1,837 results on '"Eichenfield, Lawrence F"'
Search Results
2. Practical Management of the JAK1 Inhibitor Abrocitinib for Atopic Dermatitis in Clinical Practice: Special Safety Considerations
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Gooderham, Melinda J., de Bruin-Weller, Marjolein, Weidinger, Stephan, Cork, Michael J., Eichenfield, Lawrence F., Simpson, Eric L., Tsianakas, Athanasios, Kerkmann, Urs, Feeney, Claire, and Romero, William
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- 2024
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3. Efficacy, Safety, and Long-Term Disease Control of Ruxolitinib Cream Among Adolescents with Atopic Dermatitis: Pooled Results from Two Randomized Phase 3 Studies
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Eichenfield, Lawrence F., Simpson, Eric L., Papp, Kim, Szepietowski, Jacek C., Blauvelt, Andrew, Kircik, Leon, Silverberg, Jonathan I., Siegfried, Elaine C., Kuligowski, Michael E., Venturanza, May E., Kallender, Howard, Ren, Haobo, and Paller, Amy S.
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- 2024
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4. Triple Combination Clindamycin Phosphate 1.2%/Adapalene 0.15%/Benzoyl Peroxide 3.1% for Acne: Efficacy and Safety from a Pooled Phase 3 Analysis
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Kircik, Leon H., Stein Gold, Linda, Gold, Michael, Weiss, Jonathan S., Harper, Julie C., Del Rosso, James Q., Bunick, Christopher G., Bhatia, Neal, Tanghetti, Emil A., Eichenfield, Lawrence F., Baldwin, Hilary, Draelos, Zoe D., Callender, Valerie D., Han, George, Gooderham, Melinda J., Sadick, Neil, Lupo, Mary P., Lain, Edward (Ted), and Werschler, William Philip
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- 2024
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5. Maintenance of Investigator’s Static Global Assessment Response with Once-Daily Crisaborole in Participants with Mild to Moderate Atopic Dermatitis
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Eichenfield, Lawrence F., Stein Gold, Linda F., Lynde, Charles, Guenther, Lyn, Greenberger, Shoshana, Chu, Chia-Yu, Ghodsi, Zara, Vlahos, Bonnie, Sanders, Paul, Cha, Amy, and Canosa, Juliana M.
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- 2024
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6. Satisfaction with Control of Mild to Moderate Atopic Dermatitis with Ruxolitinib Cream: US Physician and Patient Perspectives
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Eichenfield, Lawrence F., Liu, Jinan, Marwaha, Simran, Piercy, James, Sturm, Daniel, and Anderson, Peter
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- 2024
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7. Infections in Children Aged 6 Months to 5 Years Treated with Dupilumab in a Placebo-Controlled Clinical Trial of Moderate-to-Severe Atopic Dermatitis
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Paller, Amy S., Siegfried, Elaine C., Cork, Michael J., Arkwright, Peter D., Eichenfield, Lawrence F., Ramien, Michele, Khokhar, Faisal A., Chen, Zhen, Zhang, Annie, and Cyr, Sonya L.
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- 2024
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8. Safety and Efficacy of Lebrikizumab in Adolescent Patients with Moderate-to-Severe Atopic Dermatitis: A 52-Week, Open-Label, Phase 3 Study.
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Paller, Amy S, Flohr, Carsten, Eichenfield, Lawrence F, Irvine, Alan D, Weisman, Jamie, Soung, Jennifer, Pinto Correia, Ana, Natalie, Chitra R, Rodriguez Capriles, Claudia, Pierce, Evangeline, Reifeis, Sarah, Gontijo Lima, Renata, Armengol Tubau, Clara, Laquer, Vivian, and Weidinger, Stephan
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Adolescents ,Efficacy ,IL-13 ,Lebrikizumab ,Moderate-to-severe atopic dermatitis ,Safety ,Depression ,Mental Health ,Clinical Research ,Pediatric ,Patient Safety ,Clinical Trials and Supportive Activities ,Brain Disorders ,Evaluation of treatments and therapeutic interventions ,6.1 Pharmaceuticals ,Good Health and Well Being ,Clinical Sciences - Abstract
IntroductionAtopic dermatitis (AD) is a chronic inflammatory skin disorder with limited treatment options for adolescents with moderate-to-severe disease. Lebrikizumab, a monoclonal antibody targeting interleukin (IL)-13, demonstrated clinical benefit in previous Phase 3 trials: ADvocate1 (NCT04146363), ADvocate2 (NCT04178967), and ADhere (NCT04250337). We report 52-week safety and efficacy outcomes from ADore (NCT04250350), a Phase 3, open-label study of lebrikizumab in adolescent patients with moderate-to-severe AD. The primary endpoint was to describe the proportion of patients who discontinued from study treatment because of adverse events (AEs) through the last treatment visit.MethodsAdolescent patients (N = 206) (≥ 12 to
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- 2023
9. Diagnosis and Management of Pediatric Chronic Hand Eczema: The PeDRA CACHES Survey
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Haft, Michael A, Park, Helen H, Lee, Stephanie S, Sprague, Jessica M, Paller, Amy S, Cotton, Colleen H, Thyssen, Jacob P, and Eichenfield, Lawrence F
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Biomedical and Clinical Sciences ,Clinical Sciences ,Skin ,Humans ,Child ,United States ,Dermatology ,Prospective Studies ,Quality of Life ,Eczema ,Dermatitis ,Atopic ,Paediatrics and Reproductive Medicine ,Pharmacology and Pharmaceutical Sciences ,Pediatrics ,Paediatrics ,Pharmacology and pharmaceutical sciences - Abstract
BackgroundChronic hand eczema (CHE) significantly impacts quality of life. Published literature on pediatric CHE (P-CHE) in North America including knowledge on epidemiology and standard evaluation and management is limited.ObjectiveOur objective was to assess diagnostic practices when evaluating patients with P-CHE in the US and Canada, produce data on therapeutic agent prescribing practices for the disorder, and lay the foundation for future studies.MethodsWe surveyed pediatric dermatologists to collect data on clinician and patient population demographics, diagnostic methods, therapeutic agent selection, among other statistics. From June 2021 to January 2022, a survey was distributed to members of the Pediatric Dermatology Research Alliance (PeDRA).ResultsFifty PeDRA members responded stating that they would be interested in participating, and 21 surveys were completed. For patients with P-CHE, providers most often utilize the diagnoses of irritant contact dermatitis, allergic contact dermatitis, dyshidrotic hand eczema, and atopic dermatitis. Contact allergy patch testing and bacterial hand culture are the most used tests for workup. Nearly all utilize topical corticosteroids as first line therapy. Most responders report that they have treated fewer than six patients with systemic agents and prefer dupilumab as first-line systemic therapy.ConclusionsThis is the first characterization of P-CHE among pediatric dermatologists in the United States and Canada. This assessment may prove useful in designing further investigations including prospective studies of P-CHE epidemiology, morphology, nomenclature, and management.
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- 2023
10. Pediatric chronic hand eczema: Epidemiology, clinical presentation, and management
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Haft, Michael A, Park, Helen H, Lee, Stephanie S, Sprague, Jessica M, and Eichenfield, Lawrence F
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Biomedical and Clinical Sciences ,Clinical Sciences ,Pediatric AIDS ,Pediatric ,Clinical Research ,Skin ,Inflammatory and immune system ,Good Health and Well Being ,adolescent ,child ,childhood ,children ,chronic ,dermatitis ,eczema ,hand ,literature ,manus ,pediatric ,persistent ,questions ,recalcitrant ,review ,skin ,summary ,teenage ,teenager ,young - Abstract
Chronic hand eczema (CHE) is persistent inflammatory dermatitis that may significantly affect the quality of life, with psychosocial effects, impact on school, work, and leisure activities, influence on socioeconomic status, and high health care costs. Pediatric-CHE (P-CHE) has a high prevalence yet has not been extensively studied in children and adolescents. There is minimal published data on P-CHE in North America, and no specific management guidelines. Limited prevalence data show broad ranges (0.9%-4.4%) in preschool and school children, with 1 study stating up to 10.0% 1-year prevalence for ages 16 to 19 years. Atopic dermatitis and allergic contact dermatitis appear important in the pathogenesis of this disease process, although there is limited pediatric data assessing disease associations and no standardized methodology for evaluating this disorder. Given the potential life-changing consequences of P-CHE, further research into this disease process is warranted to help generate best therapeutic practices and minimize this disease process' morbidity in adulthood.
