Data Trace, the publisher of the Handbook of Lower Extremity Infections, 3^rd Edition, has started a bit of a marketing “blitz” in response to the recent release of the book.  I want to take this opportunity to welcome those of you who have just come across this blog either through the recent direct mailing or the ads in PM News or Podiatry Management Magazine.  The purpose of this site is twofold; to allow me to interact with anyone interested in the treatment of lower extremity infections and to give me an opportunity to update the readership on new developments in infectious diseases as they become available.  I regularly review the ID literature for manuscripts that have a direct bearing on the way we treat the lower extremity and attend ID meetings.  This blog allows me to disseminate that information rapidly which would be impossible if I had to wait for my next book revision.

I envision this site as being interactive.  If you have a question about an interesting case (you can even post pictures), have recently heard a lecture, been detailed by an antibiotic representative or just randomly thought of a question on which you would like my thoughts, ASK AWAY!  I will do my best to answer in a timely manner with the best available evidence to support what I say, not to mention a dose of my opinion/experience.    In the future I hope to start running the occasional poll to capture what others may do in a given situation.  If you have any other ideas for this site, please let me know.  I am open to suggestions on how to make it of value to you.

Last week I was invited by Bret Ribotsky, DPM to participate in one of his “Meet the Masters” telephone conferences (www.podiatricsuccess.com).  We had an interesting conversation covering topics such as my definition of “success”, the Journal of the APMA, and my take on some current infectious diseases topics.  After the conference Bret posted a comment on PM News Online (www.podiatrym.com) asking for others’ thoughts on my comments about so-called escalation vs. de-escalation therapy for MRSA.  I felt that I should discuss my thinking on this in a bit more detail.

Traditional approaches to empiric antibiotic selection suggests that you should chose the narrowest spectrum antibiotic against the organisms you suspect are causing the infection.  This, of course, would then be modified based on definitive culture results (if obtained) and the patient’s clinical response. Until relatively recently I would NOT have included MRSA coverage in my empiric selection for most patients.  I believed that beginning therapy against MSSA would be, for most cases except the most severe life and limb threatening infections, sufficient and then, if MRSA was cultured I could always ESCALATE therapy to include MRSA coverage.  My thinking on this approach starting changing about a year or so ago when I was called in to see a patient in our Emergency Department.  This 36 y/o healthy male had no history of any hospitalizations and related not remembering ever taking any antibiotics.  He had dropped a trash can on his foot at work and thought nothing of it until the 1^st MTP joint started becoming hot, red and painful.  During the History, I even specifically asked him “Have you or any of your family members ever had MRSA”.  Now, you pretty much have to be living under a rock not to have heard about MRSA given all of the press coverage.  His answer to me was a simple “What’s that”.  With this History and that response I turned to the Resident and basically stated that I would “eat my hat” if this guy has MRSA.  We started him on non-MRSA coverage.  Well, I think you can imagine what happened.  48 hours later the C&S was returned as CA-MRSA (Picture below is from after initial I&D by my podiatric surgical colleague).  From this point on I have started to practice DE-ESCALATION therapy.  I start the vast majority of my patients, particularly those being hospitalized, as if they have MRSA and will de-escalate to remove the MRSA therapy if MSSA or no staph is found.  Frankly, I don’t remember the last time I was even ABLE to de-escalate.  That is how prevalent MRSA is in our local hospital.

Now, this is NOT to say that my approach is appropriate in every clinical setting and every community.  In the outpatient setting in a locale with a relatively low MRSA rate, you can still begin coverage as if there is only MSSA and switch if the patient does not respond.  Notice I said, “NOT RESPOND” and not, “what the culture report says”!  I continue to believe that patients should be treated, not lab results.  Many studies have shown that, for most uncomplicated skin and skin structure infections, I&D without antibiotic therapy is still an appropriate approach to an abscess caused by MRSA.  If you want to escalate to anti-MRSA therapy then I do believe that doxycycline or minocycline is preferred over trimethoprim/sulfamethoxazole (TMP/SMX).  The reason for this is the significant rate of adverse events found in TMP/SMX and the lack of clinical evidence supporting it.  (I will try to cover this in a future post.  I do cover it in the 3^rd Edition of the Handbook)

I am pleased to announce that we have just posted a few pages from the Ulceration and Infection section of the newly revised Diabetic Foot Infection chapter of the 3rd Edition of the Handbook. Just go to “Preview the Book” in the header above and you will find the pdf link.

I chose this section to include in the book and as a preview since I feel it is important information for anyone treating lower extremity infections to understand. It contains the entire “Executive Summary” of the Infectious Diseases Society of America (IDSA) diabetic foot infection guidelines published in 2004. The Guidelines in their entirety can be found at www.idsociety.org by clicking on the link for “Clinical Practice Guidelines”. These are evidenced based recommendations based on the best available data at the time they were written. The DFI guidelines have been revised and a draft is being presented at the IDSA meeting in Philadelphia later this month  with the hopes of publishing sometime in 2010. This summary includes important points such as #4 – almost all DFIs are caused by gram positive cocci. #5 – Wound infections should be based on clinical, not laboratory grounds. #9 – evidence does not support the antibiotic treatment of clinically uninfected ulcerations, along with 16 other recommendations.

