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1. Ruxolitinib Cream in Adolescents/Adults with Atopic Dermatitis Meeting Severity Thresholds for Systemic Therapy: Exploratory Analysis of Pooled Results from Two Phase 3 Studies.

Author

Simpson, Eric, Kircik, Leon, Blauvelt, Andrew, Kallender, Howard, Sturm, Daniel, Wang, Mingyue, and Eichenfield, Lawrence

Subjects
Atopic dermatitis, JAK, Janus kinase inhibition, Ruxolitinib cream
Abstract

INTRODUCTION: Standard therapy for patients with mild to moderate atopic dermatitis (AD) typically includes topical therapies; however, patients with more extensive AD and/or AD refractory to topical therapy may benefit from systemic treatment. Ruxolitinib cream monotherapy has demonstrated superior antipruritic and anti-inflammatory effects versus vehicle in patients with mild to moderate AD, and long-term disease control with as-needed use. Here, efficacy/safety of 1.5% ruxolitinib cream through 52 weeks was assessed in a subset of patients with moderate and/or more extensive disease. METHODS: This post hoc analysis of TRuE-AD1/TRuE-AD2 included patients who, at baseline, had Investigators Global Assessment (IGA) score of 3, Eczema Area and Severity Index (EASI) ≥ 16, and affected body surface area (BSA) ≥ 10% (higher severity of disease threshold subgroup). Disease control and safety were assessed. RESULTS: Of 1249 patients in the overall population, 78 (6.2%) met all higher severity of disease threshold criteria (continuous-use vehicle-controlled period: 1.5% ruxolitinib cream, n = 32; vehicle, n = 13); 28 and 4 of these patients, respectively, continued as-needed 1.5% ruxolitinib cream during the long-term safety (LTS) period. At week 8 (continuous-use), IGA-treatment success (IGA 0/1, with ≥ 2-grade improvement from baseline) was achieved by 19/32 (59.4%) patients applying 1.5% ruxolitinib cream versus no patients applying vehicle. In the LTS period, those achieving clear/almost clear skin increased from 19/28 patients (67.9%; continuous-use: week 8) to 18/23 patients (78.3%; as-needed use: week 52) in patients applying ruxolitinib cream from day 1. Ruxolitinib cream was well tolerated, with few application site reactions, regardless of disease severity threshold. Efficacy and safety results were similar to the overall study population. CONCLUSION: Patients with AD who meet standard disease severity eligibility criteria for systemic therapy may achieve IGA-treatment success with clear/almost clear skin with continuous-use ruxolitinib cream, and maintain long term-disease control with as-needed ruxolitinib cream monotherapy. TRIAL REGISTRATION NUMBER: NCT03745638/NCT03745651.

Published
2024

2. Practical Management of the JAK1 Inhibitor Abrocitinib for Atopic Dermatitis in Clinical Practice: Special Safety Considerations.

Author

Gooderham, Melinda, de Bruin-Weller, Marjolein, Weidinger, Stephan, Cork, Michael, Eichenfield, Lawrence, Simpson, Eric, Tsianakas, Athanasios, Kerkmann, Urs, Feeney, Claire, and Romero, William

Subjects
Abrocitinib, Atopic dermatitis, JAK1-selective inhibitor, Monitoring, Safety
Abstract

Abrocitinib, an oral, once-daily, Janus kinase (JAK) 1-selective inhibitor, is approved for the treatment of adults and adolescents with moderate-to-severe atopic dermatitis (AD). Abrocitinib has shown rapid and sustained efficacy in phase 3 trials and a consistent, manageable safety profile in long-term studies. Rapid itch relief and skin clearance are more likely to be achieved with a 200-mg daily dose of abrocitinib than with dupilumab. All oral JAK inhibitors are associated with adverse events of special interest and laboratory changes, and initial risk assessment and follow-up monitoring are important. Appropriate selection of patients and adequate monitoring are key for the safe use of JAK inhibitors. Here, we review the practical use of abrocitinib and discuss characteristics of patients who are candidates for abrocitinib therapy. In general, abrocitinib may be used in all appropriate patients with moderate-to-severe AD in need of systemic therapy, provided there are no contraindications, e.g., in patients with active serious systemic infections and those with severe hepatic impairment, as well as pregnant or breastfeeding women. For patients aged ≥ 65 years, current long-time or past long-time smokers, and those with risk factors for venous thromboembolism, major adverse cardiovascular events, or malignancies, a meticulous benefit-risk assessment is recommended, and it is advised to start with the 100-mg dose, when abrocitinib is the selected treatment option.

