Abstract
To investigate the toxicity and mutagenicity of NO, methods are needed to deliver it to cell cultures at known, constant rates. To permit continuous exposures over lengthy periods, we fabricated a simple apparatus utilizing gas-permeable polydimethylsiloxane (Silastic) tubing to supply both NO and O2 to a stirred, cylindrical vessel. Mass transfer in this system was characterized by measuring the delivery rates of NO or O2 alone, and of NO to air-saturated solutions. The concentrations of NO, O2 and NO −2 (the end product of NO oxidation) were monitored continuously. The total flux of nitrogen species into the liquid (as determined from the sum of NO and NO −2 accumulation) was 50%–90% greater in the presence of O2 depending on the NO partial pressure in the gas. Also, the simultaneously measured mass transfer coefficients for NO and O2 differed greatly from the corresponding unreactive values. An analysis of the data using diffusion-reaction models showed that NO oxidation in the aqueous boundary layer contributed very little to the nitrogen flux increase or to variations in the mass transfer coefficients. However, the unusually strong dependence of the delivery rates on chemical reactions could be explained by postulating that partial oxidation of NO to NO2 occurred within the membrane. The rate constant we estimated for polydimethylsiloxane, >4.4 × 105 M−2 s−1 at 23°C, is only about one-fifth of values reported previously for water and nonpolar solvents, but the high solubilities of NO and O2 in the polymer are sufficient to make NO2 formation significant. Although considerable NO2 is calculated to enter the liquid, its reaction with aqueous NO is rapid enough to keep this undesired compound at trace levels, except within a few microns of the tubing. Thus, cells will have little exposure to NO2. © 2003 Biomedical Engineering Society.
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REFERENCES
Buga, G. M., and L. J. Ignarro. Nitric oxide and cancer. In: Nitric Oxide Physiology and Pathology, edited by L. J. Ignarro. San Diego: Academic Press, 2000, pp. 895–920.
Deen, W. M. Analysis of Transport Phenomena. New York: Oxford University Press, 1998, pp. 422–429.
Estevez, A. G., N. Spear, H. Pelluffo, A. Kamaid, L. Barbeito, and J. S. Beckman. Examining apoptosis in cultured cells after exposure to nitric oxide and peroxynitrite. Methods Enzymol.301:393402, 1999.
Gasco, A., R. Fruttero, and G. Sorba. NO Donors: An emerging class of compounds in medicinal chemistry. Farmacognosia51:617635, 1996.
Graetzel, M., S. Taniguchi, and A. Henglein. Pulse radiolytic investigation of NO oxidation and equilibrium N2O3=NO+NO2 in aqueous solution. Ber. Bunsenges. Phys. Chem.74:488492, 1970.
Green, L. C., D. A. Wagner, J. Glogowski, P. L. Skipper, and J. S. Wishnok. Analysis of nitrate, nitrite, and 15NO3 − in biological fluids. Anal. Biochem.126:131138, 1982.
Kavdia, M., S. Nagarajan, and R. S. Lewis. Novel devices for the predictable delivery of nitric oxide to aqueous solutions. Chem. Res. Toxicol.11:13461351, 1998.
Kavdia, M., J. L. Stanfield, and R. S. Lewis. Nitric oxide, superoxide, and peroxynitrite effects on the insulin secretion and viability of βTC3 cells. Ann. Biomed. Eng.28:102109, 2000.
Lange's Handbook of Chemistry, Rev. 10th ed., edited by N. A. Lange. New York: McGrawHill, 1967.
Lewis, R. S., and W. M. Deen. Kinetics of the reaction of nitric oxide with oxygen in aqueous solutions. Chem. Res. Toxicol.7:568574, 1994.
Lewis, R. S., W. M. Deen, S. R. Tannenbaum, and J. S. Wishnok. Membrane mass spectrometer inlet for quantitation of nitric oxide. Biol. Mass Spectrom.22:4552, 1993.
Lewis, R. S., S. Tamir, and W. M. Deen. Kinetic analysis of the fate of nitric oxide synthesized by macrophages. J. Biol. Chem.270:2935029355, 1995.
Licht, W. R., S. R. Tannenbaum, and W. M. Deen. Use of ascorbic acid to inhibit nitrosation: Kinetic and mass transfer considerations for an system. Carcinogenesis9:365372, 1988.