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- 2023
11. Exposure to isocyanates predicts atopic dermatitis prevalence and disrupts therapeutic pathways in commensal bacteria
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Zeldin, Jordan, Chaudhary, Prem Prashant, Spathies, Jacquelyn, Yadav, Manoj, D’Souza, Brandon N, Alishahedani, Mohammadali E, Gough, Portia, Matriz, Jobel, Ghio, Andrew J, Li, Yue, Sun, Ashleigh A, Eichenfield, Lawrence F, Simpson, Eric L, and Myles, Ian A
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Clinical Research ,Humans ,Dermatitis ,Atopic ,Dysbiosis ,Isocyanates ,Prevalence ,Bacteria ,Skin - Abstract
Atopic dermatitis (AD) is a chronic inflammatory skin condition increasing in industrial nations at a pace that suggests environmental drivers. We hypothesize that the dysbiosis associated with AD may signal microbial adaptations to modern pollutants. Having previously modeled the benefits of health-associated Roseomonas mucosa, we now show that R. mucosa fixes nitrogen in the production of protective glycerolipids and their ceramide by-products. Screening EPA databases against the clinical visit rates identified diisocyanates as the strongest predictor of AD. Diisocyanates disrupted the production of beneficial lipids and therapeutic modeling for isolates of R. mucosa as well as commensal Staphylococcus. Last, while topical R. mucosa failed to meet commercial end points in a placebo-controlled trial, the subgroup who completed the full protocol demonstrated sustained, clinically modest, but statistically significant clinical improvements that differed by study site diisocyanate levels. Therefore, diisocyanates show temporospatial and epidemiological association with AD while also inducing eczematous dysbiosis.
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- 2023
12. Impact of Ruxolitinib Cream on Work Productivity and Activity Impairment and Associated Indirect Costs in Patients with Atopic Dermatitis: Pooled Results From Two Phase III Studies
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Bloudek, Lisa, Eichenfield, Lawrence F, Silverberg, Jonathan I, Joish, Vijay N, Lofland, Jennifer H, Sun, Kang, Augustin, Matthias, Migliaccio-Walle, Kristen, and Sullivan, Sean D
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Biomedical and Clinical Sciences ,Clinical Sciences ,Comparative Effectiveness Research ,Clinical Research ,Evaluation of treatments and therapeutic interventions ,6.1 Pharmaceuticals ,Humans ,Female ,Adult ,Child ,Dermatitis ,Atopic ,Treatment Outcome ,Pyrimidines ,Nitriles ,Emollients ,Double-Blind Method ,Severity of Illness Index ,Dermatology & Venereal Diseases ,Clinical sciences - Abstract
BackgroundAtopic dermatitis is a chronic inflammatory skin disease that can negatively impact work productivity and daily activities. Ruxolitinib cream, a Janus kinase inhibitor, demonstrated efficacy and safety in patients with atopic dermatitis in two phase III studies (TRuE-AD1 and TRuE-AD2).ObjectiveThis post hoc analysis sought to describe the effects of ruxolitinib cream on work productivity and activity impairment from pooled data from the phase III studies, to estimate indirect costs due to atopic dermatitis, and to estimate the incremental cost savings with ruxolitinib cream versus vehicle cream.MethodsPatients in both studies were ≥ 12 years old with atopic dermatitis for ≥ 2 years, an Investigator's Global Assessment score of 2 or 3, and a 3-20% affected body surface area at baseline. Patients were randomized 2:2:1 to receive ruxolitinib cream (0.75% or 1.5%) or vehicle cream for 8 weeks. Patient self-reported productivity in the efficacy-evaluable population was assessed at weeks 2, 4, and 8 using the Work Productivity and Activity Impairment Questionnaire-Specific Health Problem version 2.0. Statistical significance for the two doses versus vehicle was calculated using an analysis of covariance. Work Productivity and Activity Impairment overall work impairment scores were converted to a model of costs per employed patient due to lost productivity and incremental cost savings from ruxolitinib cream treatment using a human capital approach.ResultsOf 1249 patients enrolled (median age, 32 years; female sex, 61.7%), 1208 were included in the efficacy-evaluable population. Patients applying 0.75% or 1.5% ruxolitinib cream had significant changes in overall work impairment (- 17.9% [0.75% strength] and - 15.0% [1.5% strength] vs - 5.7% for vehicle; p < 0.0001 for both) and daily activity impairment (- 20.6% [0.75% strength] and - 21.5% [1.5% strength] vs - 10.6% for vehicle; p < 0.0001 for both). These corresponded to estimated lost productivity costs in 2021 US dollars of $1313 (0.75% strength) and $1242 (1.5% strength) versus $2008 (vehicle) over the 8-week trial period. Compared with a patient receiving vehicle, incremental annual indirect cost savings were estimated to be $5302 with 0.75% ruxolitinib cream and $4228 with 1.5% ruxolitinib cream.ConclusionsRuxolitinib cream therapy is associated with improved work productivity and daily activity compared with vehicle and is estimated to reduce the indirect cost burden on the patient.Clinical trial registrationClinicalTrials.gov identifiers: NCT03745638 (registered 19 November, 2018) and NCT03745651 (registered 19 November, 2018).
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- 2023
13. No Increased Risk of Overall Infection in Adults with Moderate-to-Severe Atopic Dermatitis Treated for up to 4 Years with Dupilumab
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Blauvelt, Andrew, Wollenberg, Andreas, Eichenfield, Lawrence F, Zhang, Haixin, Sierka, Debra, Khokhar, Faisal A, Vakil, Jignesh, Shabbir, Arsalan, Marco, Ainara Rodríguez, and Cyr, Sonya L
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Trials and Supportive Activities ,Clinical Research ,Infectious Diseases ,Evaluation of treatments and therapeutic interventions ,6.1 Pharmaceuticals ,Infection ,Good Health and Well Being ,Adult ,Humans ,Dermatitis ,Atopic ,Dermatologic Agents ,Severity of Illness Index ,Treatment Outcome ,Adults ,Atopic dermatitis ,Clinical trials ,Dupilumab ,Infections ,Long-term ,Safety ,Pharmacology and Pharmaceutical Sciences ,General Clinical Medicine ,Clinical sciences ,Pharmacology and pharmaceutical sciences - Abstract
IntroductionPatients with atopic dermatitis (AD) have an increased risk for infections. This open-label extension study, LIBERTY AD OLE, reports the incidence of infections in adults with moderate-to-severe AD treated with dupilumab for up to 4 years.MethodsWe evaluated infections in adults with moderate-to-severe AD treated with dupilumab 300 mg weekly (qw) or every 2 weeks (q2w; approved regimen) for up to 4 years. Topical corticosteroids (TCS) and calcineurin inhibitors (TCI) were permitted. Exposure-adjusted incidence rates (number of patients with at least one event per 100 patient-years [nP/100 PY]) are reported.ResultsOverall, 2677 patients were enrolled and treated with dupilumab: 352 (13.1%) completed up to week 204; 226 patients (8.4%) switched from qw to q2w during the trial. Rates of overall infections (71.27 nP/100 PY), serious and/or severe infections (1.39 nP/100 PY), and infections leading to discontinuation (0.34 nP/100 PY) were consistent with a previous 3-year analysis of this study and low compared with 1-year results in adults with AD treated with placebo + TCS. The cumulative number of patients with treatment-emergent serious or severe infections, non-herpetic or herpetic infections, and total skin infections decreased year-over-year. Limitations included open-label study design with no placebo arm; decreasing sample size at later time points due to sponsor decision to close sites following regulatory approval; qw dosing differs from approved q2w dosing; and patients could use TCS/TCI throughout the study, which may have impacted infection rates.ConclusionsContinuous long-term dupilumab treatment in adults with moderate-to-severe AD is not associated with an increased risk of overall systemic or cutaneous infections.Trial registrationClinicalTrials.gov Identifier: NCT01949311. Video Abstract INFOGRAPHIC.
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- 2023
14. The Validated Investigator Global Assessment for Atopic Dermatitis (vIGA‐AD™): a clinical outcome measure for the severity of atopic dermatitis
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Simpson, Eric L, Bissonnette, Robert, Paller, Amy S, King, Brett, Silverberg, Jonathan I, Reich, Kristian, Thyssen, Jacob P, Doll, Helen, Sun, Luna, DeLozier, Amy M, Nunes, Fabio P, and Eichenfield, Lawrence F
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Research ,Adult ,Azetidines ,Clinical Trials ,Phase III as Topic ,Dermatitis ,Atopic ,Humans ,Outcome Assessment ,Health Care ,Purines ,Pyrazoles ,Reproducibility of Results ,Severity of Illness Index ,Sulfonamides ,Oncology and Carcinogenesis ,Dermatology & Venereal Diseases ,Clinical sciences - Abstract
BackgroundThe validated Investigator Global Assessment for Atopic Dermatitis (vIGA-AD™) is a standardized severity assessment for use in clinical trials and registries for atopic dermatitis (AD).ObjectivesTo investigate the reliability, validity, responsiveness and within-patient meaningful change of the vIGA-AD.MethodsData were analysed from adult patients with moderate-to-severe AD in the BREEZE-AD1 (N = 624 patients; NCT03334396), BREEZE-AD2 (N = 615; NCT03334422) and BREEZE-AD5 (N = 440; NCT03435081) phase III baricitinib clinical studies.ResultsAcross studies, test-retest reliability for stable patients showed moderate-to-good agreement [range of Kappa values for Patient Global Impression of Severity-Atopic Dermatitis (PGI-S-AD), 0·516-0·639; for Eczema Area and Severity Index (EASI), 0·658-0·778]. Moderate-to-large correlations between vIGA-AD and EASI or body surface area (range at baseline, 0·497-0·736; Week 16, 0·716-0·893) supported convergent validity. Known-groups validity was demonstrated vs. EASI and PGI-S-AD (vIGA-AD for severe vs. moderate EASI categories at baseline, P
