A study on the protein concentration dependence of the thermodynamics of micellization

An investigation on the dependence of the thermodynamics of micellization of different surfactants such as sodium dodecyl sulfate (SDS), sodium octanoate (C8HONa), and sodium perfluorooctanoate (C8FONa) on the concentration of human serum albumin (HSA) has been realized. The critical micelle concentration (cmc) and ionisation degree of micellization, β, as a function of temperature (T), in solutions containing 0.125% and 0.250% in v/w of HSA, were estimated from conductivity data. From these results, the average number of surfactant monomers per protein molecule was calculated: higher values were found for C8HONa, the lowest value corresponded to SDS. For all the systems under study, electrostatic forces mainly drive the interaction between the surfactants and the proteins. Plots of cmc against temperature appear to follow the typical U-shaped curve with a minimum T_min. Thermodynamic functions of micellization were obtained by applying the theoretical models that best fit our experimental data, showing that the addition of HSA shows different patterns depending on the surfactant and thermodynamic quantity. Changes in the protein conformation due to the adsorption of surfactant molecules have been monitored by using UV-CD spectra. Greater changes in α-helical contents correspond with the concentrations over cmc, indicating that at low concentrations surfactants act as a structure stabilizer; meanwhile they act as a destabilizer at higher concentrations. C8HONa is the most effective reducing α-helical content, SDS is the less effective content.     

A comparative study of the physicochemical properties of perfluorinated and hydrogenated amphiphiles

In this work we studied and compared the physicochemical properties of perfluorinated (sodium perfluoroheptanoate, C7FONa, and perfluorooctanoate, C8FONa) and hydrogenated (sodium octanoate, C8HONa, decanoate, C10HONa, and dodecanoate, C12HONa) amphiphiles. First, we determined their Krafft points to study the solubility and appropriate temperature range of micellization of these compounds. The critical micelle concentration (cmc) and ionization degree of micellization (beta) as a function of temperature (T) were estimated from conductivity data. Plots of cmc vs T appear to follow the typical U-shaped curve with a minimum T(min). The results show that the surfactants with CF2/CH2 ratio of 1.5 between alkyl chains (C12HONa-C8FONa and C10HONa-C7FONa) have nearly the same minimum value for cmc against temperature. The comparison between the cmc of hydrogenated amphiphiles and the corresponding perfluorinated amphiphiles must be done at this point. Thermodynamic functions of micellization were obtained by applying different theoretical models and choosing the one that best fit our experimental data. Although perfluorinated and hydrogenated amphiphiles present similar thermodynamic behavior, we have found a variation of 1.3 to 1.7 in the CF2/CH2 ratio, which did not remain constant with temperature. In the second part of this study the apparent molar volumes and adiabatic compressibilities were determined from density and ultrasound velocity measurements. Apparent molar volumes at infinite dilution presented the ratio 1.5 between alkyl chains again. However, apparent molar volumes upon micellization for sodium perfluoroheptanoate indicated a different aggregation pattern.     

Regarding the effect that different hydrocarbon/fluorocarbon surfactant mixtures have on their complexation with HSA

The complexations between human serum albumin (HSA) and the sodium perfluorooctanoate/sodium octanoate and sodium perfluorooctanoate/sodium dodecanoate systems have been studied by a combination of electrical conductivity, ion-selective electrode, electrophoresis, and spectroscopy measurements. The binary mixtures of the surfactants deviated slightly from ideality. Binding plots revealed the existence of two specific binding sites, the first site being more accessible than the second. Positive cooperative binding has been found, thus revealing the importance of the hydrophobic interactions in both kinds of surfactants. The Gibbs energies of binding per mole of surfactant (DeltaG(nu)) were calculated from the Wyman binding potential where, on the basis of the elevated number of binding sites, a statistical contribution has been included. Initially these energies are large and negative, gradually decreasing as saturation is approached. Changes in the slope of Gibbs energies have been identified with the saturation of the first binding set. These facts denote that the surfactants under study have different favorite adsorption sites along the protein and that the adsorption process of perfluorooctanoate is more closely followed by dodecanoate than by octanoate. Finally, electrophoresis and spectroscopy measurements suggest induced conformational changes on HSA depending on the surfactant mixture as well as the mixed ratio.     