Liu, X., M. J. S. Miller, M. S. Joshi, D. D. Thomas, and J. R. Lancaster. Accelerated reaction of nitric oxide with O2 within the hydrophobic interior of biological membranes. Proc. Natl. Acad. Sci. U.S.A.95:21752179, 1998.
Mertes, S., and A. Wahner. Uptake of nitrogen dioxides and nitrous acid on aqueous surfaces. J. Phys. Chem.99:1400014006, 1995.
Moncada, S., R. M. J. Palmer, and E. A. Higgs. Nitric oxide: Physiology, pathophysiology and pharmacology. Pharmacol. Rev.43:109142, 1991.
Nottingham, W., and J. R. Sutter. Kinetics of the oxidation of nitric oxide by chlorine and oxygen in nonaqueous media. Int. J. Chem. Kinet.18:12891302, 1986.
Patel, R. P., and V. M. DarleyUsmar. Using peroxynitrite as oxidant with lowdensity lipoprotein. Methods Enzymol.269:375384, 1996.
Perry's Chemical Engineer's Handbook, 6th ed., edited by Perry, R. H. and D. W. Green. New York: McGrawHill, 1984, p. 3252.
Pfeiffer, S., A. Lass, K. Schmidt, and B. Mayer. Protein tyrosine nitration in mouse peritoneal macrophages activated and: Evidence against an essential role of peroxynitrite. FASEB J.15:23552364, 2001.
Press, W. H., S. A. Teukolsky, W. T. Vetterling, and B. P. Flannery. Numerical Recipes in FORTRAN: The Art of Scientific Computing, 2nd ed. Cambridge: Cambridge University Press, 1992, pp. 704–707, 749–752.
Ramamurthi, A., and R. S. Lewis. Measurement and modeling of nitric oxide release rates for nitric oxide donors. Chem. Res. Toxicol.10:408413, 1997.
Ramamurthi, A., and R. S. Lewis. Design of a novel apparatus to study nitric oxide (NO) inhibition of platelet adhesion. Ann. Biomed. Eng.26:10361043, 1998.
Ramamurthi, A., and R. S. Lewis. Influence of agonist, shear rate, and perfusion time on nitric oxide inhibition of platelet deposition. Ann. Biomed. Eng.28:174181, 2000.
Robb, W. L.Thin silicone membranes—Their permeation properties and some applications. Ann. N.Y. Acad. Sci.46:119137, 1968.
Schmidt, K., and B. Mayer. Determination of NO with a Clarktype electrode. In: Nitric Oxide Protocols, edited by M. A. Titheradge. Totowa, NJ: Humana, 1998, pp. 101–109.
Schumpe, A.The estimation of gas solubility in salt solutions. Chem. Eng. Sci.48:153158, 1993.
Schwartz, S. E. Trace Atmosphere Constituents: Properties, Transformations, and Fates. New York: Wiley, 1983.
Tamir, S., R. S. Lewis, T. D. R. Walker, W. M. Deen, J. S. Wishnok, and S. T. Tannenbaum. The influence of delivery rate on the chemistry and biological effects of nitric oxide. Chem. Res. Toxicol.6:895899, 1993.
Thomas, D. D., X. Liu, S. P. Kantrow, and J. R. Lancaster. The biological life of nitric oxide: Implications for the perivascular dynamics of NO and O2.Proc. Natl. Acad. Sci. U.S.A.98:355360, 2001.
Treacy, J. C., and F. Daniels. Kinetic studies of the oxidation of nitric oxide with oxygen in the pressure range 1 to 20 Mm. J. Am. Chem. Soc.77:20332035, 1955.
Weisenberger, S., and A. Schumpe. Estimation of gas solubility in salt solutions at temperatures from 273 K to 363 K. AIChE J.42:298300, 1996.
Wilke, C. P., and P. Chang. Correlation of diffusion coefficient in dilute solutions. AIChE J.2:264270, 1955.
Wise, D. L., and G. Houghton. Diffusion coefficients of neon, krypton, xenon, carbon monooxide, and nitric oxide in water at 10–60°C. Chem. Eng. Sci.23:12111216, 1968.
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Wang, C., Deen, W.M. Nitric Oxide Delivery System for Cell Culture Studies. Annals of Biomedical Engineering 31, 65–79 (2003). https://doi.org/10.1114/1.1533072
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DOI: https://doi.org/10.1114/1.1533072