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type=\u0022text\/css\u0022 rel=\u0022stylesheet\u0022 href=\u0022\/\/d282kpwvnogo5m.cloudfront.net\/sites\/default\/files\/advagg_css\/css__ce2QY63WIanKyr8eSq7eavr1XQRRmFD6ZSmwpyJi8lM__zXwFqpqmxrZOXXcd_TpBQpjuELbmIP9wBR5UuTDWAO4__YJWWMMdfCJuAFm5cUEp88OsodhO3ZA-2lzRfoBsSlk4.css\u0022 media=\u0022all\u0022 \/\u003E\n\u003Clink rel=\u0027stylesheet\u0027 type=\u0027text\/css\u0027 href=\u0027\/sites\/all\/modules\/contrib\/panels\/plugins\/layouts\/onecol\/onecol.css\u0027 \/\u003E\u003C\/head\u003E\u003Cbody\u003E\u003Cdiv class=\u0022panels-ajax-tab-panel panels-ajax-tab-panel-sageoa-tab-art\u0022\u003E\u003Cdiv class=\u0022panel-display panel-1col clearfix\u0022 \u003E\n  \u003Cdiv class=\u0022panel-panel panel-col\u0022\u003E\n    \u003Cdiv\u003E\u003Cdiv class=\u0022panel-pane pane-highwire-markup\u0022 \u003E\n  \n      \n  \n  \u003Cdiv class=\u0022pane-content\u0022\u003E\n    \u003Cdiv class=\u0022highwire-markup\u0022\u003E\u003Cdiv xmlns=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022 id=\u0022content-block-markup\u0022 xmlns:xhtml=\u0022http:\/\/www.w3.org\/1999\/xhtml\u0022\u003E\u003Cdiv class=\u0022article fulltext-view \u0022\u003E\u003Cspan class=\u0022highwire-journal-article-marker-start\u0022\u003E\u003C\/span\u003E\u003Cdiv class=\u0022section abstract\u0022 id=\u0022abstract-1\u0022\u003E\u003Ch2\u003ESummary\u003C\/h2\u003E\n            \u003Cp id=\u0022p-1\u0022\u003EIt is projected that there will be 8.7 million patients with dementia who live in the United States by 2030 [Guttman R et al. \u003Cem\u003EArch Fam Med\u003C\/em\u003E 1999]. Alzheimer Disease (AD) is a complex, debilitating disease, and due to conflicting guidelines, there is confusion among practitioners regarding the best treatment practices for a patient who suffers from AD. Thus far, AD treatment is limited to symptomatic therapy, but prevention and disease-modifying therapy are the ultimate goals.\u003C\/p\u003E\n         \u003C\/div\u003E\u003Cul class=\u0022kwd-group\u0022\u003E\u003Cli class=\u0022kwd\u0022\u003EDementias Guidelines\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003EExtrapyramidal \u0026amp; Movement Disorders\u003C\/li\u003E\u003Cli class=\u0022kwd\u0022\u003ECognitive Disorders\u003C\/li\u003E\u003C\/ul\u003E\u003Cp id=\u0022p-2\u0022\u003EIIt is projected that there will be 8.7 million patients with dementia who live in the United States by 2030 [Guttman R et al. \u003Cem\u003EArch Fam Med\u003C\/em\u003E 1999]. Cognitive decline that is associated with mild to moderate Alzheimer Disease (as measured by MMSE score) progresses an average of 2 to 4 points per year if left untreated [Becker JT et al. \u003Cem\u003EArch Neurol\u003C\/em\u003E 1988]. Alzheimer Disease (AD) is a complex, debilitating disease, and due to conflicting guidelines, there is confusion among practitioners regarding the best treatment practices for a patient who suffers from AD. Thus far, AD treatment is limited to symptomatic therapy, but prevention and disease-modifying therapy are the ultimate goals.\u003C\/p\u003E\u003Cp id=\u0022p-3\u0022\u003EMethodologies for generating a consensus and evaluating evidence are evolving. Gary W. Small, MD, David Geffen School of Medicine, University of California, Los Angeles, CA, compared the American Association for Geriatric Psychiatry (AAGP) and American Psychiatric Association (APA) recommendations. Both models emphasize nonpharmacological and pharmacological therapies, but while the AAGP concentrates on AD, the APA has a wider focus that includes a recommendation coding system that is based on clinical evidence (I=substantial confidence, II=moderate confidence, and III=recommendation is based on individual circumstances with a lower level of confidence). The American Academy of Neurology (AAN) guidelines, presented by Martin R. Farlow, MD, Indiana University School of Medicine, Indianapolis, IN, use a coding system that is similar to the APA, but the recommendations are categorized by class (I=AAN Standard recommendation based on 1 or more randomized clinical trials with a high level of certainty, II=AAN Guideline recommendation based on well-designed observational trials with a moderate degree of certainty, and III=AAN Practice Option recommendation based on expert opinion and\/or case reports, so clinical utility is uncertain).