Effect of cationic surfactants on the interaction between sodium perfluorooctanoate and beta-lactoglobulin

The interaction between the fluorocarbon surfactant, sodium perfluorooctanoate (SPFO), and beta-lactoglobulin (BLG) was studied. In particular, the effects of cationic surfactants, such as alkyltriethylammonium bromide (C(n)NE, n=8, 10, 12), on SPFO-BLG interaction were examined. It was shown that the anionic fluorocarbon surfactant, SPFO, was a strong denaturant of BLG. The ability of SPFO to denature BLG could be weakened by the addition of C(n)NE. The effect of C(n)NE on SPFO-BLG interaction was related to the hydrocarbon chain length of C(n)NE, and also the molar ratio of the added C(n)NE to the SPFO in SPFO-BLG solutions ([C(n)NE]/[SPFO]). Our findings might provide a way to design surfactant systems that are less denaturing to proteins or tailor the ability of surfactant to denature proteins through the appropriate mixing with other surfactants.     

Conformational changes in human serum albumin induced by sodium perfluorooctanoate in aqueous solutions

Conformational changes in the bulk solution and at the air-aqueous interface of human serum albumin (HSA) induced by changes in concentration of sodium perfluorooctanoate (C(7)F(15)COO(-)Na(+)) were studied by difference spectroscopy, zeta-potential data, and axisymmetric drop shape analysis. zeta-potential was used to monitor the formation of the HSA-C(7)F(15)COO(-)Na(+) complex and the surface charge of the complex. The conformational transition of HSA in the bulk solution was followed as a function of denaturant concentration by absorbance measurements at 280 nm. The data were analyzed to obtain values for the Gibbs energies of the transition in water (DeltaG(0)(W)) and in a hydrophobic environment (DeltaG(0)(hc)) pertaining to saturated protein-surfactant complexes. The conformational changes that surfactants induce in HSA molecules alter its absorption behavior at the air-water interface. Dynamic surface measurements were used to evaluate this behavior. At low [C(7)F(15)COO(-)Na(+)], proteins present three adsorption regimes: induction time, monolayer saturation, and interfacial gelation. When surfactant concentration increases and conformational changes in the bulk solution occur, the adsorption regimes disappear. HSA molecules in an intermediate conformational state migrate to the air-water interface and form a unique monolayer. At high [C(7)F(15)COO(-)Na(+)], the adsorption of denatured molecules exhibits a behavior analogous to that of dilute solutions.     

Phase behavior and molecular thermodynamics of coacervation in oppositely charged polyelectrolyte/surfactant systems: a cationic polymer JR 400 and anionic surfactant SDS mixture

Coacervation in mixtures of polyelectrolytes and surfactants with opposite charge is common in nature and is also technologically important to consumer health care products. To understand the complexation behavior of these systems better, we combine multiple experimental techniques to systematically study the polymer/surfactant binding interactions and the phase behavior of anionic sodium dodecyl sulfate (SDS) surfactant in cationic JR 400 polymer aqueous solutions. The phase-behavior study resolves a discrepancy in the literature by identifying a metastable phase between the differing redissolution phase boundaries reported in the literature for the surfactant-rich regime. Isothermal titration calorimetry analyzed within the framework of the simple Satake-Yang model identifies binding parameters for the surfactant-lean phase, whereas a calculation for polymer-bound micelles coexisting with free micelles is analyzed in the surfactant-rich redissolution regime. This analysis provides a preliminary understanding of the interactions governing the observed phase behavior. The resulting thermodynamic properties, including binding constants and the molar Gibbs free energies, enthalpies, and entropies, identify the relative importance of both hydrophobic and electrostatic interactions and provide a first approximation for the corresponding microstructures in the different phases. Our study also addresses the stability and metastability of oppositely charged polyelectrolytes and surfactant mixtures.     

Formation and structural heat-stability of β-lactoglobulin/surfactant complexes

The binding of two model surfactants, sodium dodecyl sulfate and dodecyltrimethylammonium bromide to β-lactoglobulin was studied at room temperature and the thermal stability of the resulting complexes was evaluated by differential scanning calorimetry (DSC) measurements. Binding isotherms indicated both ionic and hydrophobic interactions depending on both the charge of the protein and surfactant at different pHs and on the binding molar ratios of surfactant to the globular protein. Zeta potential measurements indicated charge neutralisation of the protein, under suitable conditions, which also lead to aggregation and precipitation of the proteins. Surface tension measurements indicated similarity between the two types of oppositely charged protein-surfactant complexes and a difference between them when protein and surfactants are similarly charged. DSC measurements revealed different behavior in protein conformation in the presence of the two surfactants. The results obtained at room temperature and upon heating are discussed in terms of the nature of the surfactant/protein interactions involved in the complex formation.     

