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azithromycin a rationale choice for anterior and posterior blepharitis

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  • azithromycin a rationale choice for anterior and posterior blepharitis

    Who knows what to believe anymore. Here is an article on Azasite,

    http://otasia.advanstar.com/otasia/a...eID=1&sk=&date

    Favorable profile makes azithromycin a rationale choice for anterior and posterior blepharitis


    Evaluations by independent investigators showed drug was safe, well tolerated

    Mar 15, 2008
    By:Cheryl Guttman
    Ophthalmology Times


    Key Points
    The efficacy of azithromycin for treating both anterior and posterior blepharitis may be attributed to multiple features of this agent.

  • #2
    Hi what is Azasite?

    That link doesnt access the article, have you got another link?

    Or can you copy and paste the article on here.
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    • #3
      Favorable profile makes azithromycin a rationale choice for anterior and posterior blepharitis

      Evaluations by independent investigators showed drug was safe, well tolerated

      Mar 15, 2008
      By: Cheryl Guttman
      Ophthalmology Times



      Pages | 1 | 2


      Key Points
      The efficacy of azithromycin for treating both anterior and posterior blepharitis may be attributed to multiple features of this agent.

      Results from small studies undertaken by independent investigators indicate that azithromycin 1% ophthalmic solution (AzaSite, Inspire Pharmaceuticals) offers promise as a safe, well-tolerated, and rapidly effective therapy for anterior and posterior blepharitis.

      Jodi Luchs, MD, explored the potential of azithromycin 1% as a treatment for blepharitis in an uncontrolled pilot study including 12 patients with posterior blepharitis and 12 patients with anterior lid margin disease. Patients with posterior blepharitis used the azithromycin twice daily, instilling it into the eye or onto the lid surface, while anterior blepharitis patients used the drop twice daily for 1 week and then decreased the dosing frequency to once daily. All patients were also instructed in lid hygiene procedures, including application of warm compresses plus use of lid scrubs by the anterior blepharitis patients.

      When evaluated 2 weeks after starting azithromycin, all anterior blepharitis patients demonstrated resolution of crusting and collarettes along with significant reduction in lid margin inflammation and improvement in subjective symptoms. Ten of the 12 posterior blepharitis patients demonstrated reduced lid margin erythema and improvement in the appearance of the meibomian orifices and/or meibomian gland secretions. Especially noteworthy was the fact that most of the 10 responders in the posterior blepharitis group reported onset of benefits after just 1 week of starting treatment, said Dr. Luchs, director, department of refractive surgery, North Shore/Long Island Jewish Health System, Manhasset, NY, and assistant clinical professor of ophthalmology and visual sciences, Albert Einstein College of Medicine, Bronx, NY.


      "Lid hygiene is a cornerstone of care for both anterior and posterior blepharitis, but historically, anterior blepharitis treatment would include a topical antibiotic to address its infectious etiology while an agent with anti-inflammatory activity, either an oral tetracycline or macrolide or a topical corticosteroid, could be added to warm compresses and lid hygiene for posterior blepharitis. It appears that azithromycin 1% offers a single solution for managing both of these forms of blepharitis," he said.

      The efficacy of azithromycin for treating both anterior and posterior blepharitis may be attributed to multiple features of this agent, including a dual mechanism of action; azithromycin has both antimicrobial and anti-inflammatory properties, as well as excellent penetration into target tissues.

      "There are data to show that azithromycin has anti-inflammatory activity independent of its antimicrobial effects and also documenting that it achieves high concentrations in the cornea, conjunctiva, and lid after topical administration of just a single drop. The latter feature relates to both an intrinsic property of the molecule and the DuraSite drug delivery system used to formulate AzaSite that enhances drug tissue penetration by prolonging drug delivery," explained Dr. Luchs.

      He noted that the efficacy of azithromycin in treating anterior blepharitis was anticipated considering azithromycin provides good coverage against staphylococcal bacteria implicated in the pathogenesis of this form of lid margin disease. The rapid and significant improvement achieved by patients with posterior blepharitis was more unexpected when considered relative to the responses achieved with other commonly used treatments for posterior blepharitis. For example, it can take 6 weeks or longer for patients to respond to anti-inflammatory treatment with oral doxycycline whereas management with lid hygiene measures alone is unlikely to afford such dramatic symptomatic and objective improvement, especially after just a few weeks of therapy, noted Dr. Luchs.

      "On the other hand, the efficacy of azithromycin in treating posterior blepharitis is not that surprising if one takes into account its anti-inflammatory activity and tissue penetration properties," Dr. Luchs said.

