The promising role of Gelsolin expression to predict survival in patients with squamous cell carcinoma of the larynx

Şahin, Akın; Enver, Necati; Erçetin, Selim Yiǧit; Cinel, Zeliha Leyla; Batman, Abdullah Çaǧlar

doi:10.1016/j.bjorl.2021.05.009

Abstract

Introduction:

Gelsolin protein has important cellular functions, including cell motility and apoptosis. Altered gelsolin expression has been reported in several types of neoplasms, but clinicopathological features of gelsolin are currently unclear in patients with laryngeal squamous cell carcinoma.

Objectives:

Our aim is to investigate the clinicopathological significance of gelsolin as a prognostic biomarker for laryngeal squamous cell carcinoma.

Methods:

Tissue specimens from 168 patients with laryngeal squamous cell carcinoma were immunohistochemically assessed for the Gelsolin expression. Prognostic significance of Gelsolin and its interaction with clinical parameters was analysed.

Results:

Gelsolin expression was confirmed in 70.2% of cases. Gelsolin expression is significantly associated with tumor stage, tumor grade, and locoregional recurrence. Kaplan-Meier survival curves revealed that Gelsolin expression inversely correlated with both disease-specific and overall survival.

Conclusion:

This research is the first to demonstrate that Gelsolin expression is associated with a poor prognosis in laryngeal squamous cell carcinoma. Gelsolin is a novel promising biomarker and attractive target for the treatment of laryngeal squamous cell carcinoma.

Keywords
Gelsolin; Immunohistochemistry; Laryngeal squamous cell carcinoma; Biomarker; Prognosis

HIGHLIGHTS

Gelsolin overexpression significantly correlated with unfavorable survival.

Increased gelsolin expression was associated with lymphovascular invasion.

Gelsolin expression was higher in patients with advanced-stage laryngeal carcinoma.

Locoregional recurrence risk is higher in cases wıth gelsoline overexpression.

Gelsolin expression could be regarded as a novel independent prognostic biomarker.

Introduction

Cancer of the larynx is the second most common cancer among head and neck neoplasms, after oral cavity cancers. The incidence of laryngeal cancer is 2.7/100,000 and more than 200,000 new cases are seen worldwide annually.¹1 Nocini R, Molteni G, Mattiuzzi C, Lippi G. Updates on larynx cancer epidemiology. Chin J Cancer Res. 2020;32:18–25. Although various histological types of malignant cases can be seen in the larynx, squamous cell carcinomas (SCC) include about 95% of laryngeal cancer cases.²2 Armstrong WB, Vokes DE, Maisel RH. Malignant Tumors of the Larynx. In: Cummings Otolaryngology – Head and Neck Surgery. Elsevier; 2010. p. 1482–511. Over the past few decades, the incidence of laryngeal SCC, or LSCC, has increased in in South-East Asia and Western Pacific and gradually declined in Europe, presumably due to differences in alcohol and tobacco consumption.¹1 Nocini R, Molteni G, Mattiuzzi C, Lippi G. Updates on larynx cancer epidemiology. Chin J Cancer Res. 2020;32:18–25., ³3 Salvador-Coloma C, Cohen E. Multidisciplinary care of laryngeal cancer. J Oncol Pract. 2016;12:717–24.

Although several factors relate to LSCC prognosis, TNM stage, histopathological grade, and primary tumor site are the most important factors among them.⁴4 Brasilino de Carvalho M. Quantitative analysis of the extent of extracapsular invasion and its prognostic significance: a prospective study of 170 cases of carcinoma of the larynx and hypopharynx. Head Neck. 1998;20:16–21., ⁵5 Bradford CR, Ferlito A, Devaney KO, Mäkitie AA, Rinaldo A. Prognostic factors in laryngeal squamous cell carcinoma. Laryngoscope Investig Otolaryngol. 2020;5:74–81. Even so, these factors can provide useful information about prognosis and survival; however, they can sometimes be inadequate due to the fact that host- and tumor-related factors affect them. In order to have better tools for prognosis and survival, intracellular molecular pathways in larynx carcinogenesis must be revealed. Therefore, the discovery and validity of novel biomarkers that play a role in carcinogenesis of the larynx will enable the development of more effective laryngeal cancer treatment modalities.⁶6 Spector JG, Sessions DG, Haughey BH, Chao KS, Simpsons J, Mofty EL, et al. Delayed regional metastases, distant metastases, and second primary malignancies in squamous cell carcinomas of the larynx and hypopharynx. Laryngoscope. 2001;111:1079–87.