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- 2022
15. What’s New in Topicals for Atopic Dermatitis?
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Kleinman, Elana, Laborada, Jennifer, Metterle, Lauren, and Eichenfield, Lawrence F
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Biomedical and Clinical Sciences ,Oncology and Carcinogenesis ,2.1 Biological and endogenous factors ,6.1 Pharmaceuticals ,5.1 Pharmaceuticals ,Development of treatments and therapeutic interventions ,Aetiology ,Evaluation of treatments and therapeutic interventions ,Skin ,Administration ,Topical ,Adult ,Calcineurin Inhibitors ,Child ,Dermatitis ,Atopic ,Humans ,Quality of Life ,Clinical Sciences ,Dermatology & Venereal Diseases ,Clinical sciences - Abstract
Atopic dermatitis (AD) is a chronic inflammatory skin condition that can have tremendous impact on quality of life for affected children and adults. First-line therapy for acute management of AD includes topical therapies such as corticosteroids, calcineurin inhibitors, and, more recently, the phosphodiesterase inhibitor crisaborole. Topical agents have remained the mainstay therapy for decades; however, there has been a longstanding need for topical therapies with high efficacy and low risk of adverse effects with long-term use. Given the ongoing advances in understanding the pathogenesis of AD, there are novel targets for pharmacological intervention. We are now in an unprecedented time with more than 40 topical treatments in the pipeline for AD in addition to many developments and treatments on the horizon. This review summarizes selected therapeutic topical agents in later phases of development that target various aspects in the pathogenesis of AD such as Janus kinase inhibition (ruxolitinib and delgocitinib), phosphodiesterase-4 inhibition (roflumilast and difamilast), aryl hydrocarbon modulation (tapinarof), and modulation of the microbiome. We also review novel targeted therapies that are in early phase clinical trials, including AMTX-100, BEN-2293, and PRN473. Preliminary findings on efficacy and tolerability of most of these agents are promising, but further studies are warranted to evaluate the long-term safety and efficacy of these novel agents against the current standard of care.
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- 2022
16. Topical Therapy for Atopic Dermatitis: What is New and the New Paradigm
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Buethe, Maria Gnarra, Kellogg, Caitlyn, Seo, Young Joon, Vuong, Carrie, and Eichenfield, Lawrence F.
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- 2024
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17. Tapinarof cream 1% once daily: Significant efficacy in the treatment of moderate to severe atopic dermatitis in adults and children down to 2 years of age in the pivotal phase 3 ADORING trials
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Silverberg, Jonathan I., Eichenfield, Lawrence F., Hebert, Adelaide A., Simpson, Eric L., Stein Gold, Linda, Bissonnette, Robert, Papp, Kim A., Browning, John, Kwong, Pearl, Korman, Neil J., Brown, Philip M., Rubenstein, David S., Piscitelli, Stephen C., Somerville, Matthew C., Tallman, Anna M., and Kircik, Leon
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- 2024
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18. Topical Management of Pediatric Psoriasis: A Review of New Developments and Existing Therapies
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Lie, Erina, Choi, Mira, Wang, Sheng-Pei, and Eichenfield, Lawrence F.
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- 2023
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19. Dupilumab Safety and Efficacy in a Phase III Open-Label Extension Trial in Children 6–11 Years of Age with Severe Atopic Dermatitis
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Cork, Michael J., Thaçi, Diamant, Eichenfield, Lawrence F., Arkwright, Peter D., Chen, Zhen, Thomas, Ryan B., Kosloski, Matthew P., Dubost-Brama, Ariane, Prescilla, Randy, Bansal, Ashish, and Levit, Noah A.
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- 2023
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20. Managing Childhood and Adolescent Atopic Dermatitis in Primary Care: A US Expert Group Consensus
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Boguniewicz, Mark, Levy, Moise L., Eichenfield, Lawrence F., Lauren, Christine T., Leung, Donald Y.M., Schneider, Lynda C., Siegfried, Elaine C., Tom, Wynnis L., and Paller, Amy S.
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- 2024
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21. Recent Developments and Advances in Atopic Dermatitis: A Focus on Epidemiology, Pathophysiology, and Treatment in the Pediatric Setting
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Eichenfield, Lawrence F, Stripling, Stephen, Fung, Selwyn, Cha, Amy, O’Brien, Andryann, and Schachner, Lawrence A
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Biomedical and Clinical Sciences ,Clinical Sciences ,Pediatric ,Clinical Research ,Eczema / Atopic Dermatitis ,Skin ,Child ,Chronic Disease ,Dermatitis ,Atopic ,Humans ,Paediatrics and Reproductive Medicine ,Pharmacology and Pharmaceutical Sciences ,Pediatrics ,Paediatrics ,Pharmacology and pharmaceutical sciences - Abstract
Atopic dermatitis (AD) is a chronic inflammatory skin disorder that affects a substantial number of children and has a significant negative impact on affected patients and their caregivers/families. Recent studies have led to significant evolutions in the understanding of AD pathogenesis, epidemiology, and treatment. The first point of contact for many patients with new-onset AD is usually with their primary care provider or pediatrician. This underscores the importance for pediatricians to understand the basic pathophysiology and current standards of care for AD. This article provides up-to-date information and reviews the basic principles of AD pathophysiology, diagnosis, and management. In addition, the article highlights recent advances in scientific research regarding the mechanisms involved in the pathogenesis of atopic dermatitis that have resulted in the discovery of novel therapeutic targets and the development of targeted biologic therapies with the potential to revolutionize AD therapy.
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- 2022
22. Real-World Effectiveness of Dupilumab in Atopic Dermatitis Patients: Analysis of an Electronic Medical Records Dataset
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Eichenfield, Lawrence F, Armstrong, April, Guttman-Yassky, Emma, Lio, Peter A, Chen, Chi-Chang, Hines, Dionne M, McGuiness, Catherine B, Ganguli, Sohini, Delevry, Dimittri, Sierka, Debra, and Mallya, Usha G
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Biomedical and Clinical Sciences ,Clinical Sciences ,Aging ,Clinical Research ,Brain Disorders ,Evaluation of treatments and therapeutic interventions ,6.1 Pharmaceuticals ,Good Health and Well Being ,Atopic dermatitis ,Body surface area affected ,Dupilumab ,Investigator global assessment ,Itch ,Real-world effectiveness ,Clinical sciences - Abstract
IntroductionWhile the efficacy of dupilumab for the treatment of adults with moderate-to-severe atopic dermatitis (AD) has been demonstrated in several clinical trials, patients in such trials may not necessarily reflect the real-world clinical practice setting. This study evaluated the real-world effectiveness of dupilumab in adults with moderate-to-severe AD based on physician global assessment, percent body surface area affected, and patient-reported itch.MethodsFrom Modernizing Medicine's Electronic Medical Assistant dermatology-specific electronic medical records, adults (≥ 18 years) were identified with a diagnosis of AD and ≥ 1 dupilumab prescription (index event) between 1 April 2017 and 31 January 2019. Three cohorts were identified based on 3-month pre-index (1) Investigator Global Assessment (IGA) score ≥ 3, (2) an itch severity numerical rating scale (NRS) score ≥ 3, and (3) body surface area (BSA) affected ≥ 10%. Changes from pre-index on the outcome within each cohort were evaluated at 4 months post-index. Patients were also stratified for evaluation of outcomes by baseline demographic (sex, age) and prior AD treatments (topical therapy only or no treatment, any systemic therapy).ResultsMore than 70% of the 435 AD patients with baseline IGA score ≥ 3 improved to an IGA score of ≤ 2 at month 4 post-dupilumab initiation, including 42.8% who achieved IGA 0/1 (clear/minimal). Among 112 patients with a pre-index itch severity NRS ≥ 3, scores were reduced from mean (SD) 7.0 (2.4) pre-index to 2.8 (2.8) at month 4 (p
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- 2022
23. Once-Daily Crisaborole Ointment, 2%, as a Long-Term Maintenance Treatment in Patients Aged ≥ 3 Months with Mild-to-Moderate Atopic Dermatitis: A 52-Week Clinical Study
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Eichenfield, Lawrence F., Gower, Richard G., Xu, JinHua, Alam, Maryam S., Su, John C., Myers, Daniela E., Sanders, Paul, Vlahos, Bonnie, Zang, Chuanbo, Lan, Jar, and Werth, John
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- 2023
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24. Risk factors and outcomes of melanoma in children and adolescents: A retrospective multicenter study
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Hawryluk, Elena B., Moustafa, Danna, Barry, Kelly K., Bahrani, Eman, Reusch, Diana B., Brahmbhatt, Meera, Chen, Lily, Coughlin, Carrie C., Gerami, Pedram, Haddock, Ellen, Hook, Kristen, Humphrey, Stephen R., Kao, Pei-Chi, Kruse, Lacey L., Lawley, Leslie P., Mansour, Danny, Marghoob, Ashfaq A., Nguyen, Julie, Phung, Thuy L., Pope, Elena, Raisanen, Tom, Robinson, Sarah, Rogers, Tova, Schmidt, Birgitta, Tran, Gary, Travis, Kate, Wolner, Zachary, London, Wendy B., Eichenfield, Lawrence F., and Huang, Jennifer
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- 2024
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25. Executive summary: Guidelines of care for the management of atopic dermatitis in adults with phototherapy and systemic therapies
