1. Two normal subjects and ten patients with chronic renal failure were given 15 or 20 g of calcium carbonate in the morning and 5·6 or 8·4 g of calcium phosphate in the evening for 13-41 days.2. During the high calcium and phosphate intake there was a rise in calcium and phosphate absorption from the gut in the normal subjects and to about the same extent in the patients with chronic renal failure.3. The calcium and phosphate balances became positive while there was a rise in plasma calcium and a fall in plasma phosphate. There was also a fall in urinary phosphate excretion.
Liposomes (phospholipid vesicles) have been proposed as carriers of materials of therapeutic interest, and work in this area has been reviewed (Tyrrell et al., 1976). The possibility of utilizing such a system in tumour therapy has received some attention, and Gregoriadis et al. (1974) injected patients with liposomes using entrapped l 3 I Ilabelled albumin as a marker. Tissue distribution was measured post mortem, several days after administration. As a more versatile alternative we have been investigating the use of the yemitter 9 9 m T~ (technetium) to study liposome distribution in experimental animals. This isotope has been found ideal for radioisotope imaging. Technetium, as the pertechnetate ion (99mT~04-), has previously been used as a vesicle marker to follow the short-term fate of liposomes in mice (McDougall et al., 1975), erythrocyte 'ghosts' in rats (Tyrrell & Ryman, 1976) and to follow liposome uptake by cells in tissue culture (Dunnick et al., 1976).We have prepared liposomes from combinations of the following purified lipids; phosphatidylcholine (egg lecithin), cholesterol, dicetyl phosphate and stearylamine.Rotary-evaporated lipid films were shaken with sterile 0.9 % NaCl to give a final suspension of 20% (w/v). These were surrounded by an ice bath and sonicated with a titanium probe( 1 .Ocm diameter)for20 bursts (6,um peak-to-peak) of ~O S , with 30 scoolingbetween. Technetium label was attached to these pre-formed liposomes by an SnCI, method. To the liposomes (600mg in 3.0ml) was added 0.5ml of a sterile neutral solution of 3m-SnClz previously prepared in 02-free water and stored under Nz at 4°C. The mixture was shaken well and not more than 2.5ml of sodium pertechnetate solution in 0.9% NaCl was added to the suspension, drop by drop, with vigorous shaking, and left at room temperature for 15-30min before injection. The presence of free pertechnetate was estimated by dialysis and found to be less than 2%.The possibility that a labelled SnCI, colloid was formed in the preparation of liposome batches was explored. A preparation with NaCI, SnCI, and pertechnetate formed a labelled colloid under the conditions of the labelling used for the liposomes, and this label could be removed by centrifugation at 4000rev./min for 5min in an MSE Super Minor bench centrifuge. Liposomes labelled under the same conditions remained in the supernatant. The contamination of technetium-labelled liposomes with free pertechnetate and colloid was therefore minimal.Liposomes (20mg of lipid) labelled with 1 mCi of 99mTc were injected into the tail vein of normal Wistar rats. Tissue distribution and clearance of the label from the blood was studied at various times by killing the animals and counting individual organs for radioactivity. Immediately before killing, a picture of the distribution of radioactivity in the whole animal was obtained by a y-camera-computer system (scintiscan). This provided a photographic image and a quantitative radioactivity distribution map for each rat.For the tumour studies, Wistar rats we...
Thirty-four patients (24 females and 10 males) selected from 300 consecutive patients with established systemic sclerosis (SSc), with a current or past history of articular symptoms, were clinically documented and further studied using thermography and bone scan to define the pattern of arthritis. Clinical evidence of synovitis was observed in 30 (88%) and joint inflammation was detected in 31 (91%) by the above-mentioned imaging techniques. A distinctive subset of 10 patients with deforming arthritis was characterized in which seven (70%) patients fulfilled criteria for both rheumatoid arthritis and SSC; three of these satisfied the criteria for diagnosis of CREST, but none met the criteria of mixed connective tissue disease. These patients, as a group, when compared with the rest showed limited skin involvement (skin score of 19 +/- 11 vs 33 +/- 14; P < 0.05) and were positive for rheumatoid factor (80 vs 13%; P < 0.05) and anticentromere antibodies (37 vs 4%; P < 0.05).
Diaschisis does not independently add to the clinical deficit after stroke. It is more likely that it simply represents part of the damage done by the stroke.
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