Up-regulation of GINS1 highlighted a good diagnostic and prognostic potential of survival in three different subtypes of human cancer

Ahmad, M.; Hameed, Y.; Khan, M.; Usman, M; Rehman, A.; Abid, U.; Asif, R.; Ahmed, H.; Hussain, M. S.; Rehman, J. U.; Asif, H. M.; Arshad, R.; Atif, M.; Hadi, A.; Sarfraz, U.; Khurshid, U.

doi:10.1590/1519-6984.250575

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Brazilian Journal of Biology

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Original Article • Braz. J. Biol. 84 • 2024 • https://doi.org/10.1590/1519-6984.250575 copy

Up-regulation of GINS1 highlighted a good diagnostic and prognostic potential of survival in three different subtypes of human cancer

A regulação positiva de GINS1 destacou um bom potencial diagnóstico e prognóstico de sobrevivência em três subtipos diferentes de câncer humano

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Cancer is a fatal malignancy and its increasing worldwide prevalence demands the discovery of more sensitive and reliable molecular biomarkers. To investigate the GINS1 expression level and its prognostic value in distinct human cancers using a series of multi-layered in silico approach may help to establish it as a potential shared diagnostic and prognostic biomarker of different cancer subtypes. The GINS1 mRNA, protein expression, and promoter methylation were analyzed using UALCAN and Human Protein Atlas (HPA), while mRNA expression was further validated via GENT2. The potential prognostic values of GINS1 were evaluated through KM plotter. Then, cBioPortal was utilized to examine the GINS1-related genetic mutations and copy number variations (CNVs), while pathway enrichment analysis was performed using DAVID. Moreover, a correlational analysis between GINS1 expression and CD8+ T immune cells and a the construction of gene-drug interaction network was performed using TIMER, CDT, and Cytoscape. The GINS1 was found down-regulated in a single subtypes of human cancer while commonly up-regulated in 23 different other subtypes. The up-regulation of GINS1 was significantly correlated with the poor overall survival (OS) of Liver Hepatocellular Carcinoma (LIHC), Lung Adenocarcinoma (LUAD), and Kidney renal clear cell carcinoma (KIRC). The GINS1 was also found up-regulated in LIHC, LUAD, and KIRC patients of different clinicopathological features. Pathways enrichment analysis revealed the involvement of GINS1 in two diverse pathways, while few interesting correlations were also documented between GINS1 expression and its promoter methylation level, CD8+ T immune cells level, and CNVs. Moreover, we also predicted few drugs that could be used in the treatment of LIHC, LUAD, and KIRC by regulating the GINS1 expression. The expression profiling of GINS1 in the current study has suggested it a novel shared diagnostic and prognostic biomarker of LIHC, LUAD, and KIRC.

Keywords:
cancer; diagnostic; CD8+ T immune cells; GINS1; OS analysis; prognostic

Clinicopathological features of the LIHC cohort
Sr. No	Clinicopathological Feature	No. Samples			Total no. of LIHC samples	No. Excluded Samples with Missing Information		Total No. of Included Samples
	Cancer stage based distribution
	Stage 1
	Stage 2	168
1	Stage 3	84				31		340
	Stage 4	82
		6
	Gender based distribution
2	Male	245				9		362
	Female	117			371
	Age based distribution
	21-40 years	27
3	41-60 years	140				13		358
	61-80 years	181
	81-100 years	10
	Nodal metastasis based distribution
4	N0
	N1	252				115		256
		4
Clinicopathological features of the LUAD cohort
Sr. No	Clinicopathological Feature		No. Samples	Total no. of LUAD samples			No. Excluded Samples with Missing Information		Total No. of Included Samples
	Cancer stage based distribution
	Stage 1
	Stage 2		277
1	Stage 3		125				0		515
	Stage 4		85
			28
	Gender based distribution			515
2	Male		238				1		514
	Female		276
	Age based distribution
	21-40 years		12
3	41-60 years		90				232		283
	61-80 years		149
	81-100 years		32
	Nodal metastasis based distribution
	N0
4	N1		331
	N2		96				13		503
	N3		74
			2
Clinicopathological features of the KIRC cohort
Sr. No	Clinicopathological Feature		No. Samples	Total no. of KIRC samples			No. Excluded Samples with Missing Information		Total No. of Included Samples
	Cancer stage distribution
1	Stage 1		267
	Stage 2		57				2		531
	Stage 3		123
	Stage 4		84
	Gender distribution
3	Male		345				0		533
	Female		188	533
	Age distribution
	21-40 years		26
2	41-60 years		238				0		533
	61-80 years		246
	81-100 years		23
	Geographical distribution
4	N0		240				277		256
	N1		16

Sr. No	Cancer	Datasets	Source
1	LIHC	GSE45436, GSE49515, GSE2109, GSE58208, GSE6222, GSE62232, GSE6764, GSE75285, GSE9843, GSE40367, and GSE40873, GSE41804	Affymetrix U133A and U133 Plus2 microarray platforms
2	LUAD	GSE40791, GSE37745, GSE2109, GSE43346, GSE43580, GSE50081, GSE30219, GSE63074, GSE64766, GSE77803, GSE10445, GSE19188, GSE27262, GSE33532, GSE40791, GSE5058, and GSE7307
3	KIRC	GSE2109, GSE46699, GSE47352, GSE53224, GSE53757, GSE7023, GSE68629, GSE7392, GSE8271, GSE11045, GSE11151, GSE12090, GSE12606, GSE14762, GSE19982, GSE22541, GSE36895, GSE53757, and GSE11151

Pathway ID	Pathway Name	Gene count	P-value	Gene name
04110	Cell cycle	6	<0.05	CDC45, MCM7, MCM3, MCM4, MCM5, MCM6
03030	DNA replication	5	<0.05	MCM7, MCM3, MCM4, MCM5, MCM6

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[1] *e-mail: yasirhameed2011@gmail.com