Use of antibiotics. Antifungals.

Cartwright, R. Y.

doi:10.1136/bmj.2.6130.108

Cited by 17 publications

(6 citation statements)

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“…This is in accordance with the findings of Velupillai and Thin (1977), who detected no significant difference between the effect of combined local and oral nystatin treatment compared with local nystatin treatment alone. The oral treatment regimen adopted in this investigation has been recommended for the treatment of patients with long-standing vaginal candidosis (Nicol, 1971;Cartwright, 1978), but it failed to eradicate faecal colonisation in a substantial proportion of our patients. It is interesting that the number of patients with positive faecal culture results in the group treated with pessary alone decreased during treatment.…”

Section: Discussionmentioning

confidence: 99%

“…Oral treatment with nystatin has been shown to reduce intestinal colonisation with C. albicans (Seelig, 1968). For this reason, such treatment is often recommended as an adjunct to vaginal treatment in patients with recurrent genital infection (Nicol, 1971;Cartwright, 1978). In fact, it has not been proved that simultaneous treatment of the intestinal tract prolongs freedom from reinfection, and it has not been established that the intestinal tract is recolonised once oral treatment is discontinued.…”

Section: Introduction Patients and Methodsmentioning

confidence: 99%

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Effect of simultaneous oral and vaginal treatment on the rate of cure and relapse in vaginal candidosis.

Milne¹,

Warnock²

1979

Sexually Transmitted Infections

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SUMMARY One hundred patients with vulvovaginal candidosis were entered in a double-blind trial to compare the effect of six days' local treatment with clotrimazole with that of the same treatment plus 10 days' oral treatment with nystatin. No significant differences were detected in the rate of cure or relapse between the treatment groups. The cure rate was lowest and the relapse rate highest in patients in whom vaginal candidosis had last been diagnosed during the preceding 12 months.

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Section: Discussionmentioning

confidence: 99%

Section: Introduction Patients and Methodsmentioning

confidence: 99%

Effect of simultaneous oral and vaginal treatment on the rate of cure and relapse in vaginal candidosis.

Milne¹,

Warnock²

1979

Sexually Transmitted Infections

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“…F1ucytosine is competitively inhibited by cytarabine (cytosine arabinoside) [Cartwright, 1978] and should therefore not be used in patients receiving the latter drug.…”

Section: F1ucytosine Drug Interactionsmentioning

confidence: 99%

“…The pharmacokinetic characteristics of these drugs are the subject of the present review. Their pharmacology and therapeutic use have been reviewed by Bennett (1974), Cartwright (1978), Hoeprich (1978), Meade (1979), Sarosi et a1. (1979), Heel et a1.…”