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Davis, Dawn M.R., Drucker, Aaron M., Alikhan, Ali, Bercovitch, Lionel, Cohen, David E., Darr, Jennifer M., Eichenfield, Lawrence F., Frazer-Green, Lindsy, Paller, Amy S., Schwarzenberger, Kathryn, Silverberg, Jonathan I., Singh, Anne Marie, Wu, Peggy A., and Sidbury, Robert
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- 2024
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26. Guidelines of care for the management of atopic dermatitis in adults with phototherapy and systemic therapies
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Davis, Dawn M.R., Drucker, Aaron M., Alikhan, Ali, Bercovitch, Lionel, Cohen, David E., Darr, Jennifer M., Eichenfield, Lawrence F., Frazer-Green, Lindsy, Paller, Amy S., Schwarzenberger, Kathryn, Silverberg, Jonathan I., Singh, Anne Marie, Wu, Peggy A., and Sidbury, Robert
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- 2024
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27. Psychometric properties of the itch numeric rating scale, skin pain numeric rating scale, and atopic dermatitis sleep scale in adult patients with moderate-to-severe atopic dermatitis
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Silverberg, Jonathan I, DeLozier, Amy, Sun, Luna, Thyssen, Jacob P, Kim, Brian, Yosipovitch, Gil, Nunes, Fabio P, Gugiu, P Cristian, Doll, Helen A, and Eichenfield, Lawrence F
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Health Services and Systems ,Public Health ,Health Sciences ,Pain Research ,Neurosciences ,Clinical Research ,Chronic Pain ,Adult ,Dermatitis ,Atopic ,Humans ,Pain ,Psychometrics ,Quality of Life ,Reproducibility of Results ,Severity of Illness Index ,Sleep ,Atopic dermatitis ,Atopic dermatitis sleep scale ,Convergent-divergent validity ,Itch NRS ,Numeric rating scale ,Patient-reported outcome ,Psychometric ,Reliability ,Responsiveness ,Skin pain NRS ,Validity ,Public Health and Health Services ,Health Policy & Services ,Health services and systems ,Public health - Abstract
BackgroundThe Itch Numeric Rating Scale (NRS), Skin Pain NRS, and Atopic Dermatitis Sleep Scale (ADSS) are self-administered patient-reported outcome (PRO) instruments developed to assess symptoms in patients with atopic dermatitis (AD). The objective of this study was to evaluate the psychometric properties (reliability, validity, and responsiveness) and interpretability thresholds of these PROs using data from three pivotal Phase 3 studies in adults.MethodsBREEZE-AD1, BREEZE-AD2, and BREEZE-AD5 evaluated the safety and efficacy of baricitinib in adults with moderate-to-severe AD. Clinician-reported outcomes and other PROs commonly assessed in patients with AD were used to estimate meaningful changes and evaluate test-retest reliability, convergent and divergent validity, known-groups validity, responsiveness, and meaningful change thresholds (MCTs) of the Itch NRS, Skin Pain NRS, and ADSS.ResultsThe test-retest reliability of the Itch NRS, Skin Pain NRS, and ADSS was evidenced by generally large intraclass correlation coefficients (> 0.7) in stable groups of patients between baseline and Week 1 and Weeks 4 and 8. Moderate-to-large correlations (r > 0.4) at baseline and Week 16 were generally observed between each measure and other PROs measuring the same concept, supporting convergent validity. Small-to-moderate correlations with clinician-reported outcomes demonstrated divergent validity. Each instrument was able to distinguish between known groups of disease severity as assessed using other indicators of AD severity. The responsiveness of the Itch NRS, Skin Pain NRS, and ADSS scales was demonstrated through significant differences in their change scores from baseline to Week 16 between categories of change in another PRO also from baseline to Week 16. Thresholds for interpreting meaningful change were estimated as - 4.0 for the 0-10 Itch and Skin Pain NRS items; - 1.25 for the 0-4 ADSS Items 1 and 3 and; - 1.50 for the 0-29 ADSS Item 2, these equivalent to moderate degrees of change.ConclusionsResults of this study demonstrate that the psychometric properties of the Itch NRS, Skin Pain NRS, and ADSS are good to excellent. These findings support the use of these instruments in daily assessment of AD symptoms in adults with moderate-to-severe AD. Trial registration ClinicalTrials.gov numbers: NCT03334396, NCT03334422, and NCT03435081.
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- 2021
28. Safety and Efficacy of VP-102 (Cantharidin, 0.7% w/v) in Molluscum Contagiosum by Body Region: Post hoc Pooled Analyses from Two Phase III Randomized Trials.
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Eichenfield, Lawrence F, Kwong, Pearl, Gonzalez, Mercedes E, Yan, Albert, D'Arnaud, Pieter, Burnett, Patrick, and Olivadoti, Melissa
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Trials and Supportive Activities ,Clinical Research ,Child ,VP-102 ,cantharidin ,incidence ,infectious disease ,lesion ,molluscum ,molluscum contagiosum ,pediatric ,sensitive skin ,topical - Abstract
Trial registration>ClinicalTrials.gov identifier nos. NCT03377790 (for CAMP-1) and NCT03377803 (for CAMP-2).BackgroundVP-102 is drug-device combination product containing cantharidin (0.7% w/v) and has undergone Phase III clinical trials for the treatment of molluscum contagiosum (molluscum). Efficacy and safety may differ by body region due to variable skin anatomy.ObjectiveWe investigated the pooled safety and efficacy of VP-102 by affected body region.MethodsIndividuals at least two years of age with molluscum were randomized to topical VP-102 or vehicle once every 21 days until clear (maximum of four applications). Participants were assigned to body region groups where lesions were present at baseline. Body region lesion counts were recorded at each visit. Efficacy was measured by the percentage of participants with complete clearance of lesions by region. Pre-specified adverse events (AEs) were analyzed for those treated in the region on that visit.ResultsParticipants had a mean of two regions affected at baseline. Complete clearance was significantly higher in the VP-102-treated group than with vehicle application in all regions at the last visit (P
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- 2021
29. Approach to Mycosis Fungoides in children: Consensus-based recommendations
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Zvulunov, Alex, Neale, Holly, Stern, Jonah, Santaguida, Pasqualina, Stein, Amy Buros, Koh, Mark, Eichenfield, Lawrence F., Guitart, Joan, Goebeler, Matthias, Scarisbrick, Julia, Willemze, Rein, Coughlin, Carrie C., George, Renu, Brazzelli, Valeria, Marschalkó, Márta, Belousova, Irena, Querfeld, Christiane, Bagot, Martine, Szepietowski, Jacek C., Papadavid, Evangelina, Quaglino, Pietro, Hoeger, Peter, Ortiz-Romero, Pablo L., Nikolaou, Vasiliki, Dummer, Reinhard, Aung, Phyu P., Lawley, Leslie, Morel, Kimberly D., Ngan, Bo, Wain, Mary, Gameiro, Ana, Lacy-Niebla, Rosa María, and Pope, Elena
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- 2024
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30. Therapeutic education in atopic dermatitis: A position paper from the International Eczema Council
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Eichenfield, Lawrence F, Kusari, Ayan, Han, Allison M, Barbarot, Sébastien, Deleuran, Mette, Lio, Peter, Marcoux, Danielle, Nosbaum, Audrey, and Stalder, Jean-Francois
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Prevention ,Skin ,AD ,atopic dermatitis ,EAP ,eczema action plan ,IEC ,International Eczema Council ,QOL ,quality of life ,TPE ,therapeutic patient education ,atopic dermatitis ,corticosteroids ,e-learning ,eczema ,eczema action plan ,pruritus ,quality of life ,therapeutic education ,therapeutic patient education - Abstract
BackgroundAtopic dermatitis (AD) is a chronic, inflammatory skin disease that affects as many as 12.5% of children aged 0-17 years and 3% of the adult population. In the United States, 31.6 million children and adults are estimated to be living with AD.ObjectiveTherapeutic patient education (TPE) has proven its value in the management of chronic diseases for which adherence to therapy is suboptimal. This article explores experts' opinions and treatment practices to determine if TPE is a recommended and effective method for treating AD.MethodsForty-two (51%) of 82 Councilors and Associates of the International Eczema Council (IEC), an international group with expertise in AD, responded to an electronic survey on TPE and AD.ResultsMost respondents (97.5%) agreed that TPE should play an important role in the management of AD. Many respondents (82.9%) believed that all patients with AD, regardless of disease severity, could benefit from TPE.LimitationsThe International Eczema Council survey lacks specific information on AD severity.ConclusionsPublications have shown the positive effect of TPE on the course of the disease, the prevention of complications, and the autonomy and quality of patient life. Survey respondents agreed that TPE can improve the quality of patient care and patient satisfaction with care.
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- 2021
31. Clindamycin phosphate 1.2%/adapalene 0.15%/benzoyl peroxide 3.1% gel for moderate-to-severe acne: Efficacy and safety results from two randomized phase 3 trials
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Stein Gold, Linda, Lain, Edward, Del Rosso, James Q., Gold, Michael, Draelos, Zoe D., Eichenfield, Lawrence F., Sadick, Neil, Werschler, William P., Gooderham, Melinda J., and Lupo, Mary
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- 2023
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32. DMT310, a novel once-weekly topical treatment for patients with moderate-to-severe acne vulgaris: Results of a phase 2b randomized, double-blind, placebo-controlled trial
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Armas, E., DeValle, O., Haber, R.S., Jones, T., Kempers, S.E., Knoepp, T.G., Kuttner, B.J., Lieberman, R., Miller, M.L., Stewart, D.M., Weinberg, J., Eichenfield, Lawrence F., DuBois, Janet C., Gold, Michael H., Nardo, Christopher J., and Draelos, Zoe D.