Gelsolin is a 82-kDa actin regulator protein that plays a key role in cytoskeleton organization, cell motility, cell growth, and apoptosis.⁷7 Baig RM, Mahjabeen I, Sabir M, Masood N, Ali K, Malik FA, et al. Mutational spectrum of Gelsolin and its down regulation is associated with breast cancer. Dis Markers. 2013;34:71–80. Gelsolin has the capability of capping and severing actin molecules, thus modulating polymerization and length of filaments. Free Ca²⁺ ions, temperature, Ph, and phosphatidylinositol 4.5 bisphosphate (PIP2) are the main regulatory factors for G-protein. Intracellular interaction of gelsolin and caspase-3 has been shown to accelerate apoptosis-related morphological changes, thus promoting apoptosis. On the other hand, full-length gelsolin induced by agents such as ceramide, dexamethasone, and anti-Fas antibody inhibit apoptosis.⁸8 Koya RC, Fujita H, Shimizu S, Ohtsu M, Takimoto M, Tsujimoto Y, et al. Gelsolin inhibits apoptosis by blocking mitochondrial membrane potential loss and cytochrome c release. J Biol Chem. 2000;275:15343–9. The inhibiting or promoting effect of gelsolin may vary depends upon the type of tissues and cells. Gelsolin upregulation and an adverse effect on prognosis have been reported in lung, prostate, and oral cavity cancers;⁹9 Zhu WY, Hunag YY, Liu XG, He JY, Chen DD, Zeng F, et al. Prognostic evaluation of CapG, Gelsolin, P-gp, GSTP1, and Topo-II Proteins in non-small cell lung cancer. Anat Rec. 2012;295:208–14., ¹⁰10 Chen C-C, Chiou S-H, Yang C-L, Chow K-C, Lin T-Y, Chang H-W, et al. Secreted gelsolin desensitizes and induces apoptosis of infiltrated lymphocytes in prostate cancer. Oncotarget. 2017;8:77152–67., ¹¹11 Bin Shieh D, Chen IW, Wei TY, Shao CY, Chang HJ, Chung CH, et al. Tissue expression of gelsolin in oral carcinogenesis progression and its clinicopathological implications. Oral Oncol. 2006;42:599–606. however, decreased expression of gelsolin suggests a tumor-suppressing role in breast and colon malignancies.¹²12 Liu J, Liu YG, Huang R, Yao C, Li S, Yang W, et al. Concurrent down-regulation of Egr-1 and gelsolin in the majority of human breast cancer cells. Cancer Genomics Proteomics. 2007;4:377–86., ¹³13 Gay F, Estornes Y, Saurin JC, Joly- Pharaboz MO, Friederich E, Scoazec JY, et al. In colon carcinogenesis, the cytoskeletal protein gelsolin is down-regulated during the transition from adenoma to carcinoma. Hum Pathol. 2008;39:1420–30. Regarding the effects of gelsolin on carcinogenesis, currently no studies exists on the expression of gelsolin in LSCC tissues and its impact on prognosis.

In this study, we investigated the expression level of gelsolin using immunohistochemistry (IHC) and evaluated its correlation with clinicopathological and prognostic parameters in LSCC patients. Our aim in this research was to clarify the relationship between gelsolin and laryngeal cancer and to investigate the usability of gelsolin as a novel biomarker to predict prognosis in LSCC.

Methods

Patient population and tissue samples

We analyzed 168 patients with pathologically confirmed LSCC who underwent primary open partial or total laryngectomy between January 2010 and December 2019. None of the patients had received either chemotherapy or radiotherapy previously. Before surgery, all patients were investigated by laryngoscopy with laryngeal biopsies, head, and neck contrast-enhanced computed tomography (CT), and/or magnetic resonance imaging (MRI), neck ultrasonography, and chest radiography. Informed consent was obtained from all patients who were living during this study. This research study was approved by the Institutional Review Board (Approval ID: 09.2018.436) and was conducted in accordance with the principles of the Helsinki Declaration.

Immunohistochemistry and evaluation of staining

Immunohistochemical procedures were conducted in compliance with the manufacturer’s instructions using an automated immunohistochemical stainer (Ventana BenchMark ULTRA, Ventana Medical Systems, Inc., Tucson, AZ, USA). Surgical specimens were fixed in neutral buffered formalin and embedded in paraffin wax. The 4-μm-tissue sections were deparaffinized using the EZ Prep solution (Ventana Medical Systems, Inc., Tucson, AZ, USA). A Cell Conditioning-1 solution (Ventana Medical Systems, Inc.) was used for heat-induced antigen retrieval at 70°C for 60min. Endogenous peroxidase activity was blocked using hydrogen peroxide and 3.3'-Diaminobenzidine tetrahydrochloride (UltraView™ Universal DAB Detection Kit, Ventana Medical Systems). Tissue sections were then incubated with the monoclonal anti- gelsolin antibody (clone 2C4, Sigma-Aldrich, St. Louis, MO, USA) at a specified dilution. Afterwards, sections were counterstained with hematoxylin and bluing reagent, cleared, and coverslipped with the mounting media.

All stained sections were selected in blind fashion and examined by two pathologists independently who had no prior knowledge of patients’ clinicopathological outcomes. Cells were evaluated according to their cytoplasmic staining levels. A four-scale scoring scheme was used as follows: tumors absent of gelsolin expression were scored 0, weak expressions were scored 1, moderate expressions were scored 2, and strong expressions were scored 3 (Fig. 1). We used the Gelsolin Expression Index achieved by multiplying the percentage of staining tumor cells for each of the three positive scores (1+, 2+, or 3+), as described previously in the literature.¹⁴14 Shieh D-B, Godleski J, Herndon JE, Azuma T, Mercer H, Sugar-baker DJ, et al. Cell motility as a prognostic factor in Stage I nonsmall cell lung carcinoma. Cancer. 1999;85:47–57., ¹⁵15 Yang J, Ramnath N, Moysich KB, Asch HL, Swede H, Alrawi SJ, etal. Prognostic significance of MCM2, Ki-67 and gelsolin in non-small cell lung cancer. BMC Cancer. 2006;6:1–10. The median value was used as the cut-point for the dichotomization of the gelsolin expression due to the skewed index distribution (weak or negative if index ≤30, and strong or positive if index >30).

Figure 1
Gelsolin immunohistochemical expression in human laryngeal carcinoma. (a) Negative gelsolin expression in the neoplastic epithelium of laryngeal carcinoma (×200). (b) A case of laryngeal carcinoma with low gelsolin expression (×200). (c) High gelsolin expression in human laryngeal carcinoma (×200).

Statistical analysis

A p-value of < 0.05 was determined as a statistically significant level. Associations between clinicopathological parameters of LSCC patients and IHC score of gelsolin protein were analyzed using the Chi-Square (χ2) test or Fisher’s exact test. The Kaplan–Meier method was used to estimate Disease-Free Survival (DFS) and Overall Survival (OS) analysis, and survival differences were analyzed by a log-rank test. Multivariate analysis was determined by the Cox proportional hazards model to identify independent prognostic factors. Statistical analyses were performed using SPSS 20.0 statistical software for Windows (IBM, Chicago, Illinois, USA).