Published
2024

3. Efficacy, Safety, and Long-Term Disease Control of Ruxolitinib Cream Among Adolescents with Atopic Dermatitis: Pooled Results from Two Randomized Phase 3 Studies.

Author

Eichenfield, Lawrence, Simpson, Eric, Papp, Kim, Szepietowski, Jacek, Blauvelt, Andrew, Kircik, Leon, Silverberg, Jonathan, Siegfried, Elaine, Kuligowski, Michael, Venturanza, May, Kallender, Howard, Ren, Haobo, and Paller, Amy

Subjects
Humans, Nitriles, Pyrazoles, Pyrimidines, Adolescent, Female, Male, Dermatitis, Atopic, Child, Treatment Outcome, Severity of Illness Index, Skin Cream, Administration, Cutaneous, Double-Blind Method, Pruritus, Janus Kinase Inhibitors, Janus Kinase 1, Time Factors
Abstract

BACKGROUND: Atopic dermatitis (AD), a highly pruritic, inflammatory skin disease, affects approximately 7% of adolescents globally. A topical formulation of ruxolitinib, a Janus kinase (JAK) 1/JAK2 inhibitor, demonstrated safety and efficacy among adolescents/adults in two phase 3 studies (TRuE-AD1/TRuE-AD2). OBJECTIVE: To describe safety and efficacy of 1.5% ruxolitinib cream versus vehicle and long-term disease control of ruxolitinib cream among adolescents aged 12-17 years from pooled phase 3 study data. METHODS: Patients [≥ 12 years old with AD for ≥ 2 years, Investigators Global Assessment score (IGA) 2/3, and 3-20% affected body surface area (BSA) at baseline] were randomized 2:2:1 to ruxolitinib cream (0.75%/1.5%) or vehicle for 8 weeks of continuous use followed by a long-term safety (LTS) period up to 52 weeks with as-needed use. Patients originally applying vehicle were rerandomized 1:1 to 0.75%/1.5% ruxolitinib cream. Efficacy measures at week 8 included IGA treatment success (IGA-TS; i.e., score of 0/1 with ≥ 2 grade improvement from baseline), ≥ 75% improvement in Eczema Area and Severity Index (EASI-75), and ≥ 4-point improvement in itch numerical rating scale (NRS4). Measures of disease control during the LTS period included IGA score of 0 (clear) or 1 (almost clear) and percentage affected BSA. Safety was assessed throughout the study. RESULTS: Of 1249 randomized patients, 245 (19.6%) were aged 12-17 years. Of these, 45 patients were randomized to vehicle and 92 patients to 1.5% ruxolitinib cream. A total of 104/137 (75.9%) patients continued on 1.5% ruxolitinib cream in the LTS period [82/92 (89.1%) continued on 1.5% ruxolitinib cream; 22/45 (48.9%) patients on vehicle were reassigned to 1.5% ruxolitinib cream], and 83/104 (79.8%) of these patients completed the LTS period. At week 8, substantially more patients who applied 1.5% ruxolitinib cream versus vehicle achieved IGA-TS (50.6% versus 14.0%), EASI-75 (60.9% versus 34.9%), and NRS4 (52.1% versus 17.4%; P = 0.009). The mean (SD) reduction in itch NRS scores was significantly greater in patients applying 1.5% ruxolitinib cream versus vehicle from day 2 [- 0.9 (1.9) versus -0.2 (1.4); P = 0.03]. During the LTS period, mean (SD) trough steady-state ruxolitinib plasma concentrations at weeks 12/52 were 27.2 (55.7)/15.5 (31.5) nM. The percentage of patients achieving IGA score of 0 or 1 was sustained or further increased with 1.5% ruxolitinib cream; mean affected BSA was generally low (< 3%; i.e., mild disease). Through 52 weeks, application site reactions occurred in 1.8% of adolescent patients applying 1.5% ruxolitinib cream at any time; no patients had serious adverse events. There were no serious infections, malignancies, major adverse cardiovascular events, or thromboembolic events. CONCLUSIONS: Meaningful anti-inflammatory and antipruritic effects were demonstrated with 1.5% ruxolitinib cream in the subset of adolescent patients with AD, comparable with those observed in the overall study population; long-term, as-needed use maintained disease control and was well tolerated. CLINICAL TRIAL REGISTRATION: ClinicalTrials.gov identifiers NCT03745638 (registered 19 November 2018) and NCT03745651 (registered 19 November 2018).