\u003C\/p\u003E\u003Cp id=\u0022p-4\u0022\u003EWilliam Maurice Redden, MD, St. Louis University School of Medicine, St. Louis, MO, discussed the clinical pharmacology of approved AD therapies that are related to the Alzheimer\u0027s Disease Management Council (ADMC) consensus and the National Institute for Health and Clinical Excellence (NICE). There are currently 4 cholinesterase inhibitors that are approved by the Food and Drug Administration (FDA) for the treatment of mild to moderate AD: tacrine, donepezil, galantamine, and rivastigmine. The APA guidelines state that 30% to 40% of patients with mild to moderate AD may have modest benefits with cholinesterase inhibitor therapy, and it should also be considered for patients with dementia that is associated with Parkinson Disease (APA Coding Level I). Additionally, memantine and donepezil have been FDA-approved for the treatment of moderate to severe AD. The AAN guidelines do not address the use of cholinesterase inhibitors or memantine in AD patients. Prof. Farlow attributes this discrepancy to the fact that the AAN guidelines are 8 years old and are in need of revision.\u003C\/p\u003E\u003Cp id=\u0022p-5\u0022\u003ECharles A. Cefalu, MD, MS, Professor and Chief, Section of Geriatric Medicine, Louisiana State University Health Sciences Center and School of Medicine at New Orleans, New Orleans, LA, presented the American College of Physicians (ACP)\/American Academy of Family Physicians (AAFP) 2007 guidelines for the pharmacological management of patients with AD. The guidelines suggest that the initiation of cholinesterase inhibitor or memantine therapy should be based on individualized assessment after careful consideration of tolerability, adverse effect profiles, ease of use, and cost. The level of confidence that is associated with this ACP\/AAFP recommendation is weak, based on insufficient evidence that compares the effectiveness of these agents for the treatment of AD. Prof. Cefalu expressed that the high level of cholinesterase inhibitor discontinuation among AD patients remains a problem and that withdrawal may be associated with acceleration of cognitive and physical decline. Therefore, it is important to educate family members, caregivers, and patients (when appropriate) regarding the risks and benefits of these pharmacological treatments prior to initiating therapy.\u003C\/p\u003E\u003Cp id=\u0022p-6\u0022\u003EThere are a few topics that correspond across all of these guidelines. The use of atypical antipsychotics has been associated with an increased risk of death that is related to vascular disease in elderly patients with dementia. Also, the CATIE study suggested that the adverse effects that are associated with these agents may offset the advantages in the efficacy of atypical antipsychotic drugs in AD patients [Schneider LS et al. \u003Cem\u003EN Engl J Med\u003C\/em\u003E 2006]. Therefore, they should only be used after careful assessment of the risks and benefits. These guidelines all agree that the use of NSAIDS, statins, and estrogen are no longer recommended due to their lack of efficacy and safety. The presenters all stressed the importance of early detection and the need for disease-modifying therapies.\u003C\/p\u003E\u003Cul class=\u0022copyright-statement\u0022\u003E\u003Cli class=\u0022fn\u0022 id=\u0022copyright-statement-1\u0022\u003E\u00a9 2009 MD Conference Express\u003C\/li\u003E\u003C\/ul\u003E\u003Cspan class=\u0022highwire-journal-article-marker-end\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Cspan id=\u0022related-urls\u0022\u003E\u003C\/span\u003E\u003C\/div\u003E\u003Ca href=\u0022http:\/\/mdc.sagepub.com\/content\/9\/3\/30.abstract\u0022 class=\u0022hw-link hw-link-article-abstract\u0022 data-icon-position=\u0022\u0022 data-hide-link-title=\u00220\u0022\u003EView Summary\u003C\/a\u003E\u003C\/div\u003E  \u003C\/div\u003E\n\n  \n  \u003C\/div\u003E\n\u003C\/div\u003E\n  \u003C\/div\u003E\n\u003C\/div\u003E\n\u003C\/div\u003E\u003Cscript type=\u0022text\/javascript\u0022 src=\u0022http:\/\/mdc.sagepub.com\/sites\/all\/modules\/highwire\/highwire\/plugins\/highwire_markup_process\/js\/highwire_openurl.js?nzmk6p\u0022\u003E\u003C\/script\u003E\n\u003C\/body\u003E\u003C\/html\u003E"}