Results

Clinicopathologic parameters

This study included 168 patients who were diagnosed with LSCC. Overall average age of patients was 62.23 ± 10.36 with a range of 41–88 years. Patients were predominantly male (158 men, 10 women). More than 90% of the patients were either former smokers (63%) or current smokers (28%), and around 9% of the patients were non- smokers. LSCC was located in the glottis area of 108 (64.2%) patients, compared to 55 (32.9%) patients in the supraglottic region. Tumors were staged based on the eighth edition of the American Joint Committee on Cancer. Forty-one percent of patients were in T1 to T2 stage, 30.0% in T3, and 29% in T4. Fifty-five patients out of 168 (32.7%) with LSCC had positive lymph nodes. Sixty-four patients (38%) were classified with early-stage laryngeal cancer, while 104 patients (62%) were classified with advanced-stage laryngeal cancer. Median duration of followup was 49.2 months (3-120 months). Recurrences were observed in 60 of 168 (35.7%) cases.

Gelsolin expression in LSCC and its clinicopathological features

Analysis of protein expression using IHC was carried out for gelsolin in all samples. Immunostaining showed that gelsolin had positive expression in 118 (70.2%) of 168 human LSCC samples. There was a strong association between expression of gelsolin and tumor stage, tumor differentiation, tumor recurrence, and Lymphovascular Invasion (LVI), with p-values of 0.001, 0.031, 0.018 and 0.016 respectively (Fig. 2). Conversely, no significant correlation was identified between gelsolin protein expression and age, sex, lymph node status, perineural invasion (PNI), and primary location of laryngeal carcinoma, with p-values of 0.794, 0.937, 0.326 and 0.872 respectively (Table 1).

Figure 2
Relationship of gelsolin expression and clinicopatological features. gelsolin expression correlated with tumor stage (A), tumor grade (B), lymphovascular invasion (C), loco-regional recurrence (D).

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Table 1
Correlation between gelsolin expression and clinicopathological parameters of laryngeal squamous cell carcinoma.

The rate of immunohistochemical staining with gelsolin was found to be significantly higher in tumor tissues of patients with an advanced clinical stage than in patients with an early clinical stage (positive gelsolin expression was 79.8% for advanced-stage LSCC and 54.6% for early-stage LSCC, p<0.05).

Survival analysis

Recurrence was reported for 60 (35.7%) of 168 patients with LSCC during the follow-up period. The mean recurrence period was 28 ± 5.8 months, with a range of 3-43 months. A Kaplan–Meier analysis of survival showed that the mean period of recurrence was 30.4 months in patients with low gelsoline levels versus 17.9 months in patients with gelsoline overexpression, respectively (p = 0.002).

The median OS was 78.0 months, ranging from 1 to 120 months. The TNM stage (p = 0.031), lymph node status (p = 0.001), PNI (p = 0.041), and LVI (p = 0.002) were identified as factors associated with a significantly worse prognosis by univariate analysis. Multivariate analysis confirmed TNM stage, LVI, and positive gelsolin expression as independent prognostic factors indicating poorer outcomes, with p-values of 0.01, 0.021, 0.025 respectively.

Regarding gelsolin, Kaplan–Meier survival curves revealed that LSCC patients with gelsolin-positive tumors had lower OS rates relative to patients with gelsolin-negative tumors (p = 0.004) (Fig. 3A). On the other hand, univariate Cox regression analysis for OS demonstrated that gelsolin immunopositivity predicted an increased risk of patient death (HR=3.28, 95% CI 1.67–7.47, p = 0.004). The prognostic significance of gelsolin was shown to be independent of clinicopathological parameters (age, sex, tumor location, histological location, TNM stage, lymph node status, PNI, and LVI) of the patient (HR = 2.63, 95% CI 1.27-6.67, p = 0.025) (Table 2).

Figure 3
Kaplan–Meier survival curves showed that gelsolin expression was inversely correlated with both overall and disease-specific survival. (A) The overall survival curves of negative and positive gelsolin expression in LSCC patients (p<0.05). (B) The disease-free survival curves of negative and positive gelsolin expression in LSCC patients (p< 0.05).

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Table 2
Univariate and multivariate analysis for overall survival in patients with laryngeal squamous cell carcinoma.

The median DFS was 68.0 months, ranging from 1 to 120 months (95% Confidence Interval, 95% CI 58.7-133.8) (Fig. 3B). Univariate analysis on DFS indicated that TNM stage, lymph node status, LVI, and gelsolin expression were significantly associated with poorer outcomes (p = 0.014, 0.001, 0.002, and 0.030 respectively), all factors were confirmed as independent prognostic factors for predicting poorer outcomes (p<0.05) by multivariate analysis (Table 3).

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Table 3
Univariate and multivariate analysis for disease-free survival in patients with laryngeal squamous cell carcinoma.