Published
2024

10. Lebrikizumab Provides Rapid Clinical Responses Across All Eczema Area and Severity Index Body Regions and Clinical Signs in Adolescents and Adults with Moderate-to-Severe Atopic Dermatitis

Author

Simpson, Eric L., de Bruin-Weller, Marjolein, Hong, H. Chih-ho, Staumont-Sallé, Delphine, Blauvelt, Andrew, Eyerich, Kilian, Gooderham, Melinda, Shahriari, Mona, Mallbris, Lotus, Atwater, Amber Reck, Rueda, Maria Jose, Ding, Yuxin, Liu, Zhuqing, Agell, Helena, and Silverberg, Jonathan I.

Published
2024
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11. Upadacitinib Rapidly Improves Patient-Reported Outcomes in Atopic Dermatitis: 16-Week Results from Phase 3 Clinical Trials (Measure Up 1 and 2)

Author

Simpson, Eric L., Prajapati, Vimal H., Leshem, Yael A., Chovatiya, Raj, de Bruin-Weller, Marjolein S., Ständer, Sonja, Pink, Andrew E., Calimlim, Brian M., Lee, Wan-Ju, Teixeira, Henrique, Ladizinski, Barry, Hu, Xiaofei, Yang, Yang, Liu, Yingyi, Liu, Meng, Grada, Ayman, Platt, Andrew M., and Silverberg, Jonathan I.

Published
2024
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19. Exposure to isocyanates predicts atopic dermatitis prevalence and disrupts therapeutic pathways in commensal bacteria

Author

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

Subjects
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.

Published
2023

20. The Validated Investigator Global Assessment for Atopic Dermatitis (vIGA‐AD™): a clinical outcome measure for the severity of atopic dermatitis

Author

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

Subjects
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

Published
2022

21. 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

Author

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

Published
2024
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22. Integrated Exposure–Response of Dupilumab in Children, Adolescents, and Adults With Atopic Dermatitis Using Categorical and Continuous Efficacy Assessments: A Population Analysis

Author

Briggs, Emily, Kamal, Mohamed A., Kosloski, Matthew P., Linsmeier, Ian, Jusko, Natalie, Dolphin, Nancy, Chittenden, Jason, Simpson, Eric L., Paller, Amy S., Siegfried, Elaine C., Shumel, Brad, Levit, Noah A., Bansal, Ashish, Davis, John D., Chapel, Sunny, Smith, David E., and Huniti, Nidal

Published
2023
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26. Dupilumab treatment improves signs, symptoms, quality of life, and work productivity in patients with atopic hand and foot dermatitis: Results from a phase 3, randomized, double-blind, placebo-controlled trial

Author

Simpson, Eric L., Silverberg, Jonathan I., Worm, Margitta, Honari, Golara, Masuda, Koji, Syguła, Ewa, Schuttelaar, Marie L.A., Mortensen, Eric, Laws, Elizabeth, Akinlade, Bolanle, Patel, Naimish, Maloney, Jennifer, Paleczny, Heather, Delevry, Dimittri, Xiao, Jing, Dubost-Brama, Ariane, and Bansal, Ashish