Protein-surfactant interaction: differences between fluorinated and hydrogenated surfactants

The interactions of proteins with fluorinated/hydrogenated surfactants were investigated by circular dichroism and turbidity measurement. Pairs of fluorinated and hydrogenated surfactants with similar critical micelle concentrations (cmc), including sodium perfluorooctanoate/sodium decylsulfate and lithium perfluorononanoate/sodium dodecylsulfate were compared in view of their interactions with proteins including BSA, lysozyme, β-lactoglobulin and ubiquitin. It was found that fluorinated surfactants exhibited stronger interactions with proteins than hydrogenated ones, which, however, depended on the structures of both proteins and surfactant molecules. If the proteins are very stable, or the surfactant–protein interactions are very strong, such differences between the two kinds of surfactants might be indistinguishable.     

Thermodynamic study of the thermal denaturation of a globular protein in the presence of different ligands

By means of difference UV-Vis spectra, the thermal denaturation of catalase has been studied in the presence of different surfactants: sodium perfluorooctanoate, sodium octanoate and sodium dodecanoate. These results indicate that hydrogenated surfactants play two opposite roles in the folding and stability of catalase, they act as a structure stabiliser at a low molar concentrations (enhancing T _m) and as a destabilizer at a higher concentrations (diminishing T _m). Meanwhile sodium perfluorooctanoate enhances T _m in the whole concentration range. An approach for the determination of the heat capacity, enthalpy and entropy has been made, finding that for the three studied surfactants, at all concentrations, the enthalpy term dominates the entropy term.     

Different thermal unfolding pathways of catalase in the presence of cationic surfactants

In this paper we have corroborated the usefulness of spectroscopic techniques, such as UV-visible, in the study and thermodynamic characterization of the thermal unfolding of catalase as a function of the concentration and alkyl chain length of n-alkyltrimethylammonium bromides (CnTAB, n = 8, 10, and 12). For this reason, a thermodynamic model was used which included experimental data corresponding to the pre- and posttransition into the observable transition. It has been found that n-alkyltrimethylammonium bromides play two opposite roles in the folding and stability of catalase. They act as a structure stabilizer at a low molar concentration and as a destabilizer at a higher concentration. The maximum of the unfolding temperature has been found to decrease with the alkyl chain. The reason for this difference has been suggested to be the side chains involved. In the presence of C8TAB and C10TAB, Gibbs energies of unfolding (DeltaG(T)) decrease with concentration, whereas for C12TAB an increase has been observed. These findings can be explained by the fact that when differences in the hydrophobic nature of the surfactants exist, different pathways of unfolding may occur. Also, the presence of surfactants has been observed to affect the cold denaturation of catalase. Thermodynamic results suggest that the thermal denaturation of catalase in the presence of n-alkyltrimethylammonium bromides is a perfect transition between two states.     

NMR studies on selectivity of beta-cyclodextrin to fluorinated/hydrogenated surfactant mixtures

The interactions between beta-cyclodextrin (beta-CD) and the equimolar/nonequimolar mixtures of sodium perfluorooctanoate (C(7)F(15)COONa, SPFO) and sodium alkyl sulfate (C(n)H(2n+1)SO(4)Na, C(n)SO(4), n = 8, 10, 12) were investigated by 1H and 19F NMR. It showed that beta-CD preferentially included the fluorinated surfactant when exposed to mixtures of hydrogenated (C(n)SO(4)) and fluorinated (SPFO) surfactants, notwithstanding whether the hydrogenated surfactant C(n)SO(4) was more or less hydrophobic than the SPFO. Such preferential inclusion of the fluorinated surfactant continued to a certain concentration of beta-CD at which time the C(n)SO(4) was then observed to be included. The longer the hydrocarbon chain of C(n)SO(4) the lower the concentration of beta-CD at which the hydrogenated surfactants began to show inclusion. The inclusion process can be qualitatively divided into three stages: first, formation of 1:1 beta-CD/SPFO complexes; second, formation of 1:1 beta-CD/C(n)SO(4) complexes; and finally, formation of 2:1 beta-CD/SPFO complexes upon further increase of beta-CD concentration. In the concentration range studied, during the last stage of inclusion both 2:1 beta-CD/C(12)SO(4) and 2:1 beta-CD/SPFO complexes appear to be simultaneously formed in the system of beta-CD/SPFO/C(12)SO(4) but not in either the systems of beta-CD/SPFO/C(8)SO(4) or beta-CD/SPFO/C(10)SO(4). The selective inclusion of the shorter fluorocarbon chain surfactant might be attributed to the greater rigidity and size of the fluorocarbon chains, compared to those of the hydrocarbon chains, which provide for a tighter fit and better interaction between the host and guest. This latter effect appears to dominate the increase in hydrophobic character as the carbon chain length increases in the hydrogenated series.     

