Serum Amyloid A1 in Combination with Integrin αVβ3 Increases Glioblastoma Cells Mobility and Progression

Overview

Journal Mol Oncol

Specialties Molecular Biology
Oncology

Date 2018 Apr 1

PMID 29603594

Citations 17

Authors

Ching-Yu Lin

Shun-Tai Yang

Shing-Chuan Shen

Yi-Chen Hsieh

Fei-Ting Hsu

Cheng-Yu Chen

Yung-Hsiao Chiang

Jian-Ying Chuang

Kai-Yun Chen

Tsung-I Hsu

Wan-Chong Leong

Yu-Kai Su

Wei-Lun Lo

Yi-Shian Yeh

Yudha Nur Patria

Hsiu-Ming Shih

Che-Chang Chang

Szu-Yi Chou

Affiliations

Soon will be listed here.

Abstract

Glioblastoma multiforme (GBM) is a highly malignant type of brain tumor found in humans. GBM cells reproduce quickly, and the median survival time for patients after therapy is approximately 1 year with a high relapse rate. Current therapies and diagnostic tools for GBM are limited; therefore, we searched for a more favorable therapeutic target or marker protein for both therapy and diagnosis. We used mass spectrometry (MS) analysis to identify GBM-associated marker proteins from human plasma and GBM cell cultures. Additional plasma and 52 brain tissues obtained from patients with gliomas were used to validate the association rate of serum amyloid A1 (SAA1) in different grades of gliomas and its distribution in tumors. Microarray database analysis further validated the coefficient of SAA1 levels in gliomas. The cellular mechanisms of SAA1 in GBM proliferation and infiltration were investigated in vitro. We analyzed the correlation between SAA1 and patients' medication requirement to demonstrate the clinical effects of SAA1 in GBM. SAA1 was identified from MS analysis, and its level was revealed to be correlated with the disease grade, clinical severity, and survival rate of patients with gliomas. In vitro cultures, including GBM cells and normal astrocytes, revealed that SAA1 promotes cell migration and invasion through integrin αVβ3 to activate the Erk signaling pathway. Magnetic resonance imaging and tumor region-specific microarray analysis identified a correlation between SAA1 and GBM cell infiltration in patients. In summary, our results demonstrate that SAA1 in combination with integrin αV and β3 can serve as an indicator of high glioblastoma risk. We also identified the cellular mechanisms of SAA1 contributing to GBM progression, which can serve as the basis for future GBM therapy.

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