Published
2024
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34. Whole genome sequencing identifies novel genetic mutations in patients with eczema herpeticum

Author

Bin, Lianghua, Malley, Claire, Taylor, Patricia, Boorgula, Meher Preethi, Chavan, Sameer, Daya, Michelle, Mathias, Malaika, Shankar, Gautam, Rafaels, Nicholas, Vergara, Candelaria, Potee, Joseph, Campbell, Monica, Hanifin, Jon M, Simpson, Eric, Schneider, Lynda C, Gallo, Richard L, Hata, Tissa, Paller, Amy S, De Benedetto, Anna, Beck, Lisa A, Ong, Peck Y, Guttman‐Yassky, Emma, Richers, Brittany, Baraghoshi, David, Ruczinski, Ingo, Barnes, Kathleen C, Leung, Donald YM, and Mathias, Rasika A

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Genetics, Biotechnology, Sexually Transmitted Infections, Human Genome, 2.1 Biological and endogenous factors, Aetiology, Skin, Dermatitis, Atopic, Glutathione Transferase, Herpesvirus 1, Human, Humans, Kaposi Varicelliform Eruption, Mutation, Nucleotide Transport Proteins, Whole Genome Sequencing, atopic dermatitis, eczema herpeticum, genetics, herpes simplex virus, SIDT2, whole genome sequencing, SIDT2, Immunology, Allergy
Abstract

BackgroundEczema herpeticum (EH) is a rare complication of atopic dermatitis (AD) caused by disseminated herpes simplex virus (HSV) infection. The role of rare and/or deleterious genetic variants in disease etiology is largely unknown. This study aimed to identify genes that harbor damaging genetic variants associated with HSV infection in AD with a history of recurrent eczema herpeticum (ADEH+).MethodsWhole genome sequencing (WGS) was performed on 49 recurrent ADEH+ (≥3 EH episodes), 491 AD without a history of eczema herpeticum (ADEH-) and 237 non-atopic control (NA) subjects. Variants were annotated, and a gene-based approach (SKAT-O) was used to identify genes harboring damaging genetic variants associated with ADEH+. Genes identified through WGS were studied for effects on HSV responses and keratinocyte differentiation.ResultsEight genes were identified in the comparison of recurrent ADEH+to ADEH-and NA subjects: SIDT2, CLEC7A, GSTZ1, TPSG1, SP110, RBBP8NL, TRIM15, and FRMD3. Silencing SIDT2 and RBBP8NL in normal human primary keratinocytes (NHPKs) led to significantly increased HSV-1 replication. SIDT2-silenced NHPKs had decreased gene expression of IFNk and IL1b in response to HSV-1 infection. RBBP8NL-silenced NHPKs had decreased gene expression of IFNk, but increased IL1b. Additionally, silencing SIDT2 and RBBP8NL also inhibited gene expression of keratinocyte differentiation markers keratin 10 (KRT10) and loricrin (LOR).ConclusionSIDT2 and RBBP8NL participate in keratinocyte's response to HSV-1 infection. SIDT2 and RBBP8NL also regulate expression of keratinocyte differentiation genes of KRT10 and LOR.

Published
2021

35. Rapid reduction in Staphylococcus aureus in atopic dermatitis subjects following dupilumab treatment

Author

Simpson, Eric L., Schlievert, Patrick M., Yoshida, Takeshi, Lussier, Stephanie, Boguniewicz, Mark, Hata, Tissa, Fuxench, Zelma, De Benedetto, Anna, Ong, Peck Y., Ko, Justin, Calatroni, Agustin, Rudman Spergel, Amanda K., Plaut, Marshall, Quataert, Sally A., Kilgore, Samuel H., Peterson, Liam, Gill, Ann L., David, Gloria, Mosmann, Tim, Gill, Steven R., Leung, Donald Y.M., and Beck, Lisa A.

Published
2023
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41. International observational atopic dermatitis cohort to follow natural history and treatment course: TARGET-DERM AD study design and rationale.