      Treatment with azithromycin was also very well-tolerated. One patient with anterior blepharitis stopped azithromycin prematurely due to stinging upon instillation, but even that patient reported symptomatic improvement and had clinical resolution of the lid margin findings. Of the two posterior blepharitis patients who did not respond adequately to azithromycin, one discontinued treatment because of stinging. No other adverse events were noted.

      "Anterior blepharitis will respond to treatment with ophthalmic antibiotic ointments, such as bacitracin or erythromycin. However, these ointment preparations tend to have poor patient acceptance because they result in lid gumming and blurred vision. Systemic side effects can also be an issue with oral doxycycline that may be prescribed for patients with posterior blepharitis. Compared with these alternate regimens, azithromycin 1% ophthalmic solution is safer and better tolerated," noted Dr. Luchs.

      He added that the ability of the DuraSite vehicle to coat the ocular surface is an added benefit of using azithromycin 1% considering that tear film dysfunction and ocular surface damage are common comorbid findings in patients with posterior blepharitis.

      "A close relative of the DuraSite vehicle was previously marketed as an artificial tear. In addition to improving retention of the active ingredient on the ocular surface, this vehicle provides good ocular surface lubrication and helps to relieve dry eye symptoms that blepharitis patients may suffer as a result of an unstable tear film," said Dr. Luchs.

      Dr. Luchs has just launched a controlled trial investigating azithromycin 1% for the treatment of posterior blepharitis in which patients are being randomized to lid massage alone or combined with azithromycin. A protocol for a controlled trial evaluating the efficacy and safety of azithromycin 1% for the treatment of anterior blepharitis is under development.

      Combination regimen

      Stanley Bykov, MD, director, The Ocular Center, Brooklyn, NY, undertook a prospective study evaluating blepharitis treatment with azithromycin 1% (AzaSite, Inspire) in combination with loteprednol etabonate 0.2% (Alrex, Bausch & Lomb). A control group was treated with the fixed combination corticosteroid-antibiotic ointment containing neomycin sulfate-polymixin B-dexamethasone (Maxitrol, Alcon).

      Patients enrolled in the study presented with both anterior and posterior blepharitis. The results showed patients treated with azithromycin plus the mild corticosteroid achieved greater improvement and with a faster onset compared with the controls.


      "Azithromycin may be expected to be useful in treating blepharitis because it has excellent anti-staphylococcal activity. However, as an added benefit, azithromycin also has anti-inflammatory activity. Therefore, a regimen combining azithromycin with a mild corticosteroid may be expected to provide significant anti-inflammatory effects," said Dr. Bykov.

      He added, "If azithromycin works via dual mechanisms of action in treating blepharitis, it may be also effective as monotherapy. Investigation of that hypothesis would be the subject for another study."

      Dr. Bykov's study included 25 patients who used azithromycin 1% once daily in the evening plus loteprednol etabonate 0.2% twice daily. A second group of 25 patients were in the control group and used the fixed combination corticosteroid-antibiotic product twice daily. All patients also were instructed on the routine use of good lid hygiene, including washing the lids, applying warm compresses, and removing debris from the lids.

      Patients returned for evaluation at 2 and 4 weeks after starting treatment, and their responses were assessed using a blepharitis severity grading scale of 0 (none) to 4 (most severe). Baseline severity ratings ranged from 1 to 4.

      At the 2-week follow-up visit, 85% of patients in the azithromycin-loteprednol group achieved a 1-point or greater improvement from their baseline blepharitis severity score compared with only 45% of patients in the control group. At the end of the study, 95% of patients in the azithromycin-loteprednol group achieved clearance of blepharitis with a severity score of "0" compared with only 60% of the controls.

      Treatment with azithromycin-loteprednol was also very safe and well tolerated. There were no adverse events judged related to use of this combination of medications whereas in the control group, lid erythema, considered a sign of an allergic reaction, was noted in 6 (24%) patients when they returned for the 4-week visit.

      "Both of the antibiotic ingredients in Maxitrol are contact allergens, and hypersensitivity reactions to neomycin or polymixin might mitigate the anti-inflammatory benefits of treatment with this fixed combination antibiotic-corticosteroid product," Dr. Bykov said.

      The one patient in the azithromycin-loteprednol group who did not improve had concomitant rosacea and a longstanding history of chronic blepharitis. The blepharitis was successfully treated when oral doxycycline was added to the medication regimen.

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