Discussion

Currently, proven clinical parameters, such as TNM classification and histopathological grading, are insufficient to accurately predict the exact prognosis of LSCC patients.¹⁶16 Gioacchini FM, Alicandri-Ciufelli M, Magliulo G, Rubini C, Presutti L, Re M. The clinical relevance of Ki-67 expression in laryngeal squamous cell carcinoma. Eur Arch Otorhinolaryngol. 2015;272:1569–76. Biological markers are widely used in head and neck cancer to enhance the prediction of tumor aggression. Her-2 and p53 proteins are well-established molecules presently used to assess the prognosis of patients with LSCC.¹⁷17 Awada A, Lalami Y. Molecular markers, molecular-targeted therapies and taxanes: how to integrate the progress into clinical research and practice for the management of head and neck cancers. Curr Opin Oncol. 2005;17:209–11., ¹⁸18 Krecicki T, Smigiel R, Fraczek M, Kowalczyk M, Sasiadek MM. Studies of the cell cycle regulatory proteins P16, cyclin D1 and retinoblastoma protein in laryngeal carcinoma tissue. J Laryngol Otol. 2004;118:676–80. While these biomarkers can identify poor prognosis, additional cellular research is still required to establish new innovative treatment options. With the discovery of novel biomarkers, more accurate treatment modalities can be offered for LSCC patients and may lead to longer survival rates.¹⁹19 Kontos C, ChristodoulouM-I, Scorilas A. Apoptosis-related BCL2-family members: key players in chemotherapy. Anticancer Agents Med Chem. 2014;14:353–74. In this research, we studied whether the expression level of gelsolin could serve as a potential biological marker for prognosis and survival of LSCC.

Gelsolin participates in the reorganization of actin cytoskeleton that lead to regulation of apoptosis and cell motility.⁸8 Koya RC, Fujita H, Shimizu S, Ohtsu M, Takimoto M, Tsujimoto Y, et al. Gelsolin inhibits apoptosis by blocking mitochondrial membrane potential loss and cytochrome c release. J Biol Chem. 2000;275:15343–9. Mitochondria-mediated apoptosis is well known as being stimulated by the loss of membrane potential and the release of proapoptotic cytochrome c, which activates caspase and induces nuclear fragmentation. Gelsolin over-expression prevents mitochondrial membrane potential loss and inhibits apoptosis.²⁰20 Landes T, Martinou J-C. Mitochondrial outer membrane permeabilization during apoptosis: the role of mitochondrial fission. Biochim Biophys Acta - Mol Cell Res. 2011;1813:540–5. Kusana et al. (2016) reported that gelsolin overexpression counteracts mitochondrial membrane potential loss and cytochrome c release, by blocking caspase-3, -8 and -9 activation in cancer cells, thus inhibiting apoptosis.²¹21 Kusano H, Shimizu S, Koya RC, Fujita H, Kamada S, Kuzumaki N, et al. Human gelsolin prevents apoptosis by inhibiting apoptotic mitochondrial changes via closing VDAC. Oncogene. 2000;19:4807–14.

To date, gelsolin expression in LSCC has not been studied; therefore, in this research, the potential impact of gelsolin expression on LSCC was studied and analyzed. Gelsolin expression status was found to have a statistically significant relationship in the prognosis of laryngeal cancer. However, results of this research cannot be directly compared with current literature, due to lack of similar investigations into LSCC.

Gelsolin protein might be considered as a promising molecular marker for prognostic evaluation in human cancer. It remains unclear whether the increased or decreased expression of gelsolin is associated with adverse prognosis in human neoplasms, which is possibly due to the nuanced and multifactorial nature of tumorigenesis.

Gelsolin protein has been observed to be elevated in a considerable number of solid tumors. Several studies have demonstrated that increased expression of gelsolin is related to lower survival rates among patients with human prostate cancer, lung cancer, and oral cavity cancer.⁹9 Zhu WY, Hunag YY, Liu XG, He JY, Chen DD, Zeng F, et al. Prognostic evaluation of CapG, Gelsolin, P-gp, GSTP1, and Topo-II Proteins in non-small cell lung cancer. Anat Rec. 2012;295:208–14., ¹⁰10 Chen C-C, Chiou S-H, Yang C-L, Chow K-C, Lin T-Y, Chang H-W, et al. Secreted gelsolin desensitizes and induces apoptosis of infiltrated lymphocytes in prostate cancer. Oncotarget. 2017;8:77152–67., ¹¹11 Bin Shieh D, Chen IW, Wei TY, Shao CY, Chang HJ, Chung CH, et al. Tissue expression of gelsolin in oral carcinogenesis progression and its clinicopathological implications. Oral Oncol. 2006;42:599–606., ¹⁵15 Yang J, Ramnath N, Moysich KB, Asch HL, Swede H, Alrawi SJ, etal. Prognostic significance of MCM2, Ki-67 and gelsolin in non-small cell lung cancer. BMC Cancer. 2006;6:1–10., ²²22 Wang PW, Abedini MR, Yang LX, Ding AA, Figeys D, Chang JY, et al. Gelsolin regulates cisplatin sensitivity in human head-and-neck cancer. Int J Cancer. 2014;135:2760–9.

Moreover, a negative expression of gelsolin in patients with colon carcinoma closely associated with longer survival rates.¹³13 Gay F, Estornes Y, Saurin JC, Joly- Pharaboz MO, Friederich E, Scoazec JY, et al. In colon carcinogenesis, the cytoskeletal protein gelsolin is down-regulated during the transition from adenoma to carcinoma. Hum Pathol. 2008;39:1420–30. However, the downregulation of gelsolin in renal clear cell carcinoma has been reported to be indicative of worse prognosis.²³23 Visapää H, Bui M, Huang Y, Seligson D, Tsai H, Pantuck A, et al. Correlation of Ki-67 and gelsolin expression to clinical outcome in renal clear cell carcinoma. Urology. 2003;61:845–50. Although gelsolin can apparently have opposite actions depending on tumor type, detailed analysis of its expression status in different tumor sites are crucial for understanding its impact on carcinogenesis.

