Insert Preparation

The most common substrate is steel, for which a number of preparative routes are in common use. Each route has its merits. A degreaser stage is a common precursor to all the methods, followed by either grit blasting or a chemical conversion coating. The degreaser used prior to grit blast may use either solvent or aqueous systems. 

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Chetoni, P., Di-Colo, G., Grandi, M., Morelli, M., Saettone, M.F., and Darougar, S., Silicone rubber/hydrogel composite ophthalmic inserts preparation and preliminary in vitro/in vivo evaluation, Eur. J. Pharm. Biopharm., 46 125-132 (1998). 

Saettone, M. F.,Torracca, M. T., Pagano, A., Giannaccini, B., Rodriguez, L., and Cini, M. (1992), Controlled release of pilocarpine from coated polymeric ophthalmic inserts prepared by extrusion, Ini. J. Pharm., 86(2-3), 159-166. 

Fig 3. Effect of template purity on the yield from an ECL random prime reaction. Total amounts of DNA present (labeled DNA plus template) following labeling reactions for 1 h at 37°C with various quantities of template. S jL of N-ras proto-oncogene insert prepared in low-melting-point agarose were used in the test reactions. 

The inserts prepared from polymer solutions had DSC traces very similar to those of the corresponding parent homopolymers, as far as both temperature and enthalpy changes are concerned. This implies that no DSC-appreciable physico-chemical modifications occur during the preparation of the films. 

Fig. 4. DSC curves of inserts prepared with poly(vinyl alcohol) PVA-C. Key a) polymer film b) pilocarpine nitrate c) polymer insert containing pilocarpine nitrate d) pilocarpine PAA-salt e,f) polymer insert containing pilocarpine PAA-salt heating and cooling, respectively.

Figure A3.13.12. Evolution of the probability for a right-handed ehiral stmetnre (fiill eiirve, see ( equation (A3,13.69))) of the CH eliromophore in CHD2T (a) and CHDT2 ( ) after preparation of ehiral stnietures with multiphoton laser exeitation, as diseussed in the text (see also [154]). For eomparison, the time evolution of aeeording to a one-dimensional model ineluding only the bending mode (dashed enrve) is also shown. The left-hand side insert shows the time evolution of within the one-dimensional ealeulations for a longer time interval the right-hand insert shows the time evolution within the tln-ee-dimensional ealeulation for the same time interval (see text).

Chromatographic Separation of a Mixture of o- and p-Nitroaniline. Prepare a glass tube A (Fig. 24) in which the wider portion has a diameter of 3 cm. and a length of ca. 30 cm. the narrow portion at the base has a diameter of 5-7 mm. Wash the tube thoroughly (if necessary, with chromic acid, followed by distilled water and ethanol) and then dry. Insert a small plug of cotton-wool P as shown just within the narrow neck of the tube it is essential that this plug does not project into the wider portion of the tube. Clamp the tube in a vertical position. 

All thermometers for semi-micro preparations must have very small bulbs. They may often be inserted into flasks through a short collar of rubber tubing in place of the customary corks. 

Calls subroutines that prepare work arrays and specify positions in the global system of equations where the prescribed boundary conditions should be inserted. 

Cholestenone. Place a mixture of 1 0 g. of purified cholesterol and 0-2 g. of cupric oxide in a test-tube clamped securely at the top, add a fragment of Dry Ice in order to displace the air by carbon dioxide, and insert a plug of cotton wool in the mouth of the tube. Heat in a metal bath at 300-315° for 15 minutes and allow to cool rotate the test-tube occasionally in order to spread the melt on the sides. Warm with a few ml. of benzene and pour the black suspension directly into the top of a previously prepared chromatographic column (1) rinse the test-tube with a little more benzene and pour the rinsings into the column. With the aid of shght suction (> 3-4 cm. of mercury), draw the solution into the alumina column stir the top 0 -5 cm. or so with a stout copper wire to... 

Ethyl phenylethylmalonate. In a dry 500 ml. round-bottomed flask, fitted with a reflux condenser and guard tube, prepare a solution of sodium ethoxide from 7 0 g. of clean sodium and 150 ml. of super dry ethyl alcohol in the usual manner add 1 5 ml. of pure ethyl acetate (dried over anhydrous calcium sulphate) to the solution at 60° and maintain this temperature for 30 minutes. Meanwhile equip a 1 litre threenecked flask with a dropping funnel, a mercury-sealed mechanical stirrer and a double surface reflux condenser the apparatus must be perfectly dry and guard tubes should be inserted in the funnel and condenser respectively. Place a mixture of 74 g. of ethyl phenylmalonate and 60 g. of ethyl iodide in the flask. Heat the apparatus in a bath at 80° and add the sodium ethoxide solution, with stirring, at such a rate that a drop of the reaction mixture when mixed with a drop of phenolphthalein indieator is never more than faintly pink. The addition occupies 2-2 -5 hoius continue the stirring for a fiuther 1 hour at 80°. Allow the flask to cool, equip it for distillation under reduced pressure (water pump) and distil off the alcohol. Add 100 ml. of water to the residue in the flask and extract the ester with three 100 ml. portions of benzene. Dry the combined extracts with anhydrous magnesium sulphate, distil off the benzene at atmospheric pressure and the residue under diminished pressure. C ollect the ethyl phenylethylmalonate at 159-160°/8 mm. The yield is 72 g. 

It is regretted that the size of the volume has rendered the insertion of literature references impossible the Selected Bibliography (A,5) may partly compensate for this omission. Section numbers are now included in the headings of the pages—a feature introduced in response to requests by many readers. The volume comprises virtually at least three books under one cover, viz., experimental technique, preparations, and qualitative organic analysis. It should therefore continue to be of value as a one volume reference work in the laboratory. Students at all levels will find their requirements for laboratory work (excluding quantitative organic analysis) adequately provided for and, furthermore, the writer hopes that the book will be used as a source of information to supplement their theoretical studies. 

The silyl enol ethers 209 and 212 are considered to be sources of carbanions. and their transmetallation with Pd(OAc)2 forms the Pd enolate 210. or o.w-tt-allylpalladium, which undergoes the intramolecular alkene insertion and. 1-elimination to give 3-methylcyclopentenone (211) and a bicyclic system 213[199], Five- and six-membered rings can be prepared by this reaction[200]. Use of benzoquinone makes the reaction catalytic. The reaction has been used for syntheses of skeletons of natural products, such as the phyllocladine intermediate 214[201], capnellene[202], the stemodin intermediate 215[203] and hir-sutene [204]. 

The intramolecular oxidative earbonylation has wide synthetie applieation. The 7-lactone 247 is prepared by intramolecular oxycarbonylation of the alke-nediol 244 with a stoichiometric amount of Pd(OAc)2 under atmospheric pres-sure[223]. The intermediate 245 is formed by oxypalladation, and subsequent CO insertion gives the acylpalladium 246. The oxycarbonylation of alkenols and alkanediols can be carried out with a catalytic amount of PdCl2 and a stoichiometric amount of CuCb, and has been applied to the synthesis of frenolicin(224] and frendicin B (249) from 248[225]. The carbonylation of the 4-penten-l,3-diol 250, catalyzed by PdCl2 and CuCl2, afforded in the c -3-hydroxytetrahydrofuran-2-aeetie acid lactone 251[226J. The cyclic acetal 253 is prepared from the dienone 252 in the presence of trimethyl orthoformate as an accepter of water formed by the oxidative reaction[227]. 

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