Also in this preview section is the IDSA DFI severity classification system. Unlike other classifications that look at diabetic foot ULCERATIONS, this one is specific for severity of INFECTION. It is easy to understand with only 4 categories and has been independently validated by Larry Lavery and colleagues in a paper published in Clinical Infectious Diseases in 2007 showing that, as the severity increases so do the number of hospitalizations and amputations. This system has now been accepted by most investigators in DFI and is widely used in clinical trials of the condition. It can also be used by everyday clinicians in their clinical practice. For example, under your patient assessment, consider using this system. i.e. “Patient presents today with an IDSA Moderate DFI of the 2nd metatarsal region”.

I hope that you find this new Preview interesting and useful.

It has been about 2 weeks since my first post about ICAAC which has given me some time to ruminate a bit over the happenings there. I have always enjoyed this meeting because its emphasis on new antibiotic development, an area of great interest to me. It is sometimes a bit short on clinical information relevant to lower extremity infections and this year was no different. In fact, other than my poster on the use of daptomycin in diabetic foot infections there were only two other posters, out of thousands, in which the term “diabetic foot infection” even appeared. Both of those studies supported the efficacy of linezolid in the treatment of DFI caused by MRSA. To review some other information I found interesting:

1. During a major symposium on the treatment of gram positive infections, Robert Moellering, MD, one of the gram positive deities in the ID world from Harvard, discussed vancomycin dosing with a lecture entitled “New Approaches to Vancomycin Dosing: Does a higher trough help”. He discussed the new guidelines suggesting troughs between 15-20, a topic I have addressed in this blog. Once again, at least to me, it became clear that the data to support this is very limited, is based on a pharmacokinetic theory, and mostly deals with pneumonia. Dr. Moellering suggested using the vancomycin MIC as a surrogate marker for the appropriate trough for which to aim. The most surprising statement he made was that for an MRSA with a vanco MIC of >1 there is no way to achieve a high enough trough that would still be safe and alternative treatments should be considered (my emphasis). Considering many of us don’t remember the last time we saw an MIC of <1, maybe it is time to finally put vanco to bed??

2. During that same symposium another speaker, David Snydman, MD out of Tufts, discussed linezolid and daptomycin resistance reports. What I found most interesting out of this lecture is that, even after 9+ years of clinical use, the current resistance rates of MRSA for linezolid are sitting at 0.03%. This is a pretty amazingly low number that belays the conventional wisdom, stated throughout the Handbook, that the bugs are always going to be smarter than us. In fairness, resistance rates of coagulase negative staphylococci to linezolid are higher, in some series approaching 5%.

3. I don’t know if the timing of the announcement coinciding with ICAAC was planned or not, but it was announced that another antibiotic, Telavancin, has been approved by the FDA for the treatment of complicated skin and skin structure infections caused by MRSA. This makes the 5th drug for this indication behind vancomycin, linezolid, daptomycin and tigecylcine. Telavancin (Vibativ), developed by Theravance and Astellas, is an IV only lipoglycopeptide. I saw some of their early data a few years ago but am not up on the latest so I really don’t know how to place this drug yet. I am also concerned about some adverse event rates and black box warnings. More to come in the future on this one.

4. An upstart out of the UK, NovaBiotics, presented 2 posters on a “novel fungicidal peptide” for the treatment of onychomycosis. This was really preliminary, mostly in vitro stuff but I do think that the entire peptide class of antibiotics show promise for lots of different applications (can anyone remember Pexiganin?).

5. David Nicolau, PharmD out of Hartford, has done some great work in skin and skin structure infections. Amongst the many posters he presented was one that looked at the development of carbapenem resistance to Pseudomonas aeruginosa when 25 hospitals started using ertapenem. His results echo that of previous authors who have shown time and time again that Pseudomonal cross resistance to other carbapenems does not occur just because a hospital uses ertapenem. This has been a concern voiced by many ID specialists and pharmacists effectively blocking the use of this once daily drug in many hospitals specifically in diabetic foot infections. It is one of only three drugs (along with linezolid and piperacillin/tazobactam) currently approved for this indication.

Well, that is it for my review of ICAAC. Sorry for the long post but I wanted to get as much information as I could out to you in a timely manner.

I just wanted to drop in a short post to tell everybody that the 3rd Edition of the Handbook of Lower Extremity Infections has been published and is now shipping. For anyone who ordered the book, if you have not received it already, you should be getting your copy soon. For those waiting for the finished product, wait no more! Place your order. Sorry for the commercial nature of this post, but I am really proud of the finished product and wanted to “shout it out” a bit. Many thanks to the entire staff at my new publisher, Data Trace for all of the hard work that went into this project. I have worked with many publishers over the years and Data Trace has done a wonderful job.