Exploration of the prognostic markers of multiple myeloma based on
cuproptosis-related genes
- Xiao-Han Gao,
- * Jun-Yuan,
- Xiao-Xia Zhang,
- Rui-Cang Wang,
- Jie Yang,
- Yan Li,
- Jie Li
Xiao-Han Gao
Hebei General Hospital Affiliated to Hebei Medicine University
Author Profile* Jun-Yuan
Hebei General Hospital Affiliated to Hebei Medicine University
Author ProfileXiao-Xia Zhang
Hebei General Hospital Affiliated to Hebei Medicine University
Author ProfileRui-Cang Wang
Hebei General Hospital Affiliated to Hebei Medicine University
Author ProfileJie Yang
Hebei General Hospital Affiliated to Hebei Medicine University
Author ProfileYan Li
Hebei General Hospital Affiliated to Hebei Medicine University
Author ProfileAbstract
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Background: The investigation of cuproptosis in relation to
tumor development has been limited, particularly in Multiple myeloma
(MM), indicating the need for further research. Our study aimed to
examine the impact of cuproptosis-related genes on the prognosis of MM.
Methods: Using the datasets, we filtered cuproptosis
score-related differentially expressed genes (CRDEGs) by overlapping the
DEGs between the MM and normal groups and between the high and low
cuproptosis score groups. Additionally, key module genes were identified
through weighted gene co-expression network analysis. A univariate Cox
algorithm and multivariate Cox analysis were employed to obtain
biomarkers of MM and build a prognostic model, before conducting
independent prognostic analysis. Results: A total of 59 CRDEGs
were filtered. Demonstrating their involvement in the COPII vesicle coat
and endoplasmic reticulum protein processing and protein processing in
the endoplasmic reticulum. Six prognosis-related biomarkers (PARP1,
EDEM3, SEC23A, RSL24D1, TTC37, and SRP72) were obtained, and a
prognostic model was developed. The performance of the model was
verified using a test cohort (GSE136324 dataset) and a validation cohort
(GSE24080 dataset). Risk score, age, albumin, International Staging
System (ISS) score, and β2-microglobulin (B2M) was found to be a
significant predictor of prognosis independently . Conclusion:
As a result of this investigation, a set of six biomarkers associated
with cuproptosis (PARP1, EDEM3, SEC23A, RSL24D1, TTC37 and SRP72) were
screened to provide a basis for predicting the prognosis of MM.20 Aug 2024Submitted to Cancer Reports 27 Aug 2024Submission Checks Completed
27 Aug 2024Assigned to Editor
27 Aug 2024Review(s) Completed, Editorial Evaluation Pending
28 Aug 2024Reviewer(s) Assigned
24 Oct 2024Editorial Decision: Revise Major
19 Nov 20241st Revision Received
20 Nov 2024Submission Checks Completed
20 Nov 2024Assigned to Editor
20 Nov 2024Review(s) Completed, Editorial Evaluation Pending
20 Nov 2024Reviewer(s) Assigned