Chemical structure of telithromycin.
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Ketek

Telithromycin is the first ketolide antibiotic to enter clinical use. It is used to treat mild to moderate respiratory infections. Telithromycin is sold under the brand name of Ketek. more...

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Telithromycin is a semi-synthetic erythromycin derivative. It is created by substituting the cladinose sugar with a ketogroup and adding a carbamate ring in the lactone ring. An alkyl-aryl moiety is attached to this carbamate ring. Furthermore, the carbon at position 6 has been methylated, like in clarithromycin, to achieve better acid-stability.

History

French pharmaceutical company Hoechst Marion Roussel (later Aventis) started phase II/III trials of telithromycin (HMR-3647) in 1998. Telithromycin was approved by the European Commission in July 2001 and subsequently came on sale in October 2001. In USA, telithromycin gained FDA approval April 1, 2004 .

Available forms

Telithromycin is administered as tablets. Two 400mg tablets to be taken together, daily, with or without food.

Mechanism of action

Telithromycin prevents bacteria from growing, by interfering with their protein synthesis. Telithromycin binds to the subunit 50S of the bacterial ribosome, and thus inhibits the translocation of peptides. Telithromycin has over 10 times higher affinity to the subunit 50S than erythromycin. In addition, telithromycin binds simultaneously in to two domains of 23S RNA of the ribosomal subunit 50S, where older macrolides bind only in one. Telithromycin can also inhibit the formation of ribosomal subunits 50S and 30S.

Pharmacokinetics

Unlike erythromycin, telithromycin is acid-stable and can therefore be taken orally without being protected from gastric acids. It is fairly rapidly absorbed, and diffused into most tissues and phagocytes. Due to the high concentration in phagocytes, telithromycin is actively transported to the site of infection. During active phagocytosis, large concentrations of telithromycin is released. The concentration of telithromycin in the tissues much higher than in plasma.

Metabolism

It is metabolized mainly in the liver, the main elimination route being the bile, a small portion is also excreted into the urine. About one third is excreted unchanged into the bile and urine, the biliary route being favoured. Telithromycin's half-life is approximately 10 hours.so

Side effects

Most common side-effects are gastrointestinal; diarrhoea, nausea, abdominal pain and vomiting. Headache and disturbances in taste also occur. Less common side-effects include palpitations, blurred vision and rashes.

Rare, but severe side effects reported in January 2006 involve damage to the liver. Three different incidents reported, one ending in death, one in a liver transplant and one case of drug induced hepatitis.

Has been known to cause false positive readings in drug screenings for cocaine and amphetamines.

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Early intrathecal analgesia does not increase cesarean sections
From Journal of Family Practice, 6/1/05 by C.A. Wong

Wong CA, Scavone BM, Peaceman AM, et al. The risk of cesarean delivery with neuraxial analgesia given early versus late in labor. N Eng J Med 1005; 352:655-665.

* Clinical Question

Does early administration of neuraxial analgesia in labor increase the risk of cesarean delivery?

* Bottom Line

Intrathecal fentanyl followed by epidural bupivacaine plus fentanyl, if needed for pain relief, in early labor is not associated with a higher cesarean delivery than systemic hydromorphone for early labor. The neuraxial approach also provides more effective analgesia and a shorter mean duration of first-stage labor. (LOE=1b)

Study Design

Randomized controlled trial (nonblinded)

Allocation

Concealed

Setting

Inpatient (ward only)

Synopsis

Epidural analgesia, when given before a cervical dilatation of 4 cm, has been associated with higher cesarean delivery rate. Systemic narcotics are often used for women requesting analgesia in early labor.

In this trial, 750 women with cervical dilatation of less than 4 cm were randomized at the first request for analgesia to a neuraxial analgesia group that received intrathecal fentanyl 25 mg or to a control group that received 1 mg intravenous hydromorphone plus 1 mg intramuscular hydromorphone. At the second request for analgesia, even with cervical dilatation still less than 4 cm, the neuraxial group received epidural analgesia with bupivacaine at half the usual strength plus fentanyl, while the control group received the same dosing of hydromorphone.

The cesarean delivery rate was a similar 18% to 20% in the 2 groups. The mean time from first administration of analgesia to complete dilatation was 90 minutes shorter in the neuraxial group (295 minutes vs 385 minutes). Pain control after the first dose of analgesia was better in the neuraxial group (mean = 2 vs 6, on a 0-10 scale).

DRUG BRAND NAMES

Amoxicillin * Amoxil; Trimox; Wymox Amoxicillin-clavulanate * Augmentin Hydromorphone * Dilaudid Telithromycin * Ketek Zolpidem * Ambien

COPYRIGHT 2005 Dowden Health Media, Inc.
COPYRIGHT 2005 Gale Group

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