Monitoring of the prostate tumour cells redox state and
real-time proliferation by novel biophysical techniques and
fluorescent staining

MASAŘÍK, Michal, Jaromír GUMULEC, Marián HLAVNA, Markéta SZTALMACHOVÁ, Petr BABULA, Martina RAUDENSKÁ, Monika PÁVKOVÁ GOLDBERGOVÁ, Natalia Vladimirovna CERNEI, Jiří SOCHOR, Ondřej ZÍTKA, Branislav RUTTKAY-NEDECKÝ, Soňa KŘÍŽKOVÁ, Vojtěch ADAM a René KIZEK. Monitoring of the prostate tumour cells redox state and real-time proliferation by novel biophysical techniques and fluorescent staining. Integrative Biology. 2012, roč. 4, č. 6, s. 672–684. ISSN 1757-9694. Dostupné z: https://dx.doi.org/10.1039/c2ib00157h.

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TY  - JOUR
ID  - 984961
AU  - Masařík, Michal - Gumulec, Jaromír - Hlavna, Marián - Sztalmachová, Markéta - Babula, Petr - Raudenská, Martina - Pávková Goldbergová, Monika - Cernei, Natalia Vladimirovna - Sochor, Jiří - Zítka, Ondřej - Ruttkay-Nedecký, Branislav - Křížková, Soňa - Adam, Vojtěch - Kizek, René
PY  - 2012
TI  - Monitoring of the prostate tumour cells redox state and real-time proliferation by novel biophysical techniques and fluorescent staining
JF  - Integrative Biology
VL  - 4
IS  - 6
SP  - 672–684
EP  - 672–684
SN  - 17579694
KW  - OXIDATIVE STRESS
KW  - CANCER CELLS
KW  - LIQUID-CHROMATOGRAPHY
KW  - CARCINOMA-CELLS
KW  - ACRIDINE-ORANGE
KW  - ZINC
KW  - METALLOTHIONEIN
KW  - DIFFERENTIATION
KW  - TRANSPORTER
KW  - GLUTATHIONE
N2  - The present paper is focused on zinc(II) treatment effects on prostatic cell lines PC-3 (tumour) and PNT1A (non-tumour). Oxidative status of cells was monitored by evaluation of expression of metallothionein (MT) isoforms 1A and 2A at the mRNA and protein level, glutathione (oxidised and reduced), and intracellular zinc(II) after exposition to zinc(II) treatment at concentrations of 0–150 mM using electrochemical methods, western blotting and fluorescent microscopy. A novel real-time impedance-based growth monitoring system was compared with widely used end-point MTT assay. Impedance-based IC50 for zinc(II) is 55.5 and 150.8 mM for PC-3 and PNT1A, respectively. MTTdetermined IC50 are >1.3-fold higher. Impedance-based viability correlates with viable count (r > 0.92; p o 0.03), not with MTT. Two-fold lower intracellular zinc(II) in the tumour PC-3 cell line was found. After zinc(II) treatment >2.6-fold increase of intracellular zinc(II) was observed in non-tumour PNT1A and in tumour PC-3 cells. In PC-3 cells, free and bound zinc(II) levels were enhanced more markedly as compared to PNT1A. PNT1A produced 4.2-fold less MT compared to PC3. PNT1A cells showed a 4.8-fold increase trend (r = 0.94; p = 0.005); PC-3 did show a significant trend at MT1 and MT2 protein levels (r = 0.93; p = 0.02) with nearly ten-fold increase after 100 mM zinc(II) treatment. In terms of redox state, PNT1A had a predominance of reduced GSH forms (GSH : GSSG ratio > 1), when exposed to zinc(II) compared to PC3, where predominance of oxidised forms remains at all concentrations. IC50 differs significantly when determined by MTT and real-time impedance-based assays due to dependence of impedance on cell morphology and adhesion. When real-time growth monitoring, precise electrochemical methods and fluorescent microscopy are performed together, accurate information for metal fluxes, their buffering by thiol compounds and monitoring of the redox state become a powerful tool for understanding the role of oxidative stress in carcinogenesis.
ER  -

Základní údaje
Originální název	Monitoring of the prostate tumour cells redox state and real-time proliferation by novel biophysical techniques and fluorescent staining
Autoři	MASAŘÍK, Michal (203 Česká republika, garant, domácí), Jaromír GUMULEC (203 Česká republika, domácí), Marián HLAVNA (703 Slovensko, domácí), Markéta SZTALMACHOVÁ (203 Česká republika, domácí), Petr BABULA (203 Česká republika), Martina RAUDENSKÁ (203 Česká republika, domácí), Monika PÁVKOVÁ GOLDBERGOVÁ (203 Česká republika, domácí), Natalia Vladimirovna CERNEI (498 Moldavsko), Jiří SOCHOR (203 Česká republika), Ondřej ZÍTKA (203 Česká republika), Branislav RUTTKAY-NEDECKÝ (203 Česká republika), Soňa KŘÍŽKOVÁ (203 Česká republika), Vojtěch ADAM (203 Česká republika) a René KIZEK (203 Česká republika).
Vydání	Integrative Biology, 2012, 1757-9694.

