Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort

Brian M. Feldman; Georges E. Rivard; Paul Babyn; John K.M. Wu; MacGregor Steele; Man Chiu Poon; Robert T. Card; Sara J. Israels; Nicole Laferriere; Kulwant Gill; Anthony K. Chan; Manuel Carcao; Robert J. Klaassen; Stephanie Cloutier; Victoria E. Price; Saunya Dover; Victor S. Blanchette

doi:10.1016/S2352-3026(18)30048-6

Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort

Brian M. Feldman, Georges E. Rivard, Paul Babyn, John K.M. Wu, MacGregor Steele, Man Chiu Poon, Robert T. Card, Sara J. Israels, Nicole Laferriere, Kulwant Gill, Anthony K. Chan, Manuel Carcao, Robert J. Klaassen, Stephanie Cloutier, Victoria E. Price, Saunya Dover, Victor S. Blanchette

Medicine

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33 Citas (Scopus)

Resumen

Background: Severe haemophilia A has high morbidity, and treatment, while effective, is very expensive. We report the 16-year follow-up of the Canadian Hemophilia Prophylaxis Study, which examined the effectiveness of tailored frequency-escalated primary prophylaxis with a focus on health outcomes within the domains of body structures and functions, and activities and participation (according to the WHO International Classification of Functioning, Disability and Health [WHO-ICF] framework) and a view to reducing consumption of costly clotting factor, which accounts for more than 90% of the cost of care of severe haemophilia. Methods: In this longitudinal study, boys with severe haemophilia A from 12 Canadian centres were enrolled at age 1·0–2·5 years. They were treated with standard half-life recombinant factor VIII (SHL-rFVIII), beginning as once-weekly prophylaxis with 50 IU/kg and escalating in frequency (with accompanying dose adjustments) in response to breakthrough bleeding as determined by the protocol. The primary endpoint for this analysis was joint health, as measured by the modified Colorado Child Physical Examination Scores (CCPES) at study end. All analyses were done by intention to treat. The trial is complete, and is registered with ClinicalTrials.gov, number NCT01085344. Findings: Between June 26, 1997, and Jan 30, 2007, 56 boys were enrolled. They were followed for a median of 10·2 years (to a maximum of 16·1 years). Median rFVIII usage was about 3600 IU/kg per year. The median end-of-study CCPES physical examination score was 1 (IQR 1–3; range 0–12) for the left ankle and 1 (1–2; 0–12) for the right ankle, with all other joints having a median score of 0. No treatment-related safety events occurred over the duration of the study, including central venous catheter infections. The median annualised index joint bleeding rate was 0·95 per year (IQR 0·44–1·35; range 0·00–13·43), but 17 (30%) patients had protocol-defined unacceptable breakthrough bleeding at some point during the study. Interpretation: Tailored frequency-escalated prophylaxis leads to very little arthropathy and very good health outcomes within the WHO-ICF domains, and only uses a moderate amount of expensive clotting factor as compared with standard prophylaxis protocols. Some sequelae of bleeding were observed in our cohort, and future studies should consider a more stringent protocol of escalation. Funding: This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer.

Idioma original	English
Páginas (desde-hasta)	e252-e260
Publicación	The Lancet Haematology
Volumen	5
N.º	6
DOI	https://doi.org/10.1016/S2352-3026(18)30048-6
Estado	Published - jun. 2018

Nota bibliográfica

Funding Information:
VSB reports personal fees from Advisory Board Amgen, Bayer, Novo Nordisk, Pfizer, Roche, and Shire; grants from Bioverative and Shire; non-financial support from DSMB, Octapharma, and Shire; and other support from International Prophylaxis Study Group, outside of the submitted work. MC reports grants and personal fees from Biogen/Bioverativ, Bayer, Novo Nordisk, CSL Behring, and Octapharma; and personal fees from Biotest, Baxter/Baxalta/Shire, and Pfizer, outside the submitted work. BMF reports grants from Bayer, during the conduct of the study, and grants from Baxter/Baxalta/Shire, outside the submitted work. RJK reports other support from Amgen, Hoffman-La Roche, Octapharma, Baxalta, Biogen Canada, and Agios Pharmacuetical, outside the submitted work. M-CP has received honoraria for attending advisory board meetings for Bayer, CSL-Behring, Novo Nordisk, Pfizer, Roche, and Shire and has received grant funding from Bayer and CSL-Behring. MS reports personal fees from Bayer and Roche, and personal fees and non-financial support from Baxter/Baxalta/Shire, outside of the submitted work. JKMW reports grants from Bayer Healthcare and CSL Behring; grants and personal fees from Shire; and personal fees from NovoNordisk, Roche, and Octapharma, outside of the submitted work. The remaining authors declare no competing interests.