Polymers as Hydrophobic Adsorbent Surface for Some Surfactants

Polyvinyl alcohol (PVA) and polyacrilic acid (PAA) were used as hydrophobic adsorbent surfaces at 25°C for two nonionic surfactants, namely, tetradecyl polyoxyethylenated monolaurate [La(EO)₁₄] and tetradecyl polyoxyethylenated monooleate [Ol(EO)₁₄], and two anionic surfactants, namely, sodium oleic sulfonate [OlSO₃Na] and sodium dodecyl benzene sulfonate [SDBS]. Surface tension measurements were performed to determine the critical micelle concentration (CMC) and the adsorption isotherms of the tested surfactants. All the tested surfactants display L-shape isotherms except that of OlSO₃Na onto PVA. No adsorption behavior has been shown for the anionic SDBS onto both PVA and PAA. The adsorption data show higher adsorption affinity for all the tested nonionic surfactants onto PAA than onto PVA while the investigated anionic surfactant OlSO₃Na possesses close values of Γ_max. The study reveals that the nature of the polymer surface as adsorbent besides the molecular structure of the surfactant defined the types and mechanisms of adsorption.     

Spectrophotometric study of interaction and solubilization of procaine hydrochloride in micellar systems

The interaction of Procaine hydrochloride (PC) with cationic, anionic and non-ionic surfactants; cetyltrimethylammonium bromide (CTAB), sodium dodecyl sulfate (SDS) and triton X-100, were investigated. The effect of ionic and non-ionic micelles on solubilization of Procaine in aqueous micellar solution of SDS, CTAB and triton X-100 were studied at pH 6.8 and 29°C using absorption spectrophotometry. By using pseudo-phase model, the partition coefficient between the bulk water and micelles, K_x, was calculated. The results showed that the micelles of CTAB enhanced the solubility of Procaine higher than SDS micelles (K_x = 96 and 166 for SDS and CTAB micelles, respectively) but triton X-100 did not enhanced the solubility of drug because of weak interaction with Procaine. From the resulting binding constant for Procaine-ionic surfactants interactions (K_b = 175 and 128 for SDS and CTAB surfactants, respectively), it was concluded that both electrostatic and hydrophobic interactions affect the interaction of surfactants with cationic procaine. Electrostatic interactions have a great role in the binding and consequently distribution of Procaine in micelle/water phases. These interactions for anionic surfactant (SDS) are higher than for cationic surfactant (CTAB). Gibbs free energy of binding and distribution of procaine between the bulk water and studied surfactant micelles were calculated.      

Hemiesters and hemiamides of maleic and succinic acid: synthesis and application of surfactants in emulsion polymerization with styrene and butyl acrylate

Hemiesters and hemiamides of maleic acid with different chain lengths of the hydrophobic alkyl group (R = C₈H₁₇, C₁₀H₂₁, C₁₂H₂₅, C₁₆H₃₃) have been synthesized and used as surfactants in the emulsion polymerization of styrene and butyl acrylate. The same polymerization experiments were also carried out using nonreactive surfactants with an analogous succinic structure. The chemical structure of the surfactants was confirmed by 1H nuclear magnetic resonance. The melting point and critical micelle concentration of the reactive surfactants described herein were measured. All of the surfactants studied provided good stability of styrene/butyl acrylate latexes, when compared with a reference latex of a styrene/butyl acrylate copolymer prepared with a surfactant sodium dodecyl sulfate. The amount of surfactant grafted onto the particles of the final latex was estimated by conductimetric titration. Between 33 and 68% of surfactant used in emulsion polymerization was found on the surface of latex particles. Electrolyte addition at high concentration and freeze/thaw cycle cause flocculation of latexes. Copyright © 1999 John Wiley & Sons, Ltd.     

