A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients

S. Reitamo; M. Rustin; J. Harper; K. Kalimo; A. Rubins; F. Cambazard; E. E.A. Brenninkmeijer; C. Smith; J. Berth-Jones; T. Ruzicka; G. Sharpe; A. Taieb; Linda De Raeve; Christian Groønhoøj-Larsen; Anita Remitz; Kristiina Turjanmaa; Jean Luc Perrot; Franck Boralevi; Louis Dubertret; Morad Lahfa; Laurent Misery; Yves De Prost; Christine Bodemer; Jean François Stadler; Sébastien Barbarot; Patrice Plantin; Patricia Schoenlaub; Gérard Lorette; Randa Khallouf; Claire Beylot; Leena Bruckner-Tuderman; Andreas Wollenberg; Stefanie Kamann; Alexander Kapp; Manige Fartasch; Regine Fölster-Holst; Thomas Bieber; Johannes Ring; Attila Dobozy; Lajos Kemény; Gillian Murphy; Jane Barry; John Bourke; Nora Valdmane; Maria Blaszczyk; Hanna Wolska; Jan Bos; Lecha Carralero; Cristina Carrera; Camacho Martínez; Antonio Rodríguez Pichardo; Ortiz De Frutos; Elena Sánchez Largo Uceda; Annie Waite; Adrian Green; Peter Friedmann; Andrew Finlay; Christopher Griffiths

doi:10.1111/j.1365-2133.2008.08747.x

A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients

S. Reitamo, M. Rustin, J. Harper, K. Kalimo, A. Rubins, F. Cambazard, E. E.A. Brenninkmeijer, C. Smith, J. Berth-Jones, T. Ruzicka, G. Sharpe, A. Taieb, Linda De Raeve, Christian Groønhoøj-Larsen, Anita Remitz, Kristiina Turjanmaa, Jean Luc Perrot, Franck Boralevi, Louis Dubertret, Morad LahfaLaurent Misery, Yves De Prost, Christine Bodemer, Jean François Stadler, Sébastien Barbarot, Patrice Plantin, Patricia Schoenlaub, Gérard Lorette, Randa Khallouf, Claire Beylot, Leena Bruckner-Tuderman, Andreas Wollenberg, Stefanie Kamann, Alexander Kapp, Manige Fartasch, Regine Fölster-Holst, Thomas Bieber, Johannes Ring, Attila Dobozy, Lajos Kemény, Gillian Murphy, Jane Barry, John Bourke, Nora Valdmane, Maria Blaszczyk, Hanna Wolska, Jan Bos, Lecha Carralero, Cristina Carrera, Camacho Martínez, Antonio Rodríguez Pichardo, Ortiz De Frutos, Elena Sánchez Largo Uceda, Annie Waite, Adrian Green, Peter Friedmann, Andrew Finlay, Christopher Griffiths

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Abstract

Background: For the treatment of a chronic disease like atopic dermatitis, sustained tolerability and efficacy of the applied medication are essential. Objectives: The present open-label, noncomparative study was conducted to obtain information on the long-term safety and efficacy of 0.1% tacrolimus ointment. Methods: Patients aged 2 years or older with an affected body surface area of more than 5%, who previously participated in a clinical trial on tacrolimus ointment, were eligible for this study. The treatment area was defined by the investigator at study entry. Both children and adults applied continuously or intermittently 0.1% tacrolimus ointment twice daily during episodes of active disease plus an additional week after remission over a follow-up period of up to 4 years. Results: The intent-to-treat population comprised 782 patients, with a median age of 22 years (range 2-72). Patients remained in the study for up to 4 years. Approximately half of the patients discontinued the study prematurely; the median follow-up was 1422 days. Median tacrolimus ointment use was 31.2 g during the first week; ointment use decreased during the first year and then remained stable for the remainder of the study. The median cumulative tacrolimus use was 271.5 g at month 6, 462.5 g at month 12, 739.9 g at month 24, 1029.3 g at month 36 and 1320.8 g at month 48. Altogether 51.8% of patients discontinued the study prematurely; the main reasons were withdrawal of consent (13.3%), loss to follow-up (11.3%) and lack of efficacy (9.4%). Adverse events led to study discontinuation in 3.7% of the patients. The most frequent application site events were skin burning and pruritus. These events were most often reported in adult patients during the initial treatment period; prevalence decreased after the first week and remained at a low level throughout the study. Nonapplication site events occurred with stable incidences throughout the study period. In general, calculated daily hazard rates did not indicate an increased risk of adverse events with prolonged treatment. The total affected body surface area decreased substantially upon onset of treatment and efficacy of treatment was maintained until the end of the study with smaller but continuous improvements throughout the follow-up period. Overall, 75% of the patients and 76% of the investigators rated their satisfaction with the treatment as excellent, very good or good at the end of the study or at the time of premature discontinuation. Conclusions: The safety profile of intermittent or continuous long-term application of 0.1% tacrolimus ointment for up to 4 years was consistent with that which has been established from shorter studies and gave no reason for concern. In addition, 0.1% tacrolimus ointment demonstrated sustained efficacy as reflected by the expression of high satisfaction with treatment by both patients and investigators.