Author

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

Subjects
eczema, medical history, statistics & research methods, therapeutics, statistics &amp, 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.

Published
2020

44. The IL-4Rα Q576R polymorphism is associated with increased severity of atopic dermatitis and exaggerates allergic skin inflammation in mice

Author

Yang, Barbara, Wilkie, Hazel, Das, Mrinmoy, Timilshina, Maheshwor, Bainter, Wayne, Woods, Brian, Daya, Michelle, Boorgula, Meher P., Mathias, Rasika A., Lai, Peggy, Petty, Carter R., Weller, Edie, Harb, Hani, Chatila, Talal A., Leung, Donald Y.M., Beck, Lisa A., Simpson, Eric L., Hata, Tissa R., Barnes, Kathleen C., Phipatanakul, Wanda, Leyva-Castillo, Juan-Manuel, and Geha, Raif S.

Published
2023
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46. Infections in Dupilumab Clinical Trials in Atopic Dermatitis: A Comprehensive Pooled Analysis

Author

Eichenfield, Lawrence F, Bieber, Thomas, Beck, Lisa A, Simpson, Eric L, Thaçi, Diamant, de Bruin-Weller, Marjolein, Deleuran, Mette, Silverberg, Jonathan I, Ferrandiz, Carlos, Fölster-Holst, Regina, Chen, Zhen, Graham, Neil MH, Pirozzi, Gianluca, Akinlade, Bolanle, Yancopoulos, George D, and Ardeleanu, Marius

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Infectious Diseases, Clinical Trials and Supportive Activities, Clinical Research, Patient Safety, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Skin, Inflammatory and immune system, Infection, Good Health and Well Being, Adult, Antibodies, Monoclonal, Antibodies, Monoclonal, Humanized, Clinical Trials, Phase II as Topic, Clinical Trials, Phase III as Topic, Dermatitis, Atopic, Double-Blind Method, Humans, Incidence, Injections, Subcutaneous, Placebos, Randomized Controlled Trials as Topic, Severity of Illness Index, Skin Diseases, Infectious, Treatment Outcome, Dermatology & Venereal Diseases, Clinical sciences
Abstract

BackgroundPatients with moderate-to-severe atopic dermatitis (AD) have increased infection risk, including skin infections and systemic infections. Immunomodulators (e.g., anti-tumor necrosis factors, anti-interleukin [anti-IL]-23, anti-IL-17, Janus kinase inhibitors) increase risk of infections. Dupilumab (a monoclonal antibody blocking the shared receptor component for IL-4 and IL-13) is approved for inadequately controlled moderate-to-severe AD and for moderate-to-severe eosinophilic or oral corticosteroid-dependent asthma.ObjectiveThe aim was to determine the impact of dupilumab on infection rates in patients with moderate-to-severe AD.MethodsThis analysis pooled data from seven randomized, placebo-controlled dupilumab trials in adults with moderate-to-severe AD. Exposure-adjusted analyses assessed infection rates.ResultsOf 2932 patients, 1091 received placebo, 1095 dupilumab 300 mg weekly, and 746 dupilumab 300 mg every 2 weeks. Treatment groups had similar infection rates overall per 100 patient-years (placebo, 155; dupilumab weekly, 150; dupilumab every 2 weeks, 156; dupilumab combined, 152), and similar non-skin infection rates. Serious/severe infections were reduced with dupilumab (risk ratio 0.43; p

Published
2019

47. Crisaborole Ointment Improves Quality of Life of Patients with Mild to Moderate Atopic Dermatitis and Their Families

Author

Simpson, Eric L, Paller, Amy S, Boguniewicz, Mark, Eichenfield, Lawrence F, Feldman, Steven R, Silverberg, Jonathan I, Chamlin, Sarah L, and Zane, Lee T

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Neurodegenerative, Clinical Research, Atopic dermatitis, Crisaborole, Eczema, PDE4, Phosphodiesterase 4, Quality of life, Topical treatment, Clinical sciences
Abstract