Our data revealed that overexpression of the gelsolin protein appears significantly correlated with unfavorable OS and DFS in patients with LSCC. Zhu et al. (2012) noticed that longer OS and DFS was significantly associated with the downregulation of gelsolin protein for squamous cell lung cancer, which correlates with our findings and results reported by Yang et al. (2004).⁹9 Zhu WY, Hunag YY, Liu XG, He JY, Chen DD, Zeng F, et al. Prognostic evaluation of CapG, Gelsolin, P-gp, GSTP1, and Topo-II Proteins in non-small cell lung cancer. Anat Rec. 2012;295:208–14., ²⁴24 Yang J, Tan D, Asch HL, Swede H, Bepler G, Geradts J, et al. Prognostic significance of gelsolin expression level and variability in non-small cell lung cancer. Lung Cancer. 2004;46:29–42. It is possible to infer that gelsolin immunopositivity could be a guide to identify LSCC patients with shorter OS and DFS. It is also possible to expect similar effects of gelsolin overexpression in other types of head and neck squamous cell cancers.

In the literature, only two articles have reported the effect of gelsolin on head and neck cancers. Shieh et al. (2006) studied the effects of gelsolin expression on oral carcinogenesis and found a significant relationship between gelsolin overexpression and shorter DFS. Additionally, increased gelsolin expression, from precancerous lesions to cancer cells, has been reported.¹¹11 Bin Shieh D, Chen IW, Wei TY, Shao CY, Chang HJ, Chung CH, et al. Tissue expression of gelsolin in oral carcinogenesis progression and its clinicopathological implications. Oral Oncol. 2006;42:599–606. According to Wang (2014), head and neck cancer cell lines with higher endogenous gelsolin expression were more cisplatin resistant than those with lower gelsolin expression.²²22 Wang PW, Abedini MR, Yang LX, Ding AA, Figeys D, Chang JY, et al. Gelsolin regulates cisplatin sensitivity in human head-and-neck cancer. Int J Cancer. 2014;135:2760–9. Our study supports these articles, revealing a relationship between poor prognosis and gelsolin overexpression, but gelsolin effect in the process of cancer transformation from precancerous lesions in LSCC has still not been studied.

Our analysis showed a strong association between histopathological tumor grade and expression of gelsolin. In patients with poorly differentiated LSCC, gelsolin immunopositivity was higher than in patients who had moderate or well differentiated tumors. A similar result has been reported in non-small cell lung carcinoma, where a high gelsolin expression was associated with increased tumor grade.⁹9 Zhu WY, Hunag YY, Liu XG, He JY, Chen DD, Zeng F, et al. Prognostic evaluation of CapG, Gelsolin, P-gp, GSTP1, and Topo-II Proteins in non-small cell lung cancer. Anat Rec. 2012;295:208–14. We also observed in this study that increased expression of gelsoline was correlated with higher LVI rates. Although the mechanism behind the LVI has not been clearly proven, it may represent a tumor microenvironment that predicts aggressive tumor behavior. In particular, survival rates of LSCC patients were significantly lower if LVI was observed in pathological specimens.

In addition, we have found a correlation between expression of gelsolin and tumor stage in LSCC. Expression of gelsolin was higher in patients with advanced-stage LSCC relative to those with early-stage LSCC. This may suggest that in the early stages of laryngeal carcinogenesis the pattern of gelsoline expression is of little relevance. However, some authors found no relationship between tumor stage and gelsolin expression.¹³13 Gay F, Estornes Y, Saurin JC, Joly- Pharaboz MO, Friederich E, Scoazec JY, et al. In colon carcinogenesis, the cytoskeletal protein gelsolin is down-regulated during the transition from adenoma to carcinoma. Hum Pathol. 2008;39:1420–30.

Increased motility ability is crucial for tumor cells to invade and metastasize.²⁵25 Yamazaki D, Kurisu S, Takenawa T. Regulation of cancer cell motility through actin reorganization. Cancer Sci. 2005;96:379–86. Various studies reported that increased motility functions of cells are related to higher rates of tumor invasion and reduced survival time.²⁶26 Dobashi Y, Watanabe H, Matsubara M, Yanagawa T, Raz A, Shimamiya T, et al. Autocrine motility factor/glucose-6-phosphate isomerase is a possible predictor of metastasis in bone and soft tissue tumours. J Pathol. 2006;208:44-53., ²⁷27 Kato H, Semba S, Miskad UA, Seo Y, Kasuga M, Yokozaki H. High expression of PRL-3 promotes cancer cell motility and liver metastasis in human colorectal cancer: a predictive molecular marker of metachronous liver and lung metastases. Clin Cancer Res. 2004;10:7318–28. In some animal models, the motility regulating role of gelsolin has been observed.²⁸28 Azuma T, Witke W, Stossel TP, Hartwig JH, Kwiatkowski DJ. Gelsolin is a downstream effector of rac for fibroblast motility. EMBO J. 1998;17:1362–70., ²⁹29 Crowley MR, Head KL, Kwiatkowski DJ, Asch HL, Asch BB. The mouse mammary gland requires the actin-binding protein gelsolin for proper ductal morphogenesis. Dev Biol. 2000;225:407–23. In 229 patients with lung carcinoma, Shieh et al. (1999) found a strong inverse relationship between the level of gelsolin expression and survival. So that he hypothesized that the impact of gelsolin on cell motility may be the explanation for the poor prognostic role of high gelsolin expression.¹⁴14 Shieh D-B, Godleski J, Herndon JE, Azuma T, Mercer H, Sugar-baker DJ, et al. Cell motility as a prognostic factor in Stage I nonsmall cell lung carcinoma. Cancer. 1999;85:47–57. Consequently, tumor cells might upregulate gelsolin to increase movement capability, as achieving highly mobile behavior is considered a prerequisite for the spread of a tumor cell to adjacent tissues and distant metastasis. In our study, a significant relationship was found between gelsolin overexpression and locoregional recurrence: one of the most important reasons for this phenomenon may be the enhancing effect of gelsolin on motility.