Original language	English
Pages (from-to)	942-951
Number of pages	10
Journal	British Journal of Dermatology
Volume	159
Issue number	4
DOIs	https://doi.org/10.1111/j.1365-2133.2008.08747.x
State	Published - Oct 2008

Keywords

Atopic dermatitis
Long-term
Safety
Tacrolimus ointment

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10.1111/j.1365-2133.2008.08747.x

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Reitamo, S., Rustin, M., Harper, J., Kalimo, K., Rubins, A., Cambazard, F., Brenninkmeijer, E. E. A., Smith, C., Berth-Jones, J., Ruzicka, T., Sharpe, G., Taieb, A., De Raeve, L., Groønhoøj-Larsen, C., Remitz, A., Turjanmaa, K., Perrot, J. L., Boralevi, F., Dubertret, L., ... Griffiths, C. (2008). A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients. British Journal of Dermatology, 159(4), 942-951. https://doi.org/10.1111/j.1365-2133.2008.08747.x

@article{fadd13a37e644ed1ba9b7b9008e7fa00,

title = "A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients",

abstract = "Background: For the treatment of a chronic disease like atopic dermatitis, sustained tolerability and efficacy of the applied medication are essential. Objectives: The present open-label, noncomparative study was conducted to obtain information on the long-term safety and efficacy of 0.1% tacrolimus ointment. Methods: Patients aged 2 years or older with an affected body surface area of more than 5%, who previously participated in a clinical trial on tacrolimus ointment, were eligible for this study. The treatment area was defined by the investigator at study entry. Both children and adults applied continuously or intermittently 0.1% tacrolimus ointment twice daily during episodes of active disease plus an additional week after remission over a follow-up period of up to 4 years. Results: The intent-to-treat population comprised 782 patients, with a median age of 22 years (range 2-72). Patients remained in the study for up to 4 years. Approximately half of the patients discontinued the study prematurely; the median follow-up was 1422 days. Median tacrolimus ointment use was 31.2 g during the first week; ointment use decreased during the first year and then remained stable for the remainder of the study. The median cumulative tacrolimus use was 271.5 g at month 6, 462.5 g at month 12, 739.9 g at month 24, 1029.3 g at month 36 and 1320.8 g at month 48. Altogether 51.8% of patients discontinued the study prematurely; the main reasons were withdrawal of consent (13.3%), loss to follow-up (11.3%) and lack of efficacy (9.4%). Adverse events led to study discontinuation in 3.7% of the patients. The most frequent application site events were skin burning and pruritus. These events were most often reported in adult patients during the initial treatment period; prevalence decreased after the first week and remained at a low level throughout the study. Nonapplication site events occurred with stable incidences throughout the study period. In general, calculated daily hazard rates did not indicate an increased risk of adverse events with prolonged treatment. The total affected body surface area decreased substantially upon onset of treatment and efficacy of treatment was maintained until the end of the study with smaller but continuous improvements throughout the follow-up period. Overall, 75% of the patients and 76% of the investigators rated their satisfaction with the treatment as excellent, very good or good at the end of the study or at the time of premature discontinuation. Conclusions: The safety profile of intermittent or continuous long-term application of 0.1% tacrolimus ointment for up to 4 years was consistent with that which has been established from shorter studies and gave no reason for concern. In addition, 0.1% tacrolimus ointment demonstrated sustained efficacy as reflected by the expression of high satisfaction with treatment by both patients and investigators.",

keywords = "Atopic dermatitis, Long-term, Safety, Tacrolimus ointment",

author = "S. Reitamo and M. Rustin and J. Harper and K. Kalimo and A. Rubins and F. Cambazard and Brenninkmeijer, {E. E.A.} and C. Smith and J. Berth-Jones and T. Ruzicka and G. Sharpe and A. Taieb and {De Raeve}, Linda and Christian Gro{\o}nho{\o}j-Larsen and Anita Remitz and Kristiina Turjanmaa and Perrot, {Jean Luc} and Franck Boralevi and Louis Dubertret and Morad Lahfa and Laurent Misery and {De Prost}, Yves and Christine Bodemer and Stadler, {Jean Fran{\c c}ois} and S{\'e}bastien Barbarot and Patrice Plantin and Patricia Schoenlaub and G{\'e}rard Lorette and Randa Khallouf and Claire Beylot and Leena Bruckner-Tuderman and Andreas Wollenberg and Stefanie Kamann and Alexander Kapp and Manige Fartasch and Regine F{\"o}lster-Holst and Thomas Bieber and Johannes Ring and Attila Dobozy and Lajos Kem{\'e}ny and Gillian Murphy and Jane Barry and John Bourke and Nora Valdmane and Maria Blaszczyk and Hanna Wolska and Jan Bos and Lecha Carralero and Cristina Carrera and Camacho Mart{\'i}nez and Pichardo, {Antonio Rodr{\'i}guez} and {De Frutos}, Ortiz and Uceda, {Elena S{\'a}nchez Largo} and Annie Waite and Adrian Green and Peter Friedmann and Andrew Finlay and Christopher Griffiths",