IntroductionThe impact of crisaborole ointment, a nonsteroidal phosphodiesterase 4 inhibitor for the treatment of mild to moderate atopic dermatitis (AD), on quality of life (QoL) was assessed in two identically designed phase 3 studies (AD-301: NCT02118766; AD-302: NCT02118792, both at http://www.clinicaltrials.gov ).MethodsIn both studies, patients aged ≥ 2 years with mild to moderate AD per the Investigator's Static Global Assessment were randomly assigned 2:1 to receive crisaborole or vehicle twice daily for 28 days. QoL was assessed using the Children's Dermatology Life Quality Index (CDLQI) (2-15 years), the Dermatology Life Quality Index (DLQI) (≥ 16 years), and the Dermatitis Family Impact Questionnaire (DFI) (parents/caregivers/family of patients aged 2-17 years). Established QoL score severity bands provided clinical context.ResultsGreater mean improvement in QoL was observed in crisaborole-treated patients than in vehicle-treated patients at day 29 [mean change from baseline (∆BL), CDLQI: - 4.6 vs. - 3.0; P < 0.001; DLQI: - 5.2 vs. - 3.5; P = 0.015]. At baseline, more than half the patients had a "moderate effect" or higher of AD on QoL. At day 29, there was a trend toward more crisaborole- than vehicle-treated patients having "small effect" to "no effect", The QoL of parents/caregivers/family improved more for crisaborole-treated than for vehicle-treated patients (∆BL, DFI: - 3.7 vs. - 2.7; P = 0.003).ConclusionCrisaborole treatment results in clinically meaningful improvement in QoL for patients and their parents/caregivers/families.Trial registrationAD-301: http://www.clinicaltrials.gov , NCT02118766; AD-302: http://www.clinicaltrials.gov , NCT02118792.FundingAnacor Pharmaceuticals, Inc., a wholly owned subsidiary of Pfizer Inc., New York, NY.

Published
2018

49. Dupilumab in children aged 6 months to younger than 6 years with uncontrolled atopic dermatitis: a randomised, double-blind, placebo-controlled, phase 3 trial

Author

Pepper, Amber, Paller, Amy S, Lockshin, Benjamin, Cohen, David, Pariser, David, Siegfried, Elaine C, Simpson, Eric L, Leflein, Jeffrey, Weinberg, Jeffrey, Browning, John, Teng, Joyce, Wine Lee, Lara, Sher, Lawrence, Diaz, Lucia, Schneider, Lynda, Gonzalez, Mercedes E, Rupp, Ned, Ong, Peck, Cartwright, Robert, Sidbury, Robert, Soong, Weily, Pinter, Andreas, Wollenberg, Andreas, Schnopp, Christina, Cork, Michael J, Arkwright, Peter D, Korkosz, Anna, Bystrzanowska, Dorota, Sygula, Ewa, Zdybski, Jacek, Padlewska, Kamila, Schneider, Lynda C, Meltzer, Steven, Wang, Zhixiao, Mannent, Leda P, Amin, Nikhil, Sun, Yiping, Laws, Elizabeth, Akinlade, Bolanle, Dillon, Myles, Kosloski, Matthew P, Kamal, Mohamed A, Dubost-Brama, Ariane, Patel, Naimish, Weinreich, David M, Yancopoulos, George D, O’Malley, John T, and Bansal, Ashish

Published
2022
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50. Dupilumab Demonstrates Rapid Onset of Response Across Three Type 2 Inflammatory Diseases

Author

Canonica, G. Walter, Bourdin, Arnaud, Peters, Anju T., Desrosiers, Martin, Bachert, Claus, Weidinger, Stephan, Simpson, Eric L., Daizadeh, Nadia, Chen, Zhen, Kamat, Siddhesh, Khan, Asif H., Chao, Jingdong, Graham, Neil M.H., Laws, Elizabeth, Rossi, Ana B., Ardeleanu, Marius, Mannent, Leda P., Amin, Nikhil, Ortiz, Benjamin, Deniz, Yamo, Djandji, Michel, and Rowe, Paul J.

Published
2022
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