Study on Binding Properties of Poorly Soluble Drug Trimethoprim in Anionic Micellar Solutions

Binding and distribution properties of trimethoprim (TMP) in the presence of various anionic surfactants; sodium octyl sulfate (C₈SO₄Na), sodium decyl sulfate (C₁₀SO₄Na), sodium lauryl sulfate (C₁₂SO₄Na), and sodium tetradecyl sulfate (C₁₄SO₄Na) has been studied by conductivity, spectrophotometry and surface tension measurements. The surface properties of anionic surfactants, that is, maximum surface excess concentration (Γ _max ) and minimum area per surfactant molecule (A _min ) at the air/water interface have been evaluated in the absence and presence of TMP using Gibbs adsorption isotherm. From conductivity data the ionization degree and counterion binding parameter have been obtained. Spectrophotometric experiments were used to determine binding constants of TMP to anionic micelles. With the increasing alkyl chain of surfactants, the interaction becomes stronger, which shows the importance of hydrophobic forces and incorporation of TMP molecules to the pure micelles of anionic surfactants increased. The results obtained from the surface tension and conductometric studies have been correlated with those obtained from the spectroscopic studies and binding tendency of TMP to anionic micelles followed the order as: C₁₄SO₄Na > C₁₂SO₄Na > C₁₀SO₄Na > C₈SO₄Na. From these results, the study of the interaction TMP in different anionic micellar solutions provided information about the characteristics of binding properties of poorly soluble drugs.     

Calorimetric determination of surfactant/polyelectrolyte binding isotherms

Mixing of oppositely charged surfactants and polyelectrolytes in aqueous solutions leads to cooperative surfactant adsorption onto the polyelectrolyte chains. Experimental determination of surfactant/polyelectrolyte binding isotherms is usually done using custom-built surfactant-ion-specific electrodes. As an alternative, we present an indirect isotherm approximation method that uses conventional isothermal titration calorimetry (ITC). The calorimetric data is fitted to the two-binding-state Satake-Yang adsorption model, which quantifies the extent of binding in terms of the binding constant (Ku) and the cooperativity parameter (u). This approach is investigated using two surfactant/polyelectrolyte mixtures: sodium perfluorooctanoate (FC7) and N,N,N-trimethylammonium derivatized hydroxyethyl cellulose (UCARE Polymer JR-400), whose binding behavior follows the Satake-Yang model, and dodecyltrimethylammonium bromide (DTAB) and poly(styrenesulfonate) (NaPSS), whose behavior deviates dramatically from the Satake-Yang model. These studies demonstrate that, in order to apply the indirect ITC method of binding isotherm determination, the surfactant/polyelectrolyte adsorption process must have no more than two dominant binding states. Thus, the technique works well for the FC7/JR-400 mixture. It fails in the case of the DTAB/NaPSS adsorption, but its mode of failure offers insight into the multiple-binding-state adsorption mechanism.     

Mixed adsorption of fluorinated and hydrogenated surfactants

The adsorption isotherms of sodium perfluorooctanoate and sodium decyl sulfate and their 1:1 mixture on gamma-alumina are recorded by depletion-type experiments with (1)H and (19)F NMR spectroscopy as the detection tool. The isotherms of the different surfactant species, obtained with and without added salt, closely resemble each other. Salt addition changes the isotherms from stepwise to the familiar S-shaped. After having reached saturation, a further increase of surfactant concentration in the mixed system leads to decyl sulfate desorption and increased perfluorooctanoate adsorption. The (19)F chemical shift of adsorbed perfluorooctanoate suggests that, for saturated surfaces, the two sorts of adsorbed surfactants form molecularly mixed surface aggregates.     