Although a relationship between gelsolin and LSCC was clearly revealed in our study, several limitations were associated with this article. Because of IHC evaluation was based on a subjective scoring method, results depend on the experience of the person making the assessment. In addition, it remains unclear why the increased expression of gelsolin was closely associated with adverse prognosis in patients with LSCC. Further cellular studies are required to validate prognostic value of gelsolin against other parameters in a large group of patients.

In conclusion, gelsolin immunopositivity was significantly associated with poorer prognosis in patients with LSCC. Moreover, we conclude that gelsolin expression could be regarded as a novel independent prognostic biomarker for OS and DFS in patients with LSCC. Therefore, our results may provide evidence that gelsolin may contribute to the development, progression, and prognosis of LSCC. This study also reveals that new therapeutic agents targeting gelsolin protein may be useful to treat laryngeal cancer more effectively. Further evaluation of gelsolin effects on LSCC is required to validate our results.

All authors declare no conflict of interest, and no external funding was obtained for this study.

References

¹
Nocini R, Molteni G, Mattiuzzi C, Lippi G. Updates on larynx cancer epidemiology. Chin J Cancer Res. 2020;32:18–25.
²
Armstrong WB, Vokes DE, Maisel RH. Malignant Tumors of the Larynx. In: Cummings Otolaryngology – Head and Neck Surgery. Elsevier; 2010. p. 1482–511.
³
Salvador-Coloma C, Cohen E. Multidisciplinary care of laryngeal cancer. J Oncol Pract. 2016;12:717–24.
⁴
Brasilino de Carvalho M. Quantitative analysis of the extent of extracapsular invasion and its prognostic significance: a prospective study of 170 cases of carcinoma of the larynx and hypopharynx. Head Neck. 1998;20:16–21.
⁵
Bradford CR, Ferlito A, Devaney KO, Mäkitie AA, Rinaldo A. Prognostic factors in laryngeal squamous cell carcinoma. Laryngoscope Investig Otolaryngol. 2020;5:74–81.
⁶
Spector JG, Sessions DG, Haughey BH, Chao KS, Simpsons J, Mofty EL, et al. Delayed regional metastases, distant metastases, and second primary malignancies in squamous cell carcinomas of the larynx and hypopharynx. Laryngoscope. 2001;111:1079–87.
⁷
Baig RM, Mahjabeen I, Sabir M, Masood N, Ali K, Malik FA, et al. Mutational spectrum of Gelsolin and its down regulation is associated with breast cancer. Dis Markers. 2013;34:71–80.
⁸
Koya RC, Fujita H, Shimizu S, Ohtsu M, Takimoto M, Tsujimoto Y, et al. Gelsolin inhibits apoptosis by blocking mitochondrial membrane potential loss and cytochrome c release. J Biol Chem. 2000;275:15343–9.
⁹
Zhu WY, Hunag YY, Liu XG, He JY, Chen DD, Zeng F, et al. Prognostic evaluation of CapG, Gelsolin, P-gp, GSTP1, and Topo-II Proteins in non-small cell lung cancer. Anat Rec. 2012;295:208–14.
¹⁰
Chen C-C, Chiou S-H, Yang C-L, Chow K-C, Lin T-Y, Chang H-W, et al. Secreted gelsolin desensitizes and induces apoptosis of infiltrated lymphocytes in prostate cancer. Oncotarget. 2017;8:77152–67.
¹¹
Bin Shieh D, Chen IW, Wei TY, Shao CY, Chang HJ, Chung CH, et al. Tissue expression of gelsolin in oral carcinogenesis progression and its clinicopathological implications. Oral Oncol. 2006;42:599–606.
¹²
Liu J, Liu YG, Huang R, Yao C, Li S, Yang W, et al. Concurrent down-regulation of Egr-1 and gelsolin in the majority of human breast cancer cells. Cancer Genomics Proteomics. 2007;4:377–86.
¹³
Gay F, Estornes Y, Saurin JC, Joly- Pharaboz MO, Friederich E, Scoazec JY, et al. In colon carcinogenesis, the cytoskeletal protein gelsolin is down-regulated during the transition from adenoma to carcinoma. Hum Pathol. 2008;39:1420–30.
¹⁴
Shieh D-B, Godleski J, Herndon JE, Azuma T, Mercer H, Sugar-baker DJ, et al. Cell motility as a prognostic factor in Stage I nonsmall cell lung carcinoma. Cancer. 1999;85:47–57.
¹⁵
Yang J, Ramnath N, Moysich KB, Asch HL, Swede H, Alrawi SJ, etal. Prognostic significance of MCM2, Ki-67 and gelsolin in non-small cell lung cancer. BMC Cancer. 2006;6:1–10.
¹⁶
Gioacchini FM, Alicandri-Ciufelli M, Magliulo G, Rubini C, Presutti L, Re M. The clinical relevance of Ki-67 expression in laryngeal squamous cell carcinoma. Eur Arch Otorhinolaryngol. 2015;272:1569–76.
¹⁷
Awada A, Lalami Y. Molecular markers, molecular-targeted therapies and taxanes: how to integrate the progress into clinical research and practice for the management of head and neck cancers. Curr Opin Oncol. 2005;17:209–11.
¹⁸
Krecicki T, Smigiel R, Fraczek M, Kowalczyk M, Sasiadek MM. Studies of the cell cycle regulatory proteins P16, cyclin D1 and retinoblastoma protein in laryngeal carcinoma tissue. J Laryngol Otol. 2004;118:676–80.
¹⁹
Kontos C, ChristodoulouM-I, Scorilas A. Apoptosis-related BCL2-family members: key players in chemotherapy. Anticancer Agents Med Chem. 2014;14:353–74.
²⁰
Landes T, Martinou J-C. Mitochondrial outer membrane permeabilization during apoptosis: the role of mitochondrial fission. Biochim Biophys Acta - Mol Cell Res. 2011;1813:540–5.
²¹
Kusano H, Shimizu S, Koya RC, Fujita H, Kamada S, Kuzumaki N, et al. Human gelsolin prevents apoptosis by inhibiting apoptotic mitochondrial changes via closing VDAC. Oncogene. 2000;19:4807–14.
²²
Wang PW, Abedini MR, Yang LX, Ding AA, Figeys D, Chang JY, et al. Gelsolin regulates cisplatin sensitivity in human head-and-neck cancer. Int J Cancer. 2014;135:2760–9.
²³
Visapää H, Bui M, Huang Y, Seligson D, Tsai H, Pantuck A, et al. Correlation of Ki-67 and gelsolin expression to clinical outcome in renal clear cell carcinoma. Urology. 2003;61:845–50.
²⁴
Yang J, Tan D, Asch HL, Swede H, Bepler G, Geradts J, et al. Prognostic significance of gelsolin expression level and variability in non-small cell lung cancer. Lung Cancer. 2004;46:29–42.
²⁵
Yamazaki D, Kurisu S, Takenawa T. Regulation of cancer cell motility through actin reorganization. Cancer Sci. 2005;96:379–86.
²⁶
Dobashi Y, Watanabe H, Matsubara M, Yanagawa T, Raz A, Shimamiya T, et al. Autocrine motility factor/glucose-6-phosphate isomerase is a possible predictor of metastasis in bone and soft tissue tumours. J Pathol. 2006;208:44-53.
²⁷
Kato H, Semba S, Miskad UA, Seo Y, Kasuga M, Yokozaki H. High expression of PRL-3 promotes cancer cell motility and liver metastasis in human colorectal cancer: a predictive molecular marker of metachronous liver and lung metastases. Clin Cancer Res. 2004;10:7318–28.
²⁸
Azuma T, Witke W, Stossel TP, Hartwig JH, Kwiatkowski DJ. Gelsolin is a downstream effector of rac for fibroblast motility. EMBO J. 1998;17:1362–70.
²⁹
Crowley MR, Head KL, Kwiatkowski DJ, Asch HL, Asch BB. The mouse mammary gland requires the actin-binding protein gelsolin for proper ductal morphogenesis. Dev Biol. 2000;225:407–23.

