Expression of CD 44 S, CD 44 V 3 and CD 44 V 6 in Benign and Malignant Breast Lesions: Correlation and Colocalization with Hyaluronan

Overview

Journal Histopathology

Specialties Anatomy & Histology
Pathology

Date 2005 Sep 24

PMID 16178897

Citations 26

Authors

P Auvinen

R Tammi

M Tammi

R Johansson

V-M Kosma

Affiliations

Soon will be listed here.

Abstract

Aims: To examine the expression of CD 44 s, CD 44 v 3 and CD 44 v 6 in breast lesions, and to correlate it with the expression of hyaluronan (HA).

Methods And Results: CD 44 expression was studied in 75 breast tissue samples, consisting of benign, premalignant and malignant breast lesions, using immunohistochemistry. CD 44 s, but not CD 44 v 3 or CD 44 v 6, was found in the stromal cells, and it was similar in benign and malignant tumours. In benign lesions CD 4 v 6 was detected in 20-30% of the ductal epithelial cells, while C 44 v 3 and CD 44 s were not expressed. CD 44 s, CD 44 v 3 and CD 44 v 6 were all up-regulated in the in situ carcinomas and invasive carcinomas. The level of CD 44 expression in carcinoma cells did not correlate with the type or differentiation of the tumours. CD 44 and HA expression levels were not closely linked in the benign or malignant breast lesions, because HA was overexpressed later in breast cancer progression than CD 44. However, in breast carcinomas CD 44 and HA positivity was often found in the same areas of the sections, and the dual staining confirmed actual colocalization of CD 44 s and HA in the same cells.

Conclusions: CD 44 s, CD 44 v 3 and CD 44 v 6 are up-regulated earlier than HA in breast carcinoma progression, and in later stages they often colocalize with cell surface HA.

Citing Articles

Direct interaction of TrkA/CD44v3 is essential for NGF-promoted aggressiveness of breast cancer cells.

Trouvilliez S, Cicero J, Leveque R, Aubert L, Corbet C, Van Outryve A J Exp Clin Cancer Res. 2022; 41(1):110.

PMID: 35346305 PMC: 8962522. DOI: 10.1186/s13046-022-02314-4.

Hypoxia-induced alternative splicing in human diseases: the pledge, the turn, and the prestige.

Natua S, Ashok C, Shukla S Cell Mol Life Sci. 2021; 78(6):2729-2747.

PMID: 33386889 PMC: 11072330. DOI: 10.1007/s00018-020-03727-0.

Role of Mitochondria-Cytoskeleton Interactions in the Regulation of Mitochondrial Structure and Function in Cancer Stem Cells.

Kim J, Cheong J Cells. 2020; 9(7).

PMID: 32674438 PMC: 7407978. DOI: 10.3390/cells9071691.

Multifunctional, CD44v6-Targeted ORMOSIL Nanoparticles Enhance Drugs Toxicity in Cancer Cells.

Morillas-Becerril L, Peta E, Gabrielli L, Russo V, Lubian E, Nodari L Nanomaterials (Basel). 2020; 10(2).

PMID: 32050605 PMC: 7075197. DOI: 10.3390/nano10020298.

pH Responsive Polymer Micelles Enhances Inhibitory Efficacy on Metastasis of Murine Breast Cancer Cells.

Wang J, De G, Yue Q, Ma H, Cheng J, Zhu G Front Pharmacol. 2018; 9:543.

PMID: 29875669 PMC: 5974204. DOI: 10.3389/fphar.2018.00543.