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Investigator

Mohthash Musambil

Post Doctoral Fellow Scientist · CHU de Liege Laboratoire-Unilab Lg, Molecular and Cellular Epigenetics

About

Papers

Tissue-Based Proteomic Profiling in Patients with Hyperplasia and Endometrial Cancer

Uterine cancers are among the most prevalent gynecological malignancies, and endometrial cancer (EC) is the most common in this group. This study used tissue-based proteomic profiling analysis in patients with endometrial cancer and hyperplasia, and control patients. Conventional 2D gel electrophoresis, followed by a mass spectrometry approach with bioinformatics, including a network pathway analysis pipeline, was used to identify differentially expressed proteins and associated metabolic pathways between the study groups. Thirty-six patients (twelve with endometrial cancer, twelve with hyperplasia, and twelve controls) were enrolled in this study. The mean age of the participants was 46–75 years. Eighty-seven proteins were significantly differentially expressed between the study groups, of which fifty-three were significantly differentially regulated (twenty-eight upregulated and twenty-five downregulated) in the tissue samples of EC patients compared to the control (Ctrl). Furthermore, 26 proteins were significantly dysregulated (8 upregulated and 18 downregulated) in tissue samples of hyperplasia (HY) patients compared to Ctrl. Thirty-two proteins (nineteen upregulated and thirteen downregulated) including desmin, peptidyl prolyl cis-trans isomerase A, and zinc finger protein 844 were downregulated in the EC group compared to the HY group. Additionally, fructose bisphosphate aldolase A, alpha enolase, and keratin type 1 cytoskeletal 10 were upregulated in the EC group compared to those in the HY group. The proteins identified in this study were known to regulate cellular processes (36%), followed by biological regulation (16%). Ingenuity pathway analysis found that proteins that are differentially expressed between EC and HY are linked to AKT, ACTA2, and other signaling pathways. The panels of protein markers identified in this study could be used as potential biomarkers for distinguishing between EC and HY and early diagnosis and progression of EC from hyperplasia and normal patients.

36Works

1Papers

7Collaborators

Positions

2022–

Post Doctoral Fellow Scientist

CHU de Liege Laboratoire-Unilab Lg · Molecular and Cellular Epigenetics

2015–

Researcher

King Saud University · Strategic Centre for Diabetic Research

2014–

Research Assistant (Scientific)

MES Medical College · Centre For Biomedical Research

2014–

Trainee Molecular Biology

SCDR King Saud University Riyadh · Diabetes Research Centre

2013–

Medical Technologist

Modern Multi Speciality hospital · Molecualr Biology-Genetics

2012–

Molecular biologist trainee

Manipal Life Sciences Centre, Manipal University · Molecular Biology

Education

2013

MSc.Medical Biotechnology

School of Life Science , Manipal University · Life Sciences

2011

BSc.Biotechnology,Biochemistry,Genetics

Garden City College · Biotechnology

Country

Links & IDs

0000-0003-2402-9628

Scopus: 56403330900

Researcher Id: K-1242-2014