Publication Dates

Publication in this collection
16 Jan 2023
Date of issue
2022

History

Received
07 Apr 2021
Accepted
11 May 2021
Published
03 June 2021

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.

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Awada A, Lalami Y. Molecular markers, molecular-targeted therapies and taxanes: how to integrate the progress into clinical research and practice for the management of head and neck cancers. Curr Opin Oncol. 2005;17:209–11.

[18] ¹⁸
Krecicki T, Smigiel R, Fraczek M, Kowalczyk M, Sasiadek MM. Studies of the cell cycle regulatory proteins P16, cyclin D1 and retinoblastoma protein in laryngeal carcinoma tissue. J Laryngol Otol. 2004;118:676–80.

[19] ¹⁹
Kontos C, ChristodoulouM-I, Scorilas A. Apoptosis-related BCL2-family members: key players in chemotherapy. Anticancer Agents Med Chem. 2014;14:353–74.

[20] ²⁰
Landes T, Martinou J-C. Mitochondrial outer membrane permeabilization during apoptosis: the role of mitochondrial fission. Biochim Biophys Acta - Mol Cell Res. 2011;1813:540–5.

[21] ²¹
Kusano H, Shimizu S, Koya RC, Fujita H, Kamada S, Kuzumaki N, et al. Human gelsolin prevents apoptosis by inhibiting apoptotic mitochondrial changes via closing VDAC. Oncogene. 2000;19:4807–14.

[22] ²²
Wang PW, Abedini MR, Yang LX, Ding AA, Figeys D, Chang JY, et al. Gelsolin regulates cisplatin sensitivity in human head-and-neck cancer. Int J Cancer. 2014;135:2760–9.

[23] ²³
Visapää H, Bui M, Huang Y, Seligson D, Tsai H, Pantuck A, et al. Correlation of Ki-67 and gelsolin expression to clinical outcome in renal clear cell carcinoma. Urology. 2003;61:845–50.

[24] ²⁴
Yang J, Tan D, Asch HL, Swede H, Bepler G, Geradts J, et al. Prognostic significance of gelsolin expression level and variability in non-small cell lung cancer. Lung Cancer. 2004;46:29–42.

[25] ²⁵
Yamazaki D, Kurisu S, Takenawa T. Regulation of cancer cell motility through actin reorganization. Cancer Sci. 2005;96:379–86.

[26] ²⁶
Dobashi Y, Watanabe H, Matsubara M, Yanagawa T, Raz A, Shimamiya T, et al. Autocrine motility factor/glucose-6-phosphate isomerase is a possible predictor of metastasis in bone and soft tissue tumours. J Pathol. 2006;208:44-53.

[27] ²⁷
Kato H, Semba S, Miskad UA, Seo Y, Kasuga M, Yokozaki H. High expression of PRL-3 promotes cancer cell motility and liver metastasis in human colorectal cancer: a predictive molecular marker of metachronous liver and lung metastases. Clin Cancer Res. 2004;10:7318–28.

[28] ²⁸
Azuma T, Witke W, Stossel TP, Hartwig JH, Kwiatkowski DJ. Gelsolin is a downstream effector of rac for fibroblast motility. EMBO J. 1998;17:1362–70.