mentioning

confidence: 99%

Clinical Pharmacokinetics of Systemic Antifungal Drugs

Daneshmend

Warnock

1983

Clinical Pharmacokinetics

171

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The currently available drugs for the treatment of systemic fungal infections are amphotericin B. flucytosine. miconazole and ketoconazole.Amphotericin B has to be given intravenously in the treatment of deep mycoses. The dose is gradually increased following a small initial dose. though this may delay the attail/menl of therapeutic concentrations. Amphotericin B. serum concentrations are proportiol/al to dose but only up to doses of 50mg. The serum pharmacokinetics fit a 3-compartment model. while cerebrospinal fluid pharmacokinetics fit a 2-compartment model. The precise identities of these compartments have not been determined. In the serum there is a relatively rapid initial half-life of 1 to 2 days. and a slower elimination phase of 15 days. Amphotericin B penetrates poorly into other body tissues. and concentrations are usually well below those in serum. This may partly be due to its high protein binding. The routes of amphotericin B elimination in man are unknown. Amphotericin B invariably causes doserelated renal damage. but this does not markedly alter its pharmacokinetics; mannitol infusions do not reduce this nephrotoxicity. Concurrent gentamicin administration and sodium depletion may enhance amphotericin B nephrotoxicity.Flucytosine may be given orally or intravenously. It has a high (greater than 80%) oral bioavailability. but this is lower in patients with renal failure. Flucytosine absorption is delayed in renal failure and by antacids. The serum pharmacokinetics fit a I-compartment model. and the apparent volume of distribution approximates to body water. Flucytosine has low protein binding and good tissue penetration. There is minimal metabolism in man; conversion to 5-fluorouracil may be the basis of flucytosine toxicity. Since flucytosine is largely eliminated by renal excretion. serum concentrations are markedly increased in the presence of renal impairment. The renal clearance of flucytosine closely parallels creatinine clearance. and in renal failure the half-life is considerably prolonged. Toxicity can be avoided by therapeutic monitoring of serum concentrations and reducing the dose when renal functiol/ is impaired.Miconazole is poorly absorbed from the gut; therefore intravenous administration is required for treatment of systemic fungal infections. Its serum pharmacokinetics fit a 3-compartment model with a short initial half-life of less than 1 hour. an intermediate half-life of 2 hours. and a terminal half-life of 20 hours. Despite this long terminal half-life. miconazole has to be given every 8 hours. It has a high apparent volume of distribution and is highly bound to plasma proteins. Adequate penetration only occurs into certain body tissues. Pen-

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“…Η δράση τους περιορίζεται σε Gram-αρνητικά βακτήρια και φαίνεται ότι η ευαισθησία των τελευταίων σχετίζεται με το ποσό των φωσφολιπιδίων που περιέ χουν στην κυτταροπλασματική μεμβράνη τους (Brown, Wood, 1972) Η νυστατίνη και η αμφοτερικίνη Β δρουν κατά παρόμοιο μη χανισμό όπως και τα προηγούμενα φάρμακα, όμως στην περίπτωση αυτή συνδέονται με τις στερόλες της κυτταροπλασματικής μεμ βράνης διαταράσσοντας την διαπερατότητα της τελευταίας. Αυτές οι στερόλες ανευρίσκονται μόνο στην κυτταροπλασματική μεμβρά νη των μυκήτων και όχι των βακτηρίων, γεγονός που εξηγεί την εκλεκτική του δράση επί των μυκήτων (Cartwright, 1978).…”

