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Silencing the Metallothionein‐2A Gene Induces Entosis in Adherent MCF‐7 Breast Cancer Cells
Author(s) -
Lai Yiyang,
Lim Daina,
Tan PuayHoon,
Leung Thomas KingChor,
Yip George WaiCheong,
Bay BoonHuat
Publication year - 2010
Publication title -
the anatomical record: advances in integrative anatomy and evolutionary biology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.678
H-Index - 62
eISSN - 1932-8494
pISSN - 1932-8486
DOI - 10.1002/ar.21215
Subject(s) - gene silencing , microbiology and biotechnology , downregulation and upregulation , biology , autophagy , cell , cytoplasm , metallothionein , cancer research , transfection , gene expression , gene , genetics , apoptosis
The presence of a live cell cohabiting within another cell has fascinated scientists for many decades. Far from being a spurious event, many have attempted to uncover the molecular mechanism underlying this phenomenon. In this study, we observed anchorage‐dependent MCF‐7 cells internalizing neighboring epithelial cells (entosis) after siRNA‐mediated silencing of the Metallothionein‐2A (MT‐2A ) gene. MTs belong to a family of low‐molecular weight proteins, which bind metal ions endogenously and its over‐expression has been reported in a variety of cancers that include breast, prostate, and colon. We provide microscopic evidence at light and ultrastructural levels of the occurrence of entosis after altering MT expression in a subpopulation of MCF‐7 breast cancer cells by silencing the MT‐2A gene. Our results demonstrate that adheren junctions may play important roles in the formation of cell‐in‐cell cytostructure after MT‐2A gene downregulation and the entotic process does not appear to involve genes associated with autophagy. Interiorized cells often underwent lysosomal degradation within the cytoplasmic body of the engulfing cell. It would appear that a subset of breast cancer cells could die via entosis after MT‐2A gene silencing. Anat Rec 293:1685–1691, 2010. © 2010 Wiley‐Liss, Inc.