu Z-P, et al. Expression of huCdc7 in colorectal cancer. World J Gastroenterol. 2013;19:3130-3.
¹¹
Hou Y, Wang HQ, Ba Y. High expression of cell division cycle 7 protein correlates with poor prognosis in patients with diffuse large B-cell lymphoma. Med Oncol. 2012;29:3498-503.
¹²
Kulkarni AA, Kingsbury SR, Tudzarova S, Hong H-K, Loddo M, Rashid M, et al. Cdc7 kinase is a predictor of survival and a novel therapeutic target in epithelial ovarian carcinoma. Clin Cancer Res. 2009;15:2417-25.
¹³
Ito S, Taniyami C, Arai N, Masai H. Cdc7 as a potential new target for cancer therapy. Drug News Perspect. 2008;21:481-8.
¹⁴
Miller CT, Gabrielse C, Chen YC, Weinreich M. Cdc7p-Dbf4p regulates mitotic exit by inhibiting Polo kinase. PLoS Genet. 2009;5:e1000498.
¹⁵
Jurikova M, Danihel L, Polak S, Varga I. Ki67, PCNA, and MCM proteins: markers of proliferation in the diagnosis of breast cancer. Acta Histochem. 2016;118:544-52.
¹⁶
Razavi SM, Jafari M, Heidarpoor M, Khalesi S. Minichromosome maintenance-2 (MCM2) expression differentiates oral squamous cell carcinoma from pre-cancerous lesions. Malays J Pathol. 2015;37:253-8.
¹⁷
Vargas PA, Cheng Y, Barrett AW, Craig GT, Speight PM. Expression of Mcm-2, Ki-67 and geminin in benign and malignant salivary gland tumours. J Oral Pathol Med. 2008;37:309-18.
¹⁸
Jaafari-Ashkavandi Z, Najvani AD, Tadbir AA, Pardis S, Ranjbar MA, Ashraf MJ. MCM3 as a novel diagnostic marker in benign and malignant salivary gland tumors. Asian Pac J Cancer Prev. 2013;14:3479-82.
¹⁹
Vanotti E, Amici R, Bargiotti A, Berthelsen J, Bosotti R, Ciavolella A, et al. Cdc7 kinase inhibitors: pyrrolopyridinones as potential antitumor agents. 1. Synthesis and structure-activity relationships. J Med Chem. 2008;51:487-501.
²⁰
Al-Rawi NH, Omer H, Al Kawas S. Immunohistochemical analysis of P(53) and bcl-2 in benign and malignant salivary glands tumors. J Oral Pathol Med. 2010;39:48-55.
²¹
Sato N, Sato M, Nakayama M, Saitoh R, Arai K, Masai H. Cell cycle regulation of chromatin binding and nuclear localization of human Cdc7-ASK kinase complex. Genes Cells. 2003;8:451-63.

Publication Dates

Publication in this collection
29 Apr 2019
Date of issue
Mar-Apr 2019

History

Received
5 Sept 2017
Accepted
8 Nov 2017
Published
26 Dec 2017

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] Peer Review under the responsibility of Associação Brasileira de Otorrinolaringologia e Cirurgia Cérvico-Facial.

[2] ☆
Please cite this article as: Jaafari-Ashkavandi Z, Ashraf MJ, Abbaspoorfard AA. Overexpression of CDC7 in malignant salivary gland tumors correlates with tumor differentiation. Braz J Otorhinolaryngol. 2019;85:144-9.

Group (n)	PA (14)	MEC (12)	AdCC (15)	NSG (5)	Total (46)
Age	39.4 ± 14	60.6 ± 12	49.7 ± 12	49 ± 14	49.4 ± 15.1
(M/F)	5/9	7/5	4/11	2/3	18/28
Site (Major/Minor)	11/2	10/2	6/8	1/4	28/16
Grade (1, 2, 3)	-	3, 0, 8	5, 10, 0	-	8, 10, 8
Stage (1, 2, 3, 4)	-	1, 3, 2, 5	1, 3, 4, 5	-	2, 6, 6, 10
Size (1, 2, 3, 4)	-	1, 5, 2, 3	1, 4, 3, 5	-	2, 9, 5, 8

	PA	MEC	AdCC	NSG
CDC7 mean score
1	5	0	0	2
2	9	1	7	0
3	0	10	7	0
Intensity score
1	10 (71.4)	2 (18.2)	0	0
2	4 (28.6)	9 (81.8)	15 (100)	2 (100)

Brasil

Brasil

Abstract

Introduction:

Objectives:

Methods:

Results:

Conclusions:

Resumo

Introdução:

Objetivos:

Método:

Resultados:

Conclusões:

Introduction

Methods

Tissue samples

Immunohistochemistry

Results

Discussion

Conclusion

Acknowledgment

References

Publication Dates

History