Transcriptomics analysis identified ezrin as a potential druggable target in cervical and gastric cancer cells

Carvalho, Maria Fernanda Lopes; Calicchio, Carolina Santana; Almeida, Bruna Oliveira de; Miranda, Livia Bassani Lins de; Silva, Jean Carlos Lipreri da; Lima, Keli; Machado-Neto, João Agostinho

doi:10.1016/j.clinsp.2024.100422

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Original articles • Clinics 79 • 2024 • https://doi.org/10.1016/j.clinsp.2024.100422 copy

Transcriptomics analysis identified ezrin as a potential druggable target in cervical and gastric cancer cells

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Objective:

Cancer genomics and transcriptomics studies have provided a large volume of data that enables to test of hypotheses based on real data from cancer patients. Ezrin (encoded by the EZR gene) is a highly expressed protein in cancer that contributes to linking the actin cytoskeleton to the cell membrane and signal transduction pathways involved in oncogenesis and disease progression. NSC305787 is a pharmacological ezrin inhibitor with potential antineoplastic effects. In the present study, the authors prospected EZR mRNA levels in a pan-cancer analysis and identified potential cancers that could benefit from anti-EZR therapies.

Methods:

This study analyzed TCGA data for 32 cancer types, emphasizing cervical squamous cell carcinoma and stomach adenocarcinoma. It investigated the impact of EZR transcript levels on clinical outcomes and identified differentially expressed genes. Cell lines were treated with NSC305787, and its effects were assessed through various cellular and molecular assays.

Results:

EZR mRNA levels are highly expressed, and their expression is associated with biologically relevant molecular processes in cervical squamous carcinoma and stomach adenocarcinoma. In cellular models of cervical and gastric cancer, NSC305787 reduces cell viability and clonal growth (p < 0.05). Molecular analyses indicate that the pharmacological inhibition of EZR induces molecular markers of cell death and DNA damage, in addition, to promoting the expression of genes associated with apoptosis and inhibiting the expression of genes related to survival and proliferation.

Conclusion:

The present findings provide promising evidence that ezrin may be a molecular target in the treatment of cervical and gastric carcinoma.

Keywords:
Ezrin; Transcriptomics; Cervical cancer; Gastric cancer; Pharmacology

HIGHLIGHTS

Ezrin (EZR) is involved in oncogenesis and disease progression.

EZR is highly expressed in cervical squamous cell carcinoma and stomach adenocarcinoma.

NSC305787, an EZR inhibitor, reduces cell viability and clonal growth in cervical and gastric cancer cells.

EZR may be a molecular target in the treatment of cervical and gastric carcinoma.

Clinicopathological factors		EZR, n (%)
Clinicopathological factors	n	Low	High	p-value^a a Missing values were excluded from calculation of p-values.
Total	294	97 (33.0)	197 (67.0)
Age				0.812
< 60	231	77 (33.3)	154 (67.7)
≥ 60	63	20 (31.7)	43 (68.3)
Total	234	77 (32.9)	157 (67.1)
Primary tumor size (TNM system)				0.736
T1 and T2	206	67 (32.5)	139 (67.5)
T3 and T4	28	10 (35.7)	18 (64.3)
Total	186	60 (32.3)	126 (67.7)
Regional lymph node metastasis (TNM system)				0.136
N0	129	46 (35.7)	83 (64.3)
N1, N2 and N3	57	14 (24.6)	43 (75.4)
Total	120	47 (39.2)	73 (60.8)
Distant metastasis (TNM system)				0.079
M0	111	41 (36.9)	70 (63.1)
M1	9	6 (66.7)	3 (33.3)
Total	262	92 (35.1)	170 (64.9)
Histological grade				0.337
G1	17	5 (29.5)	12 (70.6)
G2	130	41 (31.5)	89 (68.5)
G3	115	46 (40)	69 (60)

Clinicopathological factors		EZR, n (%)
Clinicopathological factors	n	Low	High	p-value^a a Missing values were excluded from calculation of p-values.
Total	408	203 (49.8)	205 (50.2)
Age				0.05
< 60	121	69 (57.0)	52 (43.0)
≥ 60	287	134 (46.7)	153 (53.3)
Total	412	206 (50.0)	206 (50.0)
Sex				0.92
Female	145	73 (50.3)	72 (49.7)
Male	267	133 (49.8)	134 (50.2)
Total	403	203 (50.4)	200 (49.6)
Primary tumor size (TNM system)				0.89
T1 and T2	108	55 (54.4)	53 (53.6)
T3 and T4	295	148 (50.2)	147 (49.8)
Total	394	198 (50.3)	196 (49.7)
Regional lymph node metastasis (TNM system)				0.71
N0	122	63 (51.6)	59 (48.4)
N1, N2 and N3	172	135 (49.6)	137 (50.4)
Total	392	200 (51.0)	192 (49.0)	0.47
Distant metastasis (TNM system)
M0	367	189 (51.5)	178 (48.5)
M1	25	11 (44.0)	14 (56.0)
Total	394	199 (50.5)	195 (49.5)
TNM stage				0.70
Stage I and II	180	89 (49.4)	91 (50.6)
Stage III and IV	214	110 (51.4)	104 (48.6)
Total	375	185 (49.3)	190 (50.7)
Molecular subtype				<0.0001
Genomically stable	50	36 (72.0)	14 (28.0)
Epstein-Barr virus	29	10 (34.5)	19 (65.5)
Chromosomal instability	223	124 (55.6)	99 (44.4)
Microsatellite instability	73	15 (20.5)	58 (79.5)
Total	403	202 (50.1)	201(49.9)
Histological grade				0.48
G1	12	8 (66.7)	4 (33.3)
G2	144	73 (50.7)	71 (49.3)
G3	247	121 (49.0)	126 (51.0)

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[1] *Corresponding author. E-mail address:jamachadoneto@usp.br (J.A. Machado-Neto).