Journal of Andrology, Vol. 25, No. 1, January/February 2004
Copyright © American Society of Andrology
Zinc and Metallothionein Levels and Expression of Zinc Transporters in Androgen-Independent Subline of LNCaP Cells
KAZUHIRO IGUCHI*,
TAKASHI OTSUKA*,
SHIGEYUKI USUI*,
KENICHIRO ISHII
,
TAKEHISA ONISHI
,
YOSHIKI SUGIMURA
AND
KAZUYUKI HIRANO*
From the * Laboratory of Pharmaceutics, Gifu
Pharmaceutical University, Mitahora-higashi, Gifu, Japan;
Department of Urologic Surgery, Vanderbilt
University Medical Center, Nashville, Tennessee; and the
Department of Urology, Mie University School
of Medicine, Edobashi, Tsu, Mie, Japan.
|
Correspondence to: Dr Kazuyuki Hirano, Laboratory of Pharmaceutics, Gifu
Pharmaceutical University, 5-6-1 Mitahora-higashi, Gifu 502-8585, Japan
(e-mail:
hirano{at}gifu-pu.ac.jp). |
Zinc levels in the prostate have been reported to be associated with the
development and progression of malignant prostate cells. To investigate the
reason why the zinc content decreases during the progression of prostate
cancer to an androgen-independent state, we compared the expression levels of
metallothionein and zinc transporters between androgen-responsive LNCaP cells
and its androgen-independent subline, AIDL cells. AIDL cells showed lower zinc
levels than LNCaP cells and comparable levels of androgen receptor expression
to LNCaP cells, consistent with some clinical aspects of androgen-independent
prostatic cancer. AIDL cells exhibited a lower expression of zinc transporter
1 (ZnT1) and higher expression of ZnT3 than LNCaP cells. The content of
metallothionein, which is a major zinc-binding protein, was significantly
lower in AIDL cells than in LNCaP cells. Furthermore, the expression of ZnT3
mRNA was decreased by incubating LNCaP cells in medium containing
hormone-stripped fetal calf serum and increased by addition of synthetic
androgen R1881 to the medium, whereas the intracellular zinc levels were not
affected under these conditions. These findings suggest that factors such as
ZnT1 and metallothioneins other than ZnT3 are associated with the low
intracellular zinc content in AIDL cells.
Key words: Hormone-refractory, metallothionein, ZnT1, ZnT3
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Copyright © 2004 by The American Society of Andrology.