Statistical recommendations for count, binary, and ordinal data in rare disease cross-over trials

Martin Geroldinger; Johan Verbeeck; Andrew C Hooker; Konstantin E Thiel; Geert Molenberghs; Joakim Nyberg; Johann Bauer; Martin Laimer; Verena Wally; Arne C Bathke; Georg Zimmermann

doi:10.1186/s13023-023-02990-1

Statistical recommendations for count, binary, and ordinal data in rare disease cross-over trials

Martin Geroldinger^* (Erstautor/-in), Johan Verbeeck, Andrew C Hooker, Konstantin E Thiel, Geert Molenberghs, Joakim Nyberg, Johann Bauer (Co-Autor/-in), Martin Laimer (Co-Autor/-in), Verena Wally (Co-Autor/-in), Arne C Bathke, Georg Zimmermann (Letztautor/-in)

^*Korrespondierende/r Autor/-in für diese Arbeit

Publikation: Beitrag in Fachzeitschrift › Originalarbeit › Begutachtung

Abstract

BACKGROUND: Recommendations for statistical methods in rare disease trials are scarce, especially for cross-over designs. As a result various state-of-the-art methodologies were compared as neutrally as possible using an illustrative data set from epidermolysis bullosa research to build recommendations for count, binary, and ordinal outcome variables. For this purpose, parametric (model averaging), semiparametric (generalized estimating equations type [GEE-like]) and nonparametric (generalized pairwise comparisons [GPC] and a marginal model implemented in the R package nparLD) methods were chosen by an international consortium of statisticians.

RESULTS: It was found that there is no uniformly best method for the aforementioned types of outcome variables, but in particular situations, there are methods that perform better than others. Especially if maximizing power is the primary goal, the prioritized unmatched GPC method was able to achieve particularly good results, besides being appropriate for prioritizing clinically relevant time points. Model averaging led to favorable results in some scenarios especially within the binary outcome setting and, like the GEE-like semiparametric method, also allows for considering period and carry-over effects properly. Inference based on the nonparametric marginal model was able to achieve high power, especially in the ordinal outcome scenario, despite small sample sizes due to separate testing of treatment periods, and is suitable when longitudinal and interaction effects have to be considered.

CONCLUSION: Overall, a balance has to be found between achieving high power, accounting for cross-over, period, or carry-over effects, and prioritizing clinically relevant time points.

Originalsprache	Englisch
Seiten (von - bis)	391
Seitenumfang	12
Fachzeitschrift	ORPHANET JOURNAL OF RARE DISEASES
Jahrgang	18
Ausgabenummer	1
DOIs	https://doi.org/10.1186/s13023-023-02990-1
Publikationsstatus	Veröffentlicht - 19 Dez. 2023

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10.1186/s13023-023-02990-1

State-of-the-art statistical design and analysis for maximal success with minimal patient burden in Epidermolysis bullosa trials
Zimmermann, G. J. (Weitere Forschende), Bauer, J. (Leitende(r) Forscher/-in), Geroldinger, M. (Weitere Forschende) & Thiel, K. (Weitere Forschende)
1/01/21 → 1/01/23
Projekt: Forschung

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title = "Statistical recommendations for count, binary, and ordinal data in rare disease cross-over trials",

abstract = "BACKGROUND: Recommendations for statistical methods in rare disease trials are scarce, especially for cross-over designs. As a result various state-of-the-art methodologies were compared as neutrally as possible using an illustrative data set from epidermolysis bullosa research to build recommendations for count, binary, and ordinal outcome variables. For this purpose, parametric (model averaging), semiparametric (generalized estimating equations type [GEE-like]) and nonparametric (generalized pairwise comparisons [GPC] and a marginal model implemented in the R package nparLD) methods were chosen by an international consortium of statisticians.RESULTS: It was found that there is no uniformly best method for the aforementioned types of outcome variables, but in particular situations, there are methods that perform better than others. Especially if maximizing power is the primary goal, the prioritized unmatched GPC method was able to achieve particularly good results, besides being appropriate for prioritizing clinically relevant time points. Model averaging led to favorable results in some scenarios especially within the binary outcome setting and, like the GEE-like semiparametric method, also allows for considering period and carry-over effects properly. Inference based on the nonparametric marginal model was able to achieve high power, especially in the ordinal outcome scenario, despite small sample sizes due to separate testing of treatment periods, and is suitable when longitudinal and interaction effects have to be considered.CONCLUSION: Overall, a balance has to be found between achieving high power, accounting for cross-over, period, or carry-over effects, and prioritizing clinically relevant time points.",

keywords = "Guidance, Repeated measures, Model averaging, Small sample size, NparLD, Rare Diseases, GEE-like semiparametric model, Epidermolysis bullosa simplex, Cross-over, Generalized pairwise comparison (GPC), Recommendation",

author = "Martin Geroldinger and Johan Verbeeck and Hooker, {Andrew C} and Thiel, {Konstantin E} and Geert Molenberghs and Joakim Nyberg and Johann Bauer and Martin Laimer and Verena Wally and Bathke, {Arne C} and Georg Zimmermann",

note = "Geroldinger, Thiel, Zimmermann: Team Biostatistics and Big Medical Data, IDA Lab Salzburg, Paracelsus Medical University, Strubergasse 21, Salzburg, 5020, Austria; Geroldinger: Department of Neurology, Christian Doppler Medical Centre, Full Member of European Reference Network on Rare and Complex Epilepsies EpiCARE, Paracelsus Medical University, Ignaz-Harrer Stra{\ss}e 79, Salzburg, 5020, Austria; Bauer, Laimer:Department of Dermatology and Allergology, Paracelsus Medical University, Salzburg, 5020, Austria; Bauer, Laimer, Wally:B House Austria, Research Program for Molecular Therapy of Genodermatoses, Department of Dermatology and Allergology, University Hospital of the Paracelsus Medical University Salzburg, Salzburg, 5020, Austria; ",

year = "2023",

month = dec,

day = "19",

doi = "10.1186/s13023-023-02990-1",

language = "English",

volume = "18",

pages = "391",

journal = "ORPHANET JOURNAL OF RARE DISEASES",

issn = "1750-1172",

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TY - JOUR

T1 - Statistical recommendations for count, binary, and ordinal data in rare disease cross-over trials

AU - Geroldinger, Martin

AU - Verbeeck, Johan

AU - Hooker, Andrew C

AU - Thiel, Konstantin E

AU - Molenberghs, Geert

AU - Nyberg, Joakim

AU - Bauer, Johann

AU - Laimer, Martin

AU - Wally, Verena

AU - Bathke, Arne C