Microstructure of un-neutralized hydrophobically modified alkali-soluble emulsion latex in different surfactant solutions

At low pH conditions and in the presence of anionic, cationic, and nonionic surfactants, hydrophobically modified alkali-soluble emulsions (HASE) exhibit pronounced interaction that results in the solubilization of the latex. The interaction between HASE latex and surfactant was studied using various techniques, such as light transmittance, isothermal titration calorimetry, laser light scattering, and electrophoresis. For anionic surfactant, noncooperative hydrophobic binding dominates the interaction at concentrations lower than the critical aggregation concentration (CAC) (C < CAC). However, cooperative hydrophobic binding controls the formation of mixed micelles at high surfactant concentrations (C > or = CAC), where the cloudy solution becomes clear. For cross-linked HASE latex, anionic surfactant binds only noncooperatively to the latex and causes it to swell. For cationic surfactant, electrostatic interaction occurs at very low surfactant concentrations, resulting in phase separation. With further increase in surfactant concentration, noncooperative hydrophobic and cooperative hydrophobic interactions dominate the binding at low and high surfactant concentrations, respectively. For anionic and cationic surfactant systems, the CAC is lower than the critical micelle concentration (CMC) of surfactants in water. In addition, counterion condensation plays an important role during the binding interaction between HASE latex and ionic surfactants. In the case of nonionic surfactants, free surfactant micelles are formed in solution due to their relatively low CMC values, and HASE latexes are directly solubilized into the micellar core of nonionic surfactants.     

Synthesis and micellar properties of surface-active ionic liquids: 1-alkyl-3-methylimidazolium chlorides

A series of surface-active ionic liquids, RMeImCl, has been synthesized by the reaction of purified 1-methylimidazole and 1-chloroalkanes, RCl, R=C(10),C(12),C(14), and C(16), respectively. Adsorption and aggregation of these surfactants in water have been studied by surface tension measurement. Additionally, solution conductivity, electromotive force, fluorescence quenching of micelle-solubilized pyrene, and static light scattering have been employed to investigate micelle formation. The following changes resulted from an increase in the length of R: an increase of micelle aggregation number; a decrease of: minimum area/surfactant molecule at solution/air interface; critical micelle concentration, and degree of counter-ion dissociation. Theoretically-calculated aggregation numbers and those based on quenching of pyrene are in good agreement. Gibbs free energies of adsorption at solution/air interface, DeltaG(ads)(0), and micelle formation in water, DeltaG(mic)(0), were calculated, and compared to those of three surfactant series, alkylpyridinium chlorides, RPyCl, alkylbenzyldimethylammonium chlorides, RBzMe(2)Cl, and benzyl(3-acylaminoethyl)dimethylammonium chlorides, R(')AEtBzMe(2)Cl, respectively. Contributions to the above-mentioned Gibbs free energies from surfactant methylene groups (in the hydrophobic tail) and the head-group were calculated. For RMeImCl, the former energy is similar to that of other cationic surfactants. The corresponding free energy contribution of the head-group to DeltaG(mic)(0) showed the following order: RPyCl approximately RBzMe(2)Cl>RMeImCl>R(')AEtBzMe(2)Cl. The head-groups of the first two surfactant series are more hydrophobic than the imidazolium ring of RMeImCl, this should favor their aggregation. Micellization of RMeImCl, however, is driven by a relatively strong hydrogen-bonding between the chloride ion and the hydrogens in the imidazolium ring, in particular the relatively acidic H2. This interaction more than compensates for the relative hydrophilic character of the diazolium ring. As indicated by the corresponding DeltaG(mic)(0), micellization of R(')AEtBzMe(2)Cl is more favorable than that of RMeImCl because the CONH group of the former surfactant series forms hydrogen bonds to both the counter-ion and the neighboring molecules in the micelle.     

The interaction between n-alkyl trimethylammonium bromides with poly(l-aspartate): a thermodynamics study

Specific conductivities of a homologous series of n-alkyl trimethylammonium bromides (C₈,C₁₀,C₁₂ and C₁₄TABs) in the presence of poly(l-aspartate) in glycine buffer at pH 3.2 and 25 ^∘C have been measured over a range of C _n TAB concentrations. From the conductivity changes, the number of surfactant molecules absorbed onto the polymer, the Gibbs free energies of adsorption and the equilibrium constants have been calculated. A statistical thermodynamics analysis was used to obtain the Gibbs free energies of adsorption. The results obtained using both methods are compared and analysed. Received: 15 December 1999 Revised form: 29 February 2000 Accepted: 3 March 2000