year = "2008",

month = oct,

doi = "10.1111/j.1365-2133.2008.08747.x",

language = "English",

volume = "159",

pages = "942--951",

journal = "British Journal of Dermatology",

issn = "0007-0963",

publisher = "Oxford University Press",

number = "4",

}

Reitamo, S, Rustin, M, Harper, J, Kalimo, K, Rubins, A, Cambazard, F, Brenninkmeijer, EEA, Smith, C, Berth-Jones, J, Ruzicka, T, Sharpe, G, Taieb, A, De Raeve, L, Groønhoøj-Larsen, C, Remitz, A, Turjanmaa, K, Perrot, JL, Boralevi, F, Dubertret, L, Lahfa, M, Misery, L, De Prost, Y, Bodemer, C, Stadler, JF, Barbarot, S, Plantin, P, Schoenlaub, P, Lorette, G, Khallouf, R, Beylot, C, Bruckner-Tuderman, L, Wollenberg, A, Kamann, S, Kapp, A, Fartasch, M, Fölster-Holst, R, Bieber, T, Ring, J, Dobozy, A, Kemény, L, Murphy, G, Barry, J, Bourke, J, Valdmane, N, Blaszczyk, M, Wolska, H, Bos, J, Carralero, L, Carrera, C, Martínez, C, Pichardo, AR, De Frutos, O, Uceda, ESL, Waite, A, Green, A, Friedmann, P, Finlay, A & Griffiths, C 2008, 'A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients', British Journal of Dermatology, vol. 159, no. 4, pp. 942-951. https://doi.org/10.1111/j.1365-2133.2008.08747.x

TY - JOUR

T1 - A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients

AU - Reitamo, S.

AU - Rustin, M.

AU - Harper, J.

AU - Kalimo, K.

AU - Rubins, A.

AU - Cambazard, F.

AU - Brenninkmeijer, E. E.A.

AU - Smith, C.

AU - Berth-Jones, J.

AU - Ruzicka, T.

AU - Sharpe, G.

AU - Taieb, A.