Další údaje
Originální jazyk	angličtina
Typ výsledku	Článek v odborném periodiku
Obor	30000 3. Medical and Health Sciences
Stát vydavatele	Velká Británie a Severní Irsko
Utajení	není předmětem státního či obchodního tajemství
Impakt faktor	Impact factor: 4.321
Kód RIV	RIV/00216224:14110/12:00057446
Organizační jednotka	Lékařská fakulta
Doi	http://dx.doi.org/10.1039/c2ib00157h
UT WoS	000304487300010
Klíčová slova anglicky	OXIDATIVE STRESS; CANCER CELLS; LIQUID-CHROMATOGRAPHY; CARCINOMA-CELLS; ACRIDINE-ORANGE; ZINC; METALLOTHIONEIN; DIFFERENTIATION; TRANSPORTER; GLUTATHIONE
Příznaky	Mezinárodní význam
Změnil	Změnila: Ing. Mgr. Věra Pospíšilíková, učo 9005. Změněno: 25. 3. 2013 14:56.

Anotace

The present paper is focused on zinc(II) treatment effects on prostatic cell lines PC-3 (tumour) and PNT1A (non-tumour). Oxidative status of cells was monitored by evaluation of expression of metallothionein (MT) isoforms 1A and 2A at the mRNA and protein level, glutathione (oxidised and reduced), and intracellular zinc(II) after exposition to zinc(II) treatment at concentrations of 0–150 mM using electrochemical methods, western blotting and fluorescent microscopy. A novel real-time impedance-based growth monitoring system was compared with widely used end-point MTT assay. Impedance-based IC50 for zinc(II) is 55.5 and 150.8 mM for PC-3 and PNT1A, respectively. MTTdetermined IC50 are >1.3-fold higher. Impedance-based viability correlates with viable count (r > 0.92; p o 0.03), not with MTT. Two-fold lower intracellular zinc(II) in the tumour PC-3 cell line was found. After zinc(II) treatment >2.6-fold increase of intracellular zinc(II) was observed in non-tumour PNT1A and in tumour PC-3 cells. In PC-3 cells, free and bound zinc(II) levels were enhanced more markedly as compared to PNT1A. PNT1A produced 4.2-fold less MT compared to PC3. PNT1A cells showed a 4.8-fold increase trend (r = 0.94; p = 0.005); PC-3 did show a significant trend at MT1 and MT2 protein levels (r = 0.93; p = 0.02) with nearly ten-fold increase after 100 mM zinc(II) treatment. In terms of redox state, PNT1A had a predominance of reduced GSH forms (GSH : GSSG ratio > 1), when exposed to zinc(II) compared to PC3, where predominance of oxidised forms remains at all concentrations. IC50 differs significantly when determined by MTT and real-time impedance-based assays due to dependence of impedance on cell morphology and adhesion. When real-time growth monitoring, precise electrochemical methods and fluorescent microscopy are performed together, accurate information for metal fluxes, their buffering by thiol compounds and monitoring of the redox state become a powerful tool for understanding the role of oxidative stress in carcinogenesis.

Návaznosti
GP301/09/P436, projekt VaV	Název: Analýza metalothioneinu u karcinomu prostaty na úrovni DNA, RNA a proteinu.
GP301/09/P436, projekt VaV	Investor: Grantová agentura ČR, Analýza metalothioneinu u karcinomu prostaty na úrovni DNA, RNA a proteinu
MUNI/A/0839/2011, interní kód MU	Název: Patofyziologické aspekty vybraných genotypů a fenotypů komplexních nemocí (Akronym: Patofyziologie komplexních nemocí)
MUNI/A/0839/2011, interní kód MU	Investor: Masarykova univerzita, Patofyziologické aspekty vybraných genotypů a fenotypů komplexních nemocí, DO R. 2020_Kategorie A - Specifický výzkum - Studentské výzkumné projekty

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Monitoring of the prostate tumour cells redox state and real-time proliferation by novel ...

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