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- 2023
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33. Pooled Results of Two Randomized Phase III Trials Evaluating VP-102, a Drug-Device Combination Product Containing Cantharidin 0.7% (w/v) for the Treatment of Molluscum Contagiosum
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Eichenfield, Lawrence F, Siegfried, Elaine, Kwong, Pearl, McBride, Mark, Rieger, Jayson, Glover, David, Willson, Cynthia, Davidson, Matthew, Burnett, Patrick, and Olivadoti, Melissa
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Trials and Supportive Activities ,Clinical Research ,Patient Safety ,6.1 Pharmaceuticals ,Evaluation of treatments and therapeutic interventions ,Administration ,Cutaneous ,Adolescent ,Cantharidin ,Child ,Child ,Preschool ,Double-Blind Method ,Equipment Design ,Erythema ,Humans ,Irritants ,Male ,Molluscum Contagiosum ,Pain ,Pruritus ,Severity of Illness Index ,Treatment Outcome ,Young Adult ,Dermatology & Venereal Diseases ,Clinical sciences - Abstract
BackgroundCompounded cantharidin has been used for decades to treat molluscum contagiosum but lacks rigorous clinical evidence to support its safety and efficacy. VP-102 is a shelf-stable drug-device combination product that contains topical cantharidin (0.7% weight/volume [w/v]) and is being evaluated for the treatment of molluscum.ObjectivesOur objective was to present pooled safety and efficacy analyses of VP-102 in the treatment of molluscum compared with vehicle.MethodsParticipants aged ≥ 2 years were randomized 3:2 to topical administration of VP-102 or vehicle in two randomized, double-blind, vehicle-controlled phase III trials. Study drug was applied to all baseline and new lesions once every 21 days until clear or for a maximum of four applications. Assessors blinded to treatment counted all lesions at each study visit. All adverse events (AEs) were documented. Data were pooled for analyses.ResultsIn total, 310 participants received VP-102 and 218 received vehicle. Mean age was 7.5 years (range 2-60) for VP-102 and 6.8 (2-54) for vehicle. Complete clearance of all molluscum lesions at day 84 occurred in 50% of VP-102 participants and 15.6% of vehicle recipients (p
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- 2021
34. Prevalence and burden of atopic dermatitis involving the head, neck, face, and hand: A cross sectional study from the TARGET-DERM AD cohort
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Silverberg, Jonathan I., Simpson, Brenda, Abuabara, Katrina, Guttman-Yassky, Emma, Calimlim, Brian, Wegzyn, Colleen, Krueger, Whitney, Gamelli, Amy, Munoz, Breda, Faller, Rachel W., Crawford, Julie M., Grada, Ayman, and Eichenfield, Lawrence F.
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- 2023
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35. Characterization of wound microbes in epidermolysis bullosa: Results from the epidermolysis bullosa clinical characterization and outcomes database
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Levin, Laura E, Shayegan, Leila H, Lucky, Anne W, Hook, Kristen P, Bruckner, Anna L, Feinstein, James A, Whittier, Susan, Lauren, Christine T, Pope, Elena, Lara‐Corrales, Irene, Wiss, Karen, McCuaig, Catherine C, Powell, Julie, Eichenfield, Lawrence F, Levy, Moise L, Diaz, Lucia, Glick, Sharon A, Paller, Amy S, Price, Harper N, Browning, John C, and Morel, Kimberly D
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Biomedical and Clinical Sciences ,Clinical Sciences ,Emerging Infectious Diseases ,Biodefense ,Infectious Diseases ,Prevention ,Vaccine Related ,Antimicrobial Resistance ,Clinical Research ,Infection ,Anti-Bacterial Agents ,Canada ,Epidermolysis Bullosa ,Humans ,Mupirocin ,Retrospective Studies ,Staphylococcal Infections ,Staphylococcus aureus ,cultures ,epidermolysis bullosa ,microbes ,resistance ,wound ,Paediatrics and Reproductive Medicine ,Dermatology & Venereal Diseases ,Clinical sciences ,Paediatrics - Abstract
Background/objectivesPatients with epidermolysis bullosa (EB) require care of wounds that are colonized or infected with bacteria. A subset of EB patients are at risk for squamous cell carcinoma, and bacterial-host interactions have been considered in this risk. The EB Clinical Characterization and Outcomes Database serves as a repository of information from EB patients at multiple centers in the United States and Canada. Access to this resource enabled broad-scale analysis of wound cultures.MethodsA retrospective analysis of 739 wound cultures from 158 patients from 13 centers between 2001 and 2018.ResultsOf 152 patients with a positive culture, Staphylococcus aureus (SA) was recovered from 131 patients (86%), Pseudomonas aeruginosa (PA) from 56 (37%), and Streptococcus pyogenes (GAS) from 34 (22%). Sixty-eight percent of patients had cultures positive for methicillin-sensitive SA, and 47%, methicillin-resistant SA (18 patients had cultures that grew both methicillin-susceptible and methicillin-resistant SA at different points in time). Of 15 patients with SA-positive cultures with recorded mupirocin susceptibility testing, 11 had mupirocin-susceptible SA and 6 patients mupirocin-resistant SA (2 patients grew both mupirocin-susceptible and mupirocin-resistant SA). SCC was reported in 23 patients in the entire database, of whom 10 had documented wound cultures positive for SA, PA, and Proteus species in 90%, 50%, and 20% of cases, respectively.ConclusionsSA and PA were the most commonly isolated bacteria from wounds. Methicillin resistance and mupirocin resistance were reported in 47% and 40% of patients tested, respectively, highlighting the importance of ongoing antimicrobial strategies to limit antibiotic resistance.
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- 2021
36. Consensus recommendations for the use of retinoids in ichthyosis and other disorders of cornification in children and adolescents
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Zaenglein, Andrea L, Levy, Moise L, Stefanko, Nicole S, Benjamin, Latanya T, Bruckner, Anna L, Choate, Keith, Craiglow, Brittany G, DiGiovanna, John J, Eichenfield, Lawrence F, Elias, Peter, Fleckman, Philip, Lawley, Leslie P, Lewis, Richard A, Lucky, Anne W, Mathes, Erin F, Milstone, Leonard M, Paller, Amy S, Patel, Sonali S, Siegel, Dawn H, Teng, Joyce, Tanumihardjo, Sherry A, Thaxton, Lauren, Williams, Mary L, and Group, PeDRA Use of Retinoids in Ichthyosis Work
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Paediatrics ,Biomedical and Clinical Sciences ,Clinical Sciences ,Prevention ,Clinical Research ,Pediatric ,Good Health and Well Being ,Adolescent ,Child ,Consensus ,Humans ,Ichthyosis ,Ichthyosis ,Lamellar ,Retinoids ,retinoid ,ichthyosis ,disorder of cornification ,systemic therapy ,topical therapy ,adverse drug effects ,drug monitoring ,safety monitoring ,bone health ,hyperlipidemia ,ectropion ,contraception ,iPLEDGE ,depression ,quality of life ,PeDRA Use of Retinoids in Ichthyosis Work Group ,Paediatrics and Reproductive Medicine ,Dermatology & Venereal Diseases ,Clinical sciences - Abstract
Topical and systemic retinoids have long been used in the treatment of ichthyoses and other disorders of cornification. Due to the need for long-term use of retinoids for these disorders, often beginning in childhood, numerous clinical concerns must be considered. Systemic retinoids have known side effects involving bone and eye. Additionally, potential psychiatric and cardiovascular effects need to be considered. Contraceptive concerns, as well as the additive cardiovascular and bone effects of systemic retinoid use with hormonal contraception must also be deliberated for patients of childbearing potential. The Pediatric Dermatology Research Alliance (PeDRA) Use of Retinoids in Ichthyosis Work Group was formed to address these issues and to establish best practices regarding the use of retinoids in ichthyoses based on available evidence and expert opinion.
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- 2021
37. International observational atopic dermatitis cohort to follow natural history and treatment course: TARGET-DERM AD study design and rationale.
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Abuabara, Katrina, Silverberg, Jonathan I, Simpson, Eric L, Paller, Amy S, Eichenfield, Lawrence F, Bissonnette, Robert, Krueger, James, Harris, John E, Dalfonso, Laura, Watkins, Stephanie E, Crawford, Julie M, Thaçi, D, and Guttman-Yassky, Emma
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eczema ,medical history ,statistics & research methods ,therapeutics ,statistics & ,research methods ,Clinical Sciences ,Public Health and Health Services ,Other Medical and Health Sciences - Abstract
IntroductionAs new topical and systemic treatments become available for atopic dermatitis (AD), there is a need to understand how treatments are being used in routine clinical practice, their comparative effectiveness and their long-term safety in diverse clinical settings.Methods and analysisThe TARGET-DERM AD cohort is a longitudinal, observational study of patients with AD of all ages, designed to provide practical information on long-term effectiveness and safety unobtainable in traditional registration trials. Patients with physician-diagnosed AD receiving prescription treatment (topical or systemic) will be enrolled at academic and community clinical centres. Up to 3 years of retrospective medical records, 5 years of prospective medical records, and optional biological samples and patient-reported outcomes will be collected. The primary aims include characterisation of AD treatment regimens, evaluation of response to therapy, and description of adverse events.Ethics and disseminationTARGET-DERM has been approved by a central IRB (Copernicus Group IRB, 5000 Centregreen Way Suite 200, Cary, North Carolina 27513) as well as local and institutional IRBs. No additional Ethics Committee reviews. Results will be reviewed by a publications committee and submitted to peer-reviewed journals.Trial registration numberNCT03661866, pre-results.