Funding Information:
We wish to thank the participants of this study, their families, and the staff of the comprehensive care haemophilia treatment centres; without their help and commitment this study would not have been possible. This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer. The study received conference funding from CSL Behring, Bayer, Baxter, and Biogen Idec. BMF holds the Ho Family Research Chair in Autoimmune Diseases. Jennifer Stimec, radiologist (MSK) at the Hospital for Sick Children, independently read all of the x-ray and MRI images used in the analysis for this study. We would like to express our thanks to all the site nurse coordinators, site physiotherapy assessors, and clinical research assistants at the different centres that participated in this study.

Publisher Copyright:
© 2018 Elsevier Ltd

ASJC Scopus Subject Areas

Hematology

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10.1016/S2352-3026(18)30048-6

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Feldman, B. M., Rivard, G. E., Babyn, P., Wu, J. K. M., Steele, M., Poon, M. C., Card, R. T., Israels, S. J., Laferriere, N., Gill, K., Chan, A. K., Carcao, M., Klaassen, R. J., Cloutier, S., Price, V. E., Dover, S., & Blanchette, V. S. (2018). Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort. The Lancet Haematology, 5(6), e252-e260. https://doi.org/10.1016/S2352-3026(18)30048-6

Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort. / Feldman, Brian M.; Rivard, Georges E.; Babyn, Paul et al.
En: The Lancet Haematology, Vol. 5, N.º 6, 06.2018, p. e252-e260.

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

Feldman, BM, Rivard, GE, Babyn, P, Wu, JKM, Steele, M, Poon, MC, Card, RT, Israels, SJ, Laferriere, N, Gill, K, Chan, AK, Carcao, M, Klaassen, RJ, Cloutier, S, Price, VE, Dover, S & Blanchette, VS 2018, 'Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort', The Lancet Haematology, vol. 5, n.º 6, pp. e252-e260. https://doi.org/10.1016/S2352-3026(18)30048-6

@article{e51cf35893ce421098236f47b3e99735,

title = "Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort",

abstract = "Background: Severe haemophilia A has high morbidity, and treatment, while effective, is very expensive. We report the 16-year follow-up of the Canadian Hemophilia Prophylaxis Study, which examined the effectiveness of tailored frequency-escalated primary prophylaxis with a focus on health outcomes within the domains of body structures and functions, and activities and participation (according to the WHO International Classification of Functioning, Disability and Health [WHO-ICF] framework) and a view to reducing consumption of costly clotting factor, which accounts for more than 90% of the cost of care of severe haemophilia. Methods: In this longitudinal study, boys with severe haemophilia A from 12 Canadian centres were enrolled at age 1·0–2·5 years. They were treated with standard half-life recombinant factor VIII (SHL-rFVIII), beginning as once-weekly prophylaxis with 50 IU/kg and escalating in frequency (with accompanying dose adjustments) in response to breakthrough bleeding as determined by the protocol. The primary endpoint for this analysis was joint health, as measured by the modified Colorado Child Physical Examination Scores (CCPES) at study end. All analyses were done by intention to treat. The trial is complete, and is registered with ClinicalTrials.gov, number NCT01085344. Findings: Between June 26, 1997, and Jan 30, 2007, 56 boys were enrolled. They were followed for a median of 10·2 years (to a maximum of 16·1 years). Median rFVIII usage was about 3600 IU/kg per year. The median end-of-study CCPES physical examination score was 1 (IQR 1–3; range 0–12) for the left ankle and 1 (1–2; 0–12) for the right ankle, with all other joints having a median score of 0. No treatment-related safety events occurred over the duration of the study, including central venous catheter infections. The median annualised index joint bleeding rate was 0·95 per year (IQR 0·44–1·35; range 0·00–13·43), but 17 (30%) patients had protocol-defined unacceptable breakthrough bleeding at some point during the study. Interpretation: Tailored frequency-escalated prophylaxis leads to very little arthropathy and very good health outcomes within the WHO-ICF domains, and only uses a moderate amount of expensive clotting factor as compared with standard prophylaxis protocols. Some sequelae of bleeding were observed in our cohort, and future studies should consider a more stringent protocol of escalation. Funding: This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer.",

author = "Feldman, {Brian M.} and Rivard, {Georges E.} and Paul Babyn and Wu, {John K.M.} and MacGregor Steele and Poon, {Man Chiu} and Card, {Robert T.} and Israels, {Sara J.} and Nicole Laferriere and Kulwant Gill and Chan, {Anthony K.} and Manuel Carcao and Klaassen, {Robert J.} and Stephanie Cloutier and Price, {Victoria E.} and Saunya Dover and Blanchette, {Victor S.}",

