Plasma minimum

Therapeutic Concentration. In plasma, minimum inhibitory concentration 0.006 to 2 pg/ml. 

The ratio between pharmacokinetic measures, such as the plasma minimum concentration (Cmin), and the 50% inhibitory concentration (ICj ) provides a measure of systemic antiviral efficacy. Similarly, the ratio of CSF concentrations to IC, may provide a better estimate of CNS efficacy than CSF concentration alone. 

From the plasma minimum (plasma frequency, wp), one can readily calculate t the electronic relaxation time by the classical Drude equation which is well established for metal films (11)- This gives a value of 1.9 X 10" sec for (SN). . From t and wp, one can calculate the dc conductivity of a metal by the well-known equation (11) ... 

The probability for a particular electron collision process to occur is expressed in tenns of the corresponding electron-impact cross section n which is a function of the energy of the colliding electron. All inelastic electron collision processes have a minimum energy (tlireshold) below which the process cannot occur for reasons of energy conservation. In plasmas, the electrons are not mono-energetic, but have an energy or velocity distribution,/(v). In those cases, it is often convenient to define a rate coefficient /cfor each two-body collision process ... 

High power pulsed lasers are used to produce plasmas and thus to sample and excite the surfaces of soHds. Improvements in minimum detectable limits and decreases in background radiation and in interelement interference effects result from the use of two lasers (99) (see Surface and interface analysis). 

A summary of the properties of the different types of dextrans available is presented in Table 25.1. Dextrans for clinical use as plasma expanders must have moleeular weights between 40000 (= 220 glucose units) and 300000. Polymers below the minimum are excreted too rapidly fiom the kidneys, whilst those above the maximum are potentially dangerous because of retention in the body. In practice, infusions containing dextrans of average molecular weights of40000,70000 and 110000 are commonly encountered. 

In this special case when the time between dosings is equal to the half-life time of the drug, we can deduce that the minimum (steady-state) plasma concentration with repeated dosing is equal to the peak concentration, obtained from a single dose. Under this condition, the corresponding maximum (steady-state) concentration is twice as much as the minimum one. 

The apphed pretreatment techniques were digestion with a combination of acids in the pressurized or atmospheric mode, programmed dry ashing, microwave digestion and irradiation with thermal neutrons. The analytical methods of final determination, at least four different for each element, covered all modern plasma techniques, various AAS modes, voltammetry, instrumental and radiochemical neutron activation analysis and isotope dilution MS. Each participating laboratory was requested to make a minimum of five independent rephcate determinations of each element on at least two different bottles on different days. Moreover, a series of different steps was undertaken in order to ensure that no substantial systematic errors were left undetected. 

In a silane-hydrogen discharge the feedstock gases SiHa and H2 take part in all the processes that occur. A large number of reactions have been proposed (see e.g. Kushner [190]). Nienhuis et al. [191] have performed a sensitivity analysis in their self-consistent fluid model, from which a minimum set of reactions have been extracted for a typical low-pressure RF discharge. Tables II and III list these reactions. They will be used in the plasma models described in subsequent sections. The review articles on silane chemistry by Perrin et al. [192] and on hydrogen by Phelps [193] and Tawara et al. [194] have been used. The electron collision data are compiled in Figure 13 [189]. 

Opioids maybe administered in a variety of routes including oral (tablet and liquid), sublingual, rectal, transdermal, transmucosal, intravenous, subcutaneous, and intraspinal. While the oral and transdermal routes are most common, the method of administration is based on patient needs (severity of pain) and characteristics (swallowing difficulty and preference). Oral opioids have an onset of effect of 45 minutes, so intravenous or subcutaneous administration maybe preferred if more rapid relief is desired. Intramuscular injections are not recommended because of pain at the injection site and wide fluctuations in drug absorption and peak plasma concentrations achieved. More invasive routes of administration such as PCA and intraspinal (epidural and intrathecal) are primarily used postoperatively, but may also be used in refractory chronic pain situations. PCA delivers a self-administered dose via an infusion pump with a preprogrammed dose, minimum dosing interval, and maximum hourly dose. Morphine, fentanyl, and hydromorphone are commonly administered via PCA pumps by the intravenous route, but less frequently by the subcutaneous or epidural route. 

While most preliminary SFC-plasma coupled techniques employed microwave-induced plasmas (MIPs), the use of ICP-MS is now increasing [469]. An advantage of microcolumn SFC-ICP hyphenation is the significantly reduced flow-rates of microcolumns compared with those of conventional columns. Both pSFC-ICP-AES [470,471] and cSFC-ICP-AES [472] were described. In the case of elemental detector selectivity (e.g. AES) complete chromatographic resolution is not required. The detector possesses linearity over several orders of concentrative magnitude. Minimum detectable quantities for nonmetals range from sub to low ng mL"1. 

Figure 14 shows that the plasma concentrations do not continue to build forever but reach a plateau where the same maximum (Cmax) and minimum (Cm n) con-... 

Cmin,ss Minimum plasma concentration at steady state fu Fraction unbound in plasma... 

It is possible to predict the steady-state minimum plasma concentration (Fig. 6.4) using the equation ... 

Cmin.ss is the minimum plasma concentration at steady state fa is the fraction absorbed in man ... 

Estimation of the potency can be made in a several ways and will be highly dependent on the nature of the target. If a purified system is used it is normal to correct for the effect of plasma protein binding (which can be measured directly in human plasma) as it is usual for the effect to be proportional to the unbound concentration [82]. This can be used to set a value for the minimum plasma concentration at steady state. 

The plasma concentration will continue to rise until it reaches a plateau, or steady state. At this time, the plasma concentration will fluctuate between a maximum (Cmav) and a minimum (CrnLn) level, but, more important, the amount of drug eliminated per dose interval will equal the amount of drug absorbed per dose. When a drug is given at a dosing interval that is equal to its elimination half-life, it will reach 50% of its steady-state plasma concentration after one half-life, 75% after two half-lives, 87.5% after three, 93.75% after four, and 96.87% after five. Thus, from a practical viewpoint,... 

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