[29] ²⁹
Crowley MR, Head KL, Kwiatkowski DJ, Asch HL, Asch BB. The mouse mammary gland requires the actin-binding protein gelsolin for proper ductal morphogenesis. Dev Biol. 2000;225:407–23.

Characteristics	Gelsolin expression
	Nº of cases (%)	Negative (n, %)	Positive (n, %)	p-value
Age
≤ 60	73 (43.4%)	22 (30.1%)	51 (69.9%)	0.794
> 60	95 (56.6%)	28 (29.4%)	67 (70.6%)
Sex
Male	158 (5.9%)	47 (29.8%)	111 (70.2%)	0.937
Female	10 (94.1%)	3 (30%)	7 (70%)
Location
Glottis	108 (64.2%)	35 (32.5%)	73 (67.5%)
Supraglottis	55 (32.9%)	14 (25.5)	41 (74.5%)	0.623
Subglottis	5 (2.9%)	1 (20%)	4 (80%)
Histological grade
Grade I	66 (39.2%)	25 (37.9%)	41 (62.1%)	0.031
Grade II	82 (48.8%)	21 (25.7%)	61 (74.3%)
Grade III	20 (11.9%)	4 (20%)	16 (80%)
TNM stage
I–II	64 (38%)	29 (45.4%)	35 (54.6%)	0.001
III -IV	104 (62%)	21 (20.2%)	83 (79.8%)
Lymph node status
Negative	113 (67.3%)	34 (31.1%)	79 (69.9%)	0.326
Positive	55 (32.7%)	16 (29.1%)	39 (70.9%)
PNI
Yes	36 (21.4%)	9 (25.0%)	27 (75.0%)	0.872
No	132 (78.6%)	41 (31.1)	91 (68.9%)
LVI
Yes	53 (31.5%)	10 (24.6%)	43 (81.1)	0.016
No	115 (68.5%)	40 (34.8%)	75 (65.2%)
Loco-regional recurrence
Yes	60 (35.7%)	9 (15%)	51 (85%)	0.018
No	108 (64.3)	41 (37.9%)	67 (62.1%)

	Univariate analysis			Multivariate analysis
	HR	95% CI	p-value	HR	95% CI	p-value
Age
≤ 60	1.00	0.96–1.07	0.351	1.00	1.01–1.27	0.498
> 60	1.02	0.96–1.07	0.351	1.16	1.01–1.27	0.498
Sex
Female	1.00	0.42–2.61	0.857	1.00	0.49–2.12	0.630
Male	1.07	0.42–2.61	0.857	1.09	0.49–2.12	0.630
Location
Glottis-subglottis	1.00	1.02–1.93	0.492	1.00	1.12–2.14	0.412
Supraglottis	1.17	1.02–1.93	0.492	1.27	1.12–2.14	0.412
Histological grade
Grade I–II	1.00	0.95–2.02	0.212	1.00	1.05–1.85	0.087
Grade III	1.14	0.95–2.02	0.212	1.28	1.05–1.85	0.087
TNM stage
I–II	1.00	1.03–4.37	0.031	1.00	1.21–4.37	0.001
III–IV	2.15	1.03–4.37	0.031	2.55	1.21–4.37	0.001
Lymph node
Negative	1.00	1.41–5.4	0.001	1.00	1.10–4.1	0.069
Positive	2.08	1.41–5.4	0.001	1.38	1.10–4.1	0.069
PNI
No	1.00	0.89–4.53	0.041	1.00	0.83–2.94	0.093
Yes	1.65	0.89–4.53	0.041	1.15	0.83–2.94	0.093
LVI
No	1.00	1.23–5.48	0.002	1.00	1.15–4.92	0.021
Yes	2.69	1.23–5.48	0.002	2.38	1.15–4.92	0.021
Gelsolin expression
Negative	1.00	1.67–7.47	0.004	1.00	1.27–6.67	0.025
Positive	3.28	1.67–7.47	0.004	2.63	1.27–6.67	0.025

	Univariate analysis			Multivariate analysis
	HR	95% CI	p-value	HR	95% CI	p-value
Age
≤ 60	1.00	0.93–1.05	0.528	1.00	0.99–1.10	0.694
> 60	1.01	0.93–1.05	0.528	1.11	0.99–1.10	0.694
Sex
Female	1.00	0.47–2.94	0.941	1.00	0.41–2.19	0.672
Male	1.03	0.47–2.94	0.941	1.05	0.41–2.19	0.672
Location
Glottis-subglottis	1.00	1.13–8.71	0.081	1.00	1.61–8.41	0.073
Supraglottis	2.15	1.13–8.71	0.081	2.94	1.61–8.41	0.073
Histological grade
Grade I–II	1.00	0.95–3.61	0.134	1.00	1.25–6.62	0.064
Grade III	1.2	0.95–3.61	0.134	1.3	1.25–6.62	0.064
TNM stage
I–II	1.00	1.01–3.94	0.014	1.00	0.89–3.03	0.014
III–IV	2.03	1.01–3.94	0.014	1.83	0.89–3.03	0.014
Lymph node
Negative	1.00	1.65–6.15	0.001	1.00	1.44–6.33	0.015
Positive	3.23	1.65–6.15	0.001	3.01	1.44–6.33	0.015
PNI
No	1.00	0.43–2.45	0.806	1.00	0.49–2.19	0.749
Yes	1.29	0.43–2.45	0.806	1.03	0.49–2.19	0.749
LVI
No	1.00	0.89–3.8	0.002	1.00	0.86–4.14	0.047
Yes	1.97	0.89–3.8	0.002	2.31	0.86–4.14	0.047
Gelsolin expression
Negative	1.00	1.32–9.38	0.030	1.00	1.49–8.12	0.020
Positive	2.86	1.32–9.38	0.030	3.51	1.49–8.12	0.020