note = "Funding Information: VSB reports personal fees from Advisory Board Amgen, Bayer, Novo Nordisk, Pfizer, Roche, and Shire; grants from Bioverative and Shire; non-financial support from DSMB, Octapharma, and Shire; and other support from International Prophylaxis Study Group, outside of the submitted work. MC reports grants and personal fees from Biogen/Bioverativ, Bayer, Novo Nordisk, CSL Behring, and Octapharma; and personal fees from Biotest, Baxter/Baxalta/Shire, and Pfizer, outside the submitted work. BMF reports grants from Bayer, during the conduct of the study, and grants from Baxter/Baxalta/Shire, outside the submitted work. RJK reports other support from Amgen, Hoffman-La Roche, Octapharma, Baxalta, Biogen Canada, and Agios Pharmacuetical, outside the submitted work. M-CP has received honoraria for attending advisory board meetings for Bayer, CSL-Behring, Novo Nordisk, Pfizer, Roche, and Shire and has received grant funding from Bayer and CSL-Behring. MS reports personal fees from Bayer and Roche, and personal fees and non-financial support from Baxter/Baxalta/Shire, outside of the submitted work. JKMW reports grants from Bayer Healthcare and CSL Behring; grants and personal fees from Shire; and personal fees from NovoNordisk, Roche, and Octapharma, outside of the submitted work. The remaining authors declare no competing interests. Funding Information: We wish to thank the participants of this study, their families, and the staff of the comprehensive care haemophilia treatment centres; without their help and commitment this study would not have been possible. This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer. The study received conference funding from CSL Behring, Bayer, Baxter, and Biogen Idec. BMF holds the Ho Family Research Chair in Autoimmune Diseases. Jennifer Stimec, radiologist (MSK) at the Hospital for Sick Children, independently read all of the x-ray and MRI images used in the analysis for this study. We would like to express our thanks to all the site nurse coordinators, site physiotherapy assessors, and clinical research assistants at the different centres that participated in this study. Publisher Copyright: {\textcopyright} 2018 Elsevier Ltd",

year = "2018",

month = jun,

doi = "10.1016/S2352-3026(18)30048-6",

language = "English",

volume = "5",

pages = "e252--e260",

journal = "The Lancet Haematology",

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TY - JOUR

T1 - Tailored frequency-escalated primary prophylaxis for severe haemophilia A

T2 - results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort

AU - Feldman, Brian M.

AU - Rivard, Georges E.

AU - Babyn, Paul

AU - Wu, John K.M.

AU - Steele, MacGregor

AU - Poon, Man Chiu

AU - Card, Robert T.

AU - Israels, Sara J.

AU - Laferriere, Nicole

AU - Gill, Kulwant

AU - Chan, Anthony K.

AU - Carcao, Manuel

AU - Klaassen, Robert J.

AU - Cloutier, Stephanie

AU - Price, Victoria E.

AU - Dover, Saunya

AU - Blanchette, Victor S.

N1 - Funding Information: VSB reports personal fees from Advisory Board Amgen, Bayer, Novo Nordisk, Pfizer, Roche, and Shire; grants from Bioverative and Shire; non-financial support from DSMB, Octapharma, and Shire; and other support from International Prophylaxis Study Group, outside of the submitted work. MC reports grants and personal fees from Biogen/Bioverativ, Bayer, Novo Nordisk, CSL Behring, and Octapharma; and personal fees from Biotest, Baxter/Baxalta/Shire, and Pfizer, outside the submitted work. BMF reports grants from Bayer, during the conduct of the study, and grants from Baxter/Baxalta/Shire, outside the submitted work. RJK reports other support from Amgen, Hoffman-La Roche, Octapharma, Baxalta, Biogen Canada, and Agios Pharmacuetical, outside the submitted work. M-CP has received honoraria for attending advisory board meetings for Bayer, CSL-Behring, Novo Nordisk, Pfizer, Roche, and Shire and has received grant funding from Bayer and CSL-Behring. MS reports personal fees from Bayer and Roche, and personal fees and non-financial support from Baxter/Baxalta/Shire, outside of the submitted work. JKMW reports grants from Bayer Healthcare and CSL Behring; grants and personal fees from Shire; and personal fees from NovoNordisk, Roche, and Octapharma, outside of the submitted work. The remaining authors declare no competing interests. Funding Information: We wish to thank the participants of this study, their families, and the staff of the comprehensive care haemophilia treatment centres; without their help and commitment this study would not have been possible. This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer. The study received conference funding from CSL Behring, Bayer, Baxter, and Biogen Idec. BMF holds the Ho Family Research Chair in Autoimmune Diseases. Jennifer Stimec, radiologist (MSK) at the Hospital for Sick Children, independently read all of the x-ray and MRI images used in the analysis for this study. We would like to express our thanks to all the site nurse coordinators, site physiotherapy assessors, and clinical research assistants at the different centres that participated in this study. Publisher Copyright: © 2018 Elsevier Ltd