AU - De Raeve, Linda

AU - Groønhoøj-Larsen, Christian

AU - Remitz, Anita

AU - Turjanmaa, Kristiina

AU - Perrot, Jean Luc

AU - Boralevi, Franck

AU - Dubertret, Louis

AU - Lahfa, Morad

AU - Misery, Laurent

AU - De Prost, Yves

AU - Bodemer, Christine

AU - Stadler, Jean François

AU - Barbarot, Sébastien

AU - Plantin, Patrice

AU - Schoenlaub, Patricia

AU - Lorette, Gérard

AU - Khallouf, Randa

AU - Beylot, Claire

AU - Bruckner-Tuderman, Leena

AU - Wollenberg, Andreas

AU - Kamann, Stefanie

AU - Kapp, Alexander

AU - Fartasch, Manige

AU - Fölster-Holst, Regine

AU - Bieber, Thomas

AU - Ring, Johannes

AU - Dobozy, Attila

AU - Kemény, Lajos

AU - Murphy, Gillian

AU - Barry, Jane

AU - Bourke, John

AU - Valdmane, Nora

AU - Blaszczyk, Maria

AU - Wolska, Hanna

AU - Bos, Jan

AU - Carralero, Lecha

AU - Carrera, Cristina

AU - Martínez, Camacho

AU - Pichardo, Antonio Rodríguez

AU - De Frutos, Ortiz

AU - Uceda, Elena Sánchez Largo

AU - Waite, Annie

AU - Green, Adrian

AU - Friedmann, Peter

AU - Finlay, Andrew

AU - Griffiths, Christopher

PY - 2008/10

Y1 - 2008/10

N2 - Background: For the treatment of a chronic disease like atopic dermatitis, sustained tolerability and efficacy of the applied medication are essential. Objectives: The present open-label, noncomparative study was conducted to obtain information on the long-term safety and efficacy of 0.1% tacrolimus ointment. Methods: Patients aged 2 years or older with an affected body surface area of more than 5%, who previously participated in a clinical trial on tacrolimus ointment, were eligible for this study. The treatment area was defined by the investigator at study entry. Both children and adults applied continuously or intermittently 0.1% tacrolimus ointment twice daily during episodes of active disease plus an additional week after remission over a follow-up period of up to 4 years. Results: The intent-to-treat population comprised 782 patients, with a median age of 22 years (range 2-72). Patients remained in the study for up to 4 years. Approximately half of the patients discontinued the study prematurely; the median follow-up was 1422 days. Median tacrolimus ointment use was 31.2 g during the first week; ointment use decreased during the first year and then remained stable for the remainder of the study. The median cumulative tacrolimus use was 271.5 g at month 6, 462.5 g at month 12, 739.9 g at month 24, 1029.3 g at month 36 and 1320.8 g at month 48. Altogether 51.8% of patients discontinued the study prematurely; the main reasons were withdrawal of consent (13.3%), loss to follow-up (11.3%) and lack of efficacy (9.4%). Adverse events led to study discontinuation in 3.7% of the patients. The most frequent application site events were skin burning and pruritus. These events were most often reported in adult patients during the initial treatment period; prevalence decreased after the first week and remained at a low level throughout the study. Nonapplication site events occurred with stable incidences throughout the study period. In general, calculated daily hazard rates did not indicate an increased risk of adverse events with prolonged treatment. The total affected body surface area decreased substantially upon onset of treatment and efficacy of treatment was maintained until the end of the study with smaller but continuous improvements throughout the follow-up period. Overall, 75% of the patients and 76% of the investigators rated their satisfaction with the treatment as excellent, very good or good at the end of the study or at the time of premature discontinuation. Conclusions: The safety profile of intermittent or continuous long-term application of 0.1% tacrolimus ointment for up to 4 years was consistent with that which has been established from shorter studies and gave no reason for concern. In addition, 0.1% tacrolimus ointment demonstrated sustained efficacy as reflected by the expression of high satisfaction with treatment by both patients and investigators.

AB - Background: For the treatment of a chronic disease like atopic dermatitis, sustained tolerability and efficacy of the applied medication are essential. Objectives: The present open-label, noncomparative study was conducted to obtain information on the long-term safety and efficacy of 0.1% tacrolimus ointment. Methods: Patients aged 2 years or older with an affected body surface area of more than 5%, who previously participated in a clinical trial on tacrolimus ointment, were eligible for this study. The treatment area was defined by the investigator at study entry. Both children and adults applied continuously or intermittently 0.1% tacrolimus ointment twice daily during episodes of active disease plus an additional week after remission over a follow-up period of up to 4 years. Results: The intent-to-treat population comprised 782 patients, with a median age of 22 years (range 2-72). Patients remained in the study for up to 4 years. Approximately half of the patients discontinued the study prematurely; the median follow-up was 1422 days. Median tacrolimus ointment use was 31.2 g during the first week; ointment use decreased during the first year and then remained stable for the remainder of the study. The median cumulative tacrolimus use was 271.5 g at month 6, 462.5 g at month 12, 739.9 g at month 24, 1029.3 g at month 36 and 1320.8 g at month 48. Altogether 51.8% of patients discontinued the study prematurely; the main reasons were withdrawal of consent (13.3%), loss to follow-up (11.3%) and lack of efficacy (9.4%). Adverse events led to study discontinuation in 3.7% of the patients. The most frequent application site events were skin burning and pruritus. These events were most often reported in adult patients during the initial treatment period; prevalence decreased after the first week and remained at a low level throughout the study. Nonapplication site events occurred with stable incidences throughout the study period. In general, calculated daily hazard rates did not indicate an increased risk of adverse events with prolonged treatment. The total affected body surface area decreased substantially upon onset of treatment and efficacy of treatment was maintained until the end of the study with smaller but continuous improvements throughout the follow-up period. Overall, 75% of the patients and 76% of the investigators rated their satisfaction with the treatment as excellent, very good or good at the end of the study or at the time of premature discontinuation. Conclusions: The safety profile of intermittent or continuous long-term application of 0.1% tacrolimus ointment for up to 4 years was consistent with that which has been established from shorter studies and gave no reason for concern. In addition, 0.1% tacrolimus ointment demonstrated sustained efficacy as reflected by the expression of high satisfaction with treatment by both patients and investigators.

KW - Atopic dermatitis

KW - Long-term

KW - Safety

KW - Tacrolimus ointment

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U2 - 10.1111/j.1365-2133.2008.08747.x

DO - 10.1111/j.1365-2133.2008.08747.x

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AN - SCOPUS:51849154755

SN - 0007-0963

VL - 159

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JO - British Journal of Dermatology

JF - British Journal of Dermatology

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ER -

A 4-year follow-up study of atopic dermatitis therapy with 0.1% tacrolimus ointment in children and adult patients

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