Section: μηχανισμος δρασεως των αντιβιοτικωνunclassified

Μικροβιολογικος Ελεγχος Αντιμικροβιακων Παραγοντων

Τουμα¹

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Η ΜΕΛΕΤΗ ΑΥΤΗ ΔΙΑΙΡΕΙΤΑΙ ΣΕ ΤΡΙΑ ΜΕΡΗ: ΣΤΟ ΠΡΩΤΟ ΜΕΡΟΣ (ΑΝΤΙΒΙΟΤΙΚΑ), ΑΞΙΟΛΟΓΗΘΗΚΕ Η IN VITRO ΑΝΤΙΜΙΚΡΟΒΙΑΚΗ ΔΡΑΣΗ 9 ΑΝΤΙΒΙΟΤΙΚΩΝ ΚΑΤΑ 150 ΣΤΕΛΕΧΩΝ P. AERUGINOSA ΠΟΥ ΑΠΟΜΟΝΩΘΗΚΑΝ ΑΠΟ ΔΙΑΦΟΡΑ ΝΟΣΟΚΟΜΕΙΑ ΤΗΣ ΑΘΗΝΑΣ. Η ΕΛΑΧΙΣΤΗ ΑΝΑΣΤΑΛΤΙΚΗ ΠΥΚΝΟΤΗΤΑ (MIC) ΥΠΟΛΟΓΙΣΤΗΚΕ ΜΕ ΤΗ ΜΕΘΟΔΟ ΤΩΝ ΔΙΑΔΟΧΙΚΩΝ ΑΡΑΙΩΣΕΩΝ ΣΕ ΑΓΑΡ. ΠΡΟΕΚΥΨΕ ΟΤΙ Η ΕΠΙ ΤΟΙΣ ΕΚΑΤΟ ΕΥΑΙΣΘΗΣΙΑ ΤΩΝ ΣΤΕΛΕΧΩΝ ΑΥΤΩΝ ΣΤΑ ΕΞΕΤΑΣΤΕΑ ΑΝΤΙΒΙΟΤΙΚΑ ΗΤΑΝ Η ΕΞΗΣ: CIPROFLOXACIN 100%, CEFTAZADIME 88%, THIENAMYCIN 82%, AZTREONAM 81%, NALIDIXIC ACID 51%, CEFOTAXIME 41%, CARBENICILLIN 36%, GENTAMICIN 23% ΚΑΙ CHLORAMPHENICOL 0%. ΣΤΟ ΔΕΥΤΕΡΟ ΜΕΡΟΣ (ΑΝΤΙΣΗΠΤΙΚΑ), ΜΕΛΕΤΗΘΗΚΕ Η ΑΝΤΙΜΙΚΡΟΒΙΑΚΗ ΔΡΑΣΗ 12 ΧΗΜΙΚΩΝ ΕΝΩΣΕΩΝ (IRGASAN - O- PHENYLPHENOL), SODIUM LAURYL SULFATE, SODIUM LAURYL ETHER SULFATE, CETRIMIDE, MIRANOL C2M, MIRANOL CM, MIRANOL C2MSF, MIRANOL H2M, MIRATAINE BB ΚΑΙ MIRATAINE CB. Ο ΠΡΟΣΔΙΟΡΙΣΜΟΣ ΤΗΣ ΑΝΤΙΜΙΚΡΟΒΙΑΚΗΣ ΔΡΑΣΗΣ ΕΓΙΝΕ ΜΕ ΤΗ ΜΕΘΟΔΟ ΔΙΑΛΥΣΕΩΣ- ΕΞΟΥΔΕΤΕΡΩΣΕΩΣ NF T72-50. ΧΡΗΣΙΜΟΠΟΙΗΘΗΚΑΝ ΤΑ ΕΞΗΣ ΣΤΕΛΕΧΗ ΜΙΚΡΟΒΙΩΝ: S.AUREUS, STR. FAECALIS, E. COLI ΚΑΙ P. AERUGINOSA. ΣΤΟ ΤΡΙΤΟ ΜΕΡΟΣ (ΑΝΤΙΜΥΚΗΤΙΑΚΑ), ΕΛΕΓΧΘΗΚΕ Η ΑΝΤΙΜΙΚΡΟΒΙΑΚΗ ΔΡΑΣΗ 5 ΧΗΜΙΚΩΝ ΕΝΩΣΕΩΝ: IRGASAN DP300, O-PHENYLPHENOL, (IRGASAN - O- PHENYLPHENOL), MIRANOL CM ΚΑΙ MIRABOL A 15. Ο ΠΡΟΣΔΙΟΡΙΣΜΟΣ ΤΗΣ ΔΡΑΣΗΣ ΕΓΙΝΕ ΜΕ ΤΗ ΜΕΘΟΔΟ ΔΙΑΛΥΣΕΩΣ-ΕΞΟΥΔΕΤΕΡΩΣΕΩΣ NF T72-200. ΧΡΗΣΙΜΟΠΟΙΗΘΗΚΑΝ ΤΑ ΕΞΗΣ ΣΤΕΛΕΧΗ ΜΥΚΗΤΩΝ: CANDIDA ALBICANS, ASPERGILLUS VERSICOLOR, PENICILLIUM VERRUCOSUM ΚΑΙ CLADOSPORIUM CLADOSPORIOIDES.

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Use of antibiotics. Antifungals.

Cited by 17 publications

References 0 publications

Effect of simultaneous oral and vaginal treatment on the rate of cure and relapse in vaginal candidosis.

Effect of simultaneous oral and vaginal treatment on the rate of cure and relapse in vaginal candidosis.

Clinical Pharmacokinetics of Systemic Antifungal Drugs

Μικροβιολογικος Ελεγχος Αντιμικροβιακων Παραγοντων

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