PY - 2018/6

Y1 - 2018/6

N2 - Background: Severe haemophilia A has high morbidity, and treatment, while effective, is very expensive. We report the 16-year follow-up of the Canadian Hemophilia Prophylaxis Study, which examined the effectiveness of tailored frequency-escalated primary prophylaxis with a focus on health outcomes within the domains of body structures and functions, and activities and participation (according to the WHO International Classification of Functioning, Disability and Health [WHO-ICF] framework) and a view to reducing consumption of costly clotting factor, which accounts for more than 90% of the cost of care of severe haemophilia. Methods: In this longitudinal study, boys with severe haemophilia A from 12 Canadian centres were enrolled at age 1·0–2·5 years. They were treated with standard half-life recombinant factor VIII (SHL-rFVIII), beginning as once-weekly prophylaxis with 50 IU/kg and escalating in frequency (with accompanying dose adjustments) in response to breakthrough bleeding as determined by the protocol. The primary endpoint for this analysis was joint health, as measured by the modified Colorado Child Physical Examination Scores (CCPES) at study end. All analyses were done by intention to treat. The trial is complete, and is registered with ClinicalTrials.gov, number NCT01085344. Findings: Between June 26, 1997, and Jan 30, 2007, 56 boys were enrolled. They were followed for a median of 10·2 years (to a maximum of 16·1 years). Median rFVIII usage was about 3600 IU/kg per year. The median end-of-study CCPES physical examination score was 1 (IQR 1–3; range 0–12) for the left ankle and 1 (1–2; 0–12) for the right ankle, with all other joints having a median score of 0. No treatment-related safety events occurred over the duration of the study, including central venous catheter infections. The median annualised index joint bleeding rate was 0·95 per year (IQR 0·44–1·35; range 0·00–13·43), but 17 (30%) patients had protocol-defined unacceptable breakthrough bleeding at some point during the study. Interpretation: Tailored frequency-escalated prophylaxis leads to very little arthropathy and very good health outcomes within the WHO-ICF domains, and only uses a moderate amount of expensive clotting factor as compared with standard prophylaxis protocols. Some sequelae of bleeding were observed in our cohort, and future studies should consider a more stringent protocol of escalation. Funding: This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer.

AB - Background: Severe haemophilia A has high morbidity, and treatment, while effective, is very expensive. We report the 16-year follow-up of the Canadian Hemophilia Prophylaxis Study, which examined the effectiveness of tailored frequency-escalated primary prophylaxis with a focus on health outcomes within the domains of body structures and functions, and activities and participation (according to the WHO International Classification of Functioning, Disability and Health [WHO-ICF] framework) and a view to reducing consumption of costly clotting factor, which accounts for more than 90% of the cost of care of severe haemophilia. Methods: In this longitudinal study, boys with severe haemophilia A from 12 Canadian centres were enrolled at age 1·0–2·5 years. They were treated with standard half-life recombinant factor VIII (SHL-rFVIII), beginning as once-weekly prophylaxis with 50 IU/kg and escalating in frequency (with accompanying dose adjustments) in response to breakthrough bleeding as determined by the protocol. The primary endpoint for this analysis was joint health, as measured by the modified Colorado Child Physical Examination Scores (CCPES) at study end. All analyses were done by intention to treat. The trial is complete, and is registered with ClinicalTrials.gov, number NCT01085344. Findings: Between June 26, 1997, and Jan 30, 2007, 56 boys were enrolled. They were followed for a median of 10·2 years (to a maximum of 16·1 years). Median rFVIII usage was about 3600 IU/kg per year. The median end-of-study CCPES physical examination score was 1 (IQR 1–3; range 0–12) for the left ankle and 1 (1–2; 0–12) for the right ankle, with all other joints having a median score of 0. No treatment-related safety events occurred over the duration of the study, including central venous catheter infections. The median annualised index joint bleeding rate was 0·95 per year (IQR 0·44–1·35; range 0·00–13·43), but 17 (30%) patients had protocol-defined unacceptable breakthrough bleeding at some point during the study. Interpretation: Tailored frequency-escalated prophylaxis leads to very little arthropathy and very good health outcomes within the WHO-ICF domains, and only uses a moderate amount of expensive clotting factor as compared with standard prophylaxis protocols. Some sequelae of bleeding were observed in our cohort, and future studies should consider a more stringent protocol of escalation. Funding: This study was initially funded by grants from the Medical Research Council of Canada/Pharmaceutical Manufacturers Association of Canada Partnership Fund and the Bayer/Canadian Blood Services/Hema-Quebec Partnership Fund. Subsequent renewals were funded by Bayer.

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Tailored frequency-escalated primary prophylaxis for severe haemophilia A: results of the 16-year Canadian Hemophilia Prophylaxis Study longitudinal cohort

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