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- 2020
38. Improvement in disease severity and pruritus outcomes with crisaborole ointment, 2%, by baseline atopic dermatitis severity in children and adolescents with mild‐to‐moderate atopic dermatitis
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Eichenfield, Lawrence F, Yosipovitch, Gil, Gold, Linda F Stein, Kalabis, Mizuho, Zang, Chuanbo, Vlahos, Bonnie, Sanders, Paul, Myers, Daniela E, Bushmakin, Andrew G, Cappelleri, Joseph C, Olivadoti, Melissa, and Paller, Amy S
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Research ,Pediatric ,Adolescent ,Boron Compounds ,Bridged Bicyclo Compounds ,Heterocyclic ,Child ,Child ,Preschool ,Dermatitis ,Atopic ,Double-Blind Method ,Humans ,Ointments ,Pruritus ,Severity of Illness Index ,Treatment Outcome ,atopic dermatitis ,pruritus ,therapy-topical ,Paediatrics and Reproductive Medicine ,Dermatology & Venereal Diseases ,Clinical sciences ,Paediatrics - Abstract
Background/objectivesCrisaborole ointment, 2%, is a nonsteroidal phosphodiesterase 4 inhibitor for the treatment of mild-to-moderate atopic dermatitis (AD). This pooled post hoc analysis of two phase 3 trials (NCT02118766, NCT02118792) assessed improvement and time to improvement in Investigator's Static Global Assessment (ISGA) and Severity of Pruritus Scale (SPS) outcomes in pediatric patients with mild-to-moderate AD.MethodsPatients aged ≥2 years were randomly assigned 2:1 to receive twice-daily crisaborole or vehicle for 28 days. Patients aged 2-17 years were pooled for this analysis. Proportions of patients and time to achieving ISGA success (clear [0] or almost clear [1] with ≥2-grade improvement from baseline), ISGA clear/almost clear, ≥1-grade improvement in ISGA, SPS success (SPS score ≤1 with ≥1-grade improvement), or ≥1-grade improvement in SPS score were analyzed and stratified by baseline ISGA.ResultsAt first postbaseline assessment (day 8), significantly higher proportions of crisaborole- than vehicle-treated patients achieved ISGA success, ISGA clear/almost clear, ≥1-grade ISGA improvement, SPS success, or ≥1-grade improvement in SPS regardless of baseline ISGA. Differences were significantly greater over time for all outcomes for patients with moderate baseline ISGA and numerically greater for those with mild baseline ISGA. Median times to ISGA and SPS outcomes were shorter for crisaborole versus vehicle.ConclusionImprovement in ISGA and SPS outcomes were observed with crisaborole in pediatric patients with mild-to-moderate baseline AD.
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- 2020
39. Guidelines of care for the management of atopic dermatitis in adults with topical therapies
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Sidbury, Robert, Alikhan, Ali, Bercovitch, Lionel, Cohen, David E., Darr, Jennifer M., Drucker, Aaron M., Eichenfield, Lawrence F., Frazer-Green, Lindsy, Paller, Amy S., Schwarzenberger, Kathryn, Silverberg, Jonathan I., Singh, Anne Marie, Wu, Peggy A., and Davis, Dawn M.R.
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- 2023
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40. Costs and Treatment Patterns Among Patients with Atopic Dermatitis Using Advanced Therapies in the United States: Analysis of a Retrospective Claims Database
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Eichenfield, Lawrence F, DiBonaventura, Marco, Xenakis, Jason, Lafeuille, Marie-Helene, Duh, Mei Sheng, Fakih, Iman, Levenberg, Mark, Cappelleri, Joseph C, and Sikirica, Vanja
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Biomedical and Clinical Sciences ,Clinical Sciences ,Clinical Research ,6.1 Pharmaceuticals ,Evaluation of treatments and therapeutic interventions ,Good Health and Well Being ,Atopic dermatitis ,Corticosteroids ,Costs ,Dupilumab ,Immunosuppressants ,Phototherapy ,Clinical sciences - Abstract
IntroductionFor many, atopic dermatitis (AD) is not adequately controlled with topical regimens. This analysis examined treatment using advanced therapies and associated costs.MethodsThe IQVIA Health Plan Claims data set was analyzed. Patients aged ≥ 12 years with AD who newly initiated advanced therapy after the availability of dupilumab (March 28, 2017) and had ≥ 6 months continuous enrollment before and after their first advanced therapy claim (index date) were included. Advanced therapies included dupilumab, systemic corticosteroids (SCSs), systemic immunosuppressants (SISs), and phototherapy. A multivariate regression model was used to predict annualized follow-up healthcare costs.ResultsIn total, 1980 patients were included (61.1% female; mean age, 41.2 years [SD, 17.4]; 11.3%
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- 2020
41. CONSENSUS STATEMENT FOR TREATMENT OF PORT WINE BIRTHMARKS IN STURGE-WEBER SYNDROME
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Sabeti, Sara, Burkhart, Craig, Eichenfield, Lawrence F, Faith, Esteban Fernandez, Frieden, Ilona J, Geronemus, Roy G, Gupta, Deepti, Krakowski, Andrew C, Levy, Moise L, Metry, Denise, Nelson, J Stuart, Tollefson, Megha, and Kelly, Kristen M
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Clinical Sciences ,Dermatology & Venereal Diseases - Published
- 2020
42. Diaper dermatitis prevalence and severity: Global perspective on the impact of caregiver behavior
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Carr, Andrew N, DeWitt, Thomas, Cork, Michael J, Eichenfield, Lawrence F, Fölster‐Holst, Regina, Hohl, Daniel, Lane, Alfred T, Paller, Amy, Pickering, Larry, Taieb, Alain, Cui, Tao Y, Xu, Zi G, Wang, Xeumin, Brink, Susanna, Niu, Yeuqing, Ogle, Julie, Odio, Mauricio, and Gibb, Roger D
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Pediatric ,Clinical Research ,Skin ,Buttocks ,Caregivers ,China ,Cross-Sectional Studies ,Diaper Rash ,Diapers ,Infant ,Female ,Germany ,Humans ,Hydrogen-Ion Concentration ,Infant ,Infant Care ,Male ,Prevalence ,Surveys and Questionnaires ,United States ,diaper dermatitis ,neonatal ,skin barrier ,Paediatrics and Reproductive Medicine ,Dermatology & Venereal Diseases - Abstract
ObjectivesTo compare prevalence and severity of diaper dermatitis (DD) in infants and toddlers (babies) across three countries (China, USA, and Germany), including diapered skin measures and caregiver practices.MethodsA cross-sectional study of 1791 babies (~600 from each country) was recruited at each clinical site. Based on regional toilet-training habits, exclusively diaper-wearing infants were recruited between ages 2-8 months in China and 2-18 months in the USA and Germany. DD was measured, as well as skin pH, transepidermal water loss (TEWL), and relative humidity (RH) in the diapered region. Caregiver habits were collected via a questionnaire and included information on hygienic practices.ResultsDiaper dermatitis was highest in the perianal area, followed by the intertriginous, genital, and buttock regions. In general, DD was significantly lower in babies in China, highest in Germany, and intermediate in the USA. This rank ordering of DD by geography was also observed in baby age 2-8 months. The lower DD observed in China was associated with lower skin pH and TEWL on diapered skin and decreased RH in the diaper. Chinese caregivers had the highest rate of prophylactic topical product usage, the most robust cleaning of the diapered area, lack of cleansing after urine-only diaper changes, and Chinese infants spent the least time in an overnight diaper.ConclusionsThese data suggest caregiver behaviors including prophylactic use of topical products, thorough cleaning after stooling and reduced time in an overnight diaper are associated with less DD, lower superficial skin pH, and enhanced skin barrier.
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- 2020
43. Exploring content and psychometric validity of newly developed assessment tools for itch and skin pain in atopic dermatitis
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Newton, Louise, DeLozier, Amy M, Griffiths, Philip C, Hill, Jennifer N, Hudgens, Stacie, Symonds, Tara, Gable, Jonathon C, Paik, Jim, Wyrwich, Kathleen W, Eichenfield, Lawrence F, Abetz-Webb, Linda, and Silverberg, Jonathan I
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Biomedical and Clinical Sciences ,Clinical Sciences ,Health Sciences ,Neurosciences ,Chronic Pain ,Clinical Research ,Pain Research ,Skin ,Adolescents ,Adults ,Atopic dermatitis ,Clinical outcomes assessment ,Health-related quality of life ,Itch ,Itch NRS ,Patient-reported outcomes ,Skin pain ,Skin pain NRS ,Biomedical and clinical sciences ,Health sciences - Abstract
BackgroundAtopic dermatitis (AD) is a common skin disorder characterized by chronic inflammation, altered skin barrier function, and inflammatory cell skin infiltration that decreases health-related quality of life (HRQoL). The study objective was to understand the patient perspective of AD burden and determine suitable patient-reported outcome (PRO) measures.MethodsThis mixed methods study involved the collection of qualitative and quantitative information from adults (≥ 18 years old) and adolescents (12 - 17 years old) with clinician-confirmed AD regarding their experiences of AD symptoms and its impact on HRQoL. The first part of the study included three stages: in-person concept elicitation (CE) interviews, a 2-week daily electronic diary (eDiary) study, and in-person cognitive debriefing (CD) interviews. An Itch numeric rating scale (NRS) (v1.0) and a Skin Pain NRS (v1.0) evaluation during CD interviews required participants to think about their 'worst' itch and 'worst' skin pain in the past 24 h. Other PRO measures allowed for psychometric testing. The second part of the study involved telephone-depth interviews (TDIs) and qualitative feedback from participants who had not participated in the CD interviews. Qualitative data were thematically analyzed. Psychometric evaluation of NRS measures was performed using eDiary data.ResultsIn the CE interviews, itch and/or itching and skin pain were the most prevalent symptoms consistently discussed by participants. Both NRS measures demonstrated strong psychometric reliability and were applicable across ages with suitable concurrent validity. During the CD interviews, some participants focused their answers on their 'average' itch/itching in the past 24 h, rather than their 'worst' itch. Some participants answered the Skin Pain NRS thinking about general pain or other types of pain, rather than skin pain specifically. Consequently, modifications to both measures addressed these issues and re-tested as paper-and-pen versions in subsequent TDIs. Itch NRS (v2.0) modifications helped participants focus on their worst itching. Most participants preferred Skin Pain NRS v2.0b, which included skin pain descriptors.ConclusionsItching and skin pain are the most important and relevant AD symptoms. The Itch NRS (v2.0) and Skin Pain NRS (v2.0b) appear to be appropriate endpoints for the assessment of itching and skin pain severity for clinical trials with adults and adolescents with AD.
- Published
- 2019
44. Purpura
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Eichenfield, Dawn Z., primary and Eichenfield, Lawrence F., additional
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- 2023
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45. Therapeutic Guideline Overview
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Bhatti, Safiyyah, primary, Tracy, Alexis, additional, and Eichenfield, Lawrence F., additional
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- 2023
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46. Contributors
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Abzug, Mark J., primary, Adderson, Elisabeth E., additional, Agarwal, Aastha, additional, Agwu, Allison L., additional, Albenberg, Lindsey, additional, Albert, Jonathan, additional, Alby, Kevin, additional, Aldrovandi, Grace M., additional, Allen, Upton D., additional, Alvarez-Hernndez, Gerardo, additional, Ampofo, Krow, additional, Anderson, Evan J., additional, Appiah, Grace D., additional, Ardura, Monica I., additional, Arnon, Stephen S., additional, Aronson, Naomi E., additional, Arvin, Ann M., additional, Ashkenazi, Shai, additional, Ashkenazi-Hoffnung, Liat, additional, Asturias, Edwin J., additional, Aukstuolis, Kestutis, additional, Badalyan, Vahe, additional, Baker, Carol J., additional, Balakrishnan, Karthik, additional, Barnett, Elizabeth D., additional, Bechtel, Kirsten, additional, Benitz, William E., additional, Berkovich, Rachel, additional, Berman, David M., additional, Bialek, Stephanie R., additional, Bijker, Else M., additional, Bizzarro, Matthew J., additional, Bloch, Karen C., additional, Bocchini, Joseph A., additional, Boyce, Thomas G., additional, Bradley, John S., additional, Bratcher, Denise F., additional, Braverman, Paula K., additional, Brook, Itzhak, additional, Brown, Kevin Edward, additional, Bryant, Kristina P., additional, Camacho-Gonzalez, Andres F., additional, Caete-Gibas, Connie F., additional, Cantey, Joseph B., additional, Cantey, Paul, additional, Cardemil, Cristina V., additional, Caserta, Mary T., additional, Castagnini, Luis A., additional, Cataldi, Jessica R., additional, Chadwick, Ellen Gould, additional, Chancey, Rebecca J., additional, Cherry, Cara C., additional, Chiang, Silvia S., additional, Choi, Mary, additional, Christenson, John C., additional, Coffin, Susan E., additional, Cohn, Amanda, additional, Contopoulos-Ioannidis, Despina G., additional, Conway, James H., additional, Cortese, Margaret M., additional, Creech, C. Buddy, additional, Crews, Jonathan D., additional, Curtis, Donna, additional, Curtis, Nigel, additional, Danziger-Isakov, Lara A., additional, Darville, Toni, additional, Dasch, Gregory A., additional, Daskalaki, Irini, additional, Davies, H. Dele, additional, Dawood, Fatimah S., additional, Day, J. Christopher, additional, Teresa de la Morena, M., additional, DeMuri, Gregory P., additional, Despommier, Dickson D., additional, Dodson, Daniel S., additional, Dolgner, Stephen J., additional, Dunn, Clinton, additional, Dyal, Jonathan, additional, Edwards, Kathryn M., additional, Edwards, Morven S., additional, Eichenfield, Dawn Z., additional, Eichenfield, Lawrence F., additional, Elston, Dirk M., additional, Emerson, Beth, additional, Enane, Leslie A., additional, Ephros, Moshe, additional, Erdem, Guliz, additional, Eremeeva, Marina E., additional, Esposito, Douglas H., additional, Farley, Monica M., additional, Feingold, Anat R., additional, Feja, Kristina N., additional, Finn, Adam, additional, Fischer, Marc, additional, Fisher, Brian T., additional, Fisher, Randall G., additional, Flynn, Patricia Michele, additional, Foster, Monique A., additional, Fox, LeAnne M., additional, Frank, Michael M., additional, Fredrick, Douglas R., additional, Frenck, Robert W., additional, Gaensbauer, James, additional, Gans, Hayley A., additional, Gauthier, Gregory M., additional, Gavigan, Patrick, additional, Gerber, Jeffrey S., additional, Gernez, Yael, additional, Gigliotti, Francis, additional, Gilger, Mark A., additional, Glaser, Carol A., additional, Gould, Jane M., additional, Graziano, James, additional, Green, Amanda M., additional, Green, Michael, additional, Griffin, Daniel, additional, Griffin, Patricia M., additional, Griffith, David C., additional, Gupta, Piyush, additional, Gutelius, Bruce J., additional, Gutman, Julie R., additional, Hall, Aron J., additional, Hamdy, Rana F., additional, Han, Jin-Young, additional, Handy, Lori K., additional, Hanisch, Benjamin, additional, Harper, Marvin B., additional, Harris, Aaron M., additional, Harrison, Christopher J., additional, Haslam, David B., additional, Haston, Julia C., additional, Hawkes, Sarah.J., additional, Heald-Sargent, Taylor, additional, Hendley, J. Owen, additional, Hersh, Adam L., additional, Hilinski, Joseph A., additional, Hills, Susan L., additional, Hong, David K., additional, Hotez, Peter J., additional, Hsu, Katherine K., additional, Huang, Felicia Scaggs, additional, Hunstad, David A., additional, Hunt, W. Garrett, additional, Hwang, Loris Y., additional, Ilboudo, Christelle M., additional, Jaggi, Preeti, additional, Jean, Sophonie, additional, Jhaveri, Ravi, additional, Jirk-Pomajbkov, Kateina, additional, Kadry, Nadia A., additional, Kamb, Mary L., additional, Kapadia, Ronak K., additional, Katz, Ben Z., additional, Katz, Sophie E., additional, Kaur, Ishminder, additional, Kersh, Gilbert J., additional, Khan, Muhammad Ali, additional, Khurana, Ananta, additional, Kimberlin, David W., additional, Klein, Bruce, additional, Kobayashi, Miwako, additional, Kociolek, Larry K., additional, Koh, Andrew Y., additional, Kotloff, Karen L., additional, Kroger, Andrew T., additional, Kronman, Matthew P., additional, Lalor, Leah, additional, Lauren, Christine T., additional, Leber, Amy, additional, Leshem, Eyal, additional, Lewis, David B., additional, Livingston, Robyn A., additional, Llata, Eloisa, additional, Lloyd, Kevin, additional, Loh, Katrina, additional, Long, Sarah S., additional, Lopman, Benjamin A., additional, Lucero, Yalda C., additional, Lugo, Debra J., additional, Lujn-Zilbermann, Jorge, additional, Maldonado, Yvonne A., additional, Manaloor, John J., additional, Manthiram, Kalpana, additional, Martin, Stacey W., additional, Mathew, Roshni, additional, Mazzulli, Tony, additional, McFarland, Elizabeth J., additional, McGann, Kathleen A., additional, McNamara, Lucy A., additional, Meislich, Debrah, additional, Meissner, H. Cody, additional, Mejias, Asuncion, additional, Mertsola, Jussi, additional, Messacar, Kevin, additional, Mhaissen, Mohammad Nael, additional, Michaels, Marian G., additional, Miller, Melissa B., additional, Miller-Handley, Hilary, additional, Mintz, Eric, additional, Mohan, Parvathi, additional, Montgomery, Susan P., additional, Montoya, Jose G., additional, Moorman, Anne C., additional, Moro, Pedro L., additional, Moscicki, Anna-Barbara, additional, Muller, William J., additional, Myers, Angela L., additional, Nadel, Simon, additional, Nayak, Jennifer Lynn, additional, Neely, Michael Noel, additional, Neil, Karen P., additional, Nelson, Christina A., additional, Nelson, Noele P., additional, Nichols, Megin, additional, Nicholson, William, additional, Nopper, Amy Jo, additional, Norton, Laura E., additional, Ochoa, Theresa J., additional, Olarte, Liset, additional, Onarecker, Timothy R., additional, Orenstein, Walter A., additional, ORyan, Miguel, additional, Otto, William R., additional, Ouellette, Christopher P., additional, Paddock, Christopher D., additional, Palazzi, Debra L., additional, Panuganti, Suresh Kumar, additional, Pappas, Diane E., additional, Paret, Michal, additional, Pastula, Daniel M., additional, Patterson, Thomas F., additional, Petersen, Brett W., additional, Petrosyan, Mikael, additional, Pickering, Larry K., additional, Pindyck, Talia, additional, Pinninti, Swetha, additional, Pittet, Laure F., additional, Planet, Paul J., additional, Pollard, Andrew J., additional, Posfay-Barbe, Klara M., additional, Poulsen, Casper S., additional, Poutanen, Susan M., additional, Powers, Ann M., additional, Prasanphanich, Nina Salinger, additional, Pritt, Bobbi S., additional, Prober, Charles G., additional, Puar, Neha, additional, Quilter, Laura A.S., additional, Ramilo, Octavio, additional, Rao, Suchitra, additional, Ratner, Adam J., additional, Rawstron, Sarah A., additional, Read, Jennifer S., additional, Relich, Ryan F., additional, Reller, Megan E., additional, Robinson, Candice L., additional, Romero, Jos R., additional, Rosen, David A., additional, Ross, Shannon A., additional, Rours, G. Ingrid J.G., additional, Rowe, Peter C., additional, Rowley, Anne H., additional, Rubin, Lorry G., additional, Ryan, Edward T., additional, Sacharok, Alexandra, additional, Sandora, Thomas J., additional, Sapp, Sarah G.H., additional, Sardana, Kabir, additional, Sauberan, Jason B., additional, Schaffzin, Joshua K., additional, Schillie, Sarah, additional, Schuster, Jennifer E., additional, Schwartz, Kevin L., additional, Sederdahl, Bethany K., additional, Serpa-Alvarez, Jose, additional, Shah, Kara N., additional, Shah, Samir S., additional, Shaikh, Nader, additional, Shane, Andi L., additional, Shapiro, Eugene D., additional, Shaw, Jana, additional, Shetty, Avinash K., additional, Shope, Timothy R., additional, Dairiki Shortliffe, Linda M., additional, Shulman, Stanford T., additional, Shust, Gail F., additional, Siberry, George Kelly, additional, Siegel, Jane D., additional, Siegel, Robert David, additional, Simonsen, Kari A., additional, Singh, Upinder, additional, Smith, Christiana, additional, Smith, Lauren L., additional, Song, Eunkyung, additional, Souder, Emily, additional, Spearman, Paul, additional, St. Geme, Joseph W., additional, Staat, Mary Allen, additional, Staples, J. Erin, additional, Starke, Jeffrey R., additional, Statler, Victoria A., additional, Steinbach, William J., additional, Stensvold, Christen Rune, additional, Stokes, Erin K., additional, Stoner, Bradley P., additional, Storch, Gregory A., additional, Straily, Anne, additional, Sullivan, Kathleen E., additional, Swanson, Douglas S., additional, Tanz, Robert R., additional, Taormina, Gillian, additional, Tate, Jacqueline E., additional, Taveras, Jeanette, additional, Tebruegge, Marc, additional, Teshale, Eyasu H., additional, Thompson, George R., additional, Thompson-Stone, Robert, additional, Thomsen, Isaac, additional, Thomson, Richard B., additional, Thorell, Emily A., additional, Tien, Vivian, additional, Tobin, Nicole H., additional, Toltzis, Philip, additional, Treat, James, additional, Troy, Stephanie B., additional, Van Dvke, Russell B., additional, Vaz, Louise Elaine, additional, Vijayan, Vini, additional, Vodzak, Jennifer, additional, Wagner, Thor A., additional, Wald, Ellen R., additional, Wallihan, Rebecca, additional, Wang, Huanyu, additional, Wangu, Zoon, additional, Washam, Matthew, additional, Waters, Valerie, additional, Watson, Joshua R., additional, Weatherhead, Jill E., additional, Weinberg, Geoffrey A., additional, Weng, Mark K., additional, Wiederhold, Nathan P., additional, Wiesenfeld, Harold C., additional, Williams, Cydni, additional, Williams, John V., additional, Willoughby, Rodney E., additional, Wittler, Robert R., additional, Wood, James B., additional, Woods, Charles Reece, additional, Workowski, Kimberly A., additional, Wright, Terry W., additional, Wu, Hsi-Yang, additional, Xu, Huan, additional, Yagupsky, Pablo, additional, Yi, Jumi, additional, Yoder, Jonathan, additional, Young, Edward J., additional, Zaenglein, Andrea L., additional, Zimmermann, Petra, additional, and Zong, Wenjing, additional
- Published
- 2023
- Full Text
- View/download PDF
47. Type VII Collagen Deficiency in the Oncogenesis of Cutaneous Squamous Cell Carcinoma in Dystrophic Epidermolysis Bullosa
- Author
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South, Andrew P., Laimer, Martin, Gueye, Mouhamed, Sui, Jennifer Y., Eichenfield, Lawrence F., Mellerio, Jemima E., and Nyström, Alexander
- Published
- 2023
- Full Text
- View/download PDF
48. Triple-Combination Clindamycin Phosphate 1.2%/Adapalene 0.15%/Benzoyl Peroxide 3.1% Gel for Acne in Adult and Pediatric Participants
- Author
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Baldwin, Hilary, primary, Gold, Linda Stein, additional, Harper, Julie C, additional, Alexis, Andrew F, additional, Callender, Valerie D., additional, Kircik, Leon, additional, Guenin, Eric, additional, and Eichenfield, Lawrence F., additional
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- 2024
- Full Text
- View/download PDF
49. Hypothalamic-Pituitary-Adrenal Axis Response in Patients With Acne Vulgaris Treated With Clascoterone
- Author
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Bhatia, Neal, primary, Eichenfield, Lawrence F., additional, Mazzetti, Alessandro, additional, Moro, Luigi, additional, Squittieri, Nicholas, additional, and Hebert, Adelaide A., additional
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- 2024
- Full Text
- View/download PDF
50. Risk Factors and Outcomes of Nonmelanoma Skin Cancer in Children and Young Adults
- Author
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Huang, Jennifer T, Coughlin, Carrie C, Hawryluk, Elena B, Hook, Kristen, Humphrey, Stephen R, Kruse, Lacey, Lawley, Leslie, Al-Sayegh, Hasan, London, Wendy B, Marghoob, Ashfaq, Phung, Thuy L, Pope, Elena, Gerami, Pedram, Schmidt, Birgitta, Robinson, Sarah, Bartenstein, Diana, Bahrani, Eman, Brahmbhatt, Meera, Chen, Lily, Haddock, Ellen, Mansour, Danny, Nguyen, Julie, Raisanen, Tom, Tran, Gary, Travis, Kate, Wolner, Zachary, and Eichenfield, Lawrence F
- Subjects
Biomedical and Clinical Sciences ,Clinical Sciences ,Oncology and Carcinogenesis ,Cancer ,Prevention ,Pediatric ,Clinical Research ,Adolescent ,Antifungal Agents ,Antineoplastic Agents ,Carcinoma ,Basal Cell ,Carcinoma ,Squamous Cell ,Case-Control Studies ,Child ,Child ,Preschool ,Female ,Genetic Predisposition to Disease ,Humans ,Immunosuppressive Agents ,Infant ,Male ,Radiotherapy ,Retrospective Studies ,Risk Factors ,Skin Neoplasms ,United States ,Voriconazole ,Young Adult ,basal cell nevus syndrome ,chemotherapy ,genodermatosis ,iatrogenic ,prolonged immunosuppression ,radiation therapy ,voriconazole ,xeroderma pigmentosum ,Human Movement and Sports Sciences ,Paediatrics and Reproductive Medicine ,Pediatrics ,Paediatrics - Abstract
ObjectiveTo identify risk factors associated with nonmelanoma skin cancer (NMSC) occurrence and survival in children.Study designThis was a multicenter, retrospective, case-control study of patients 12 months prior to diagnosis and 49% of patients were diagnosed with ≥2 skin cancers. At last follow-up, 5% (6 of 124) of patients with NMSC died. Voriconazole exposure was noted in 7 cases and associated with worse 3-year overall survival (P = .001).ConclusionsNMSC in children and young adults is often associated with a predisposing condition or iatrogenic exposure. High-risk patients should be identified early to provide appropriate counseling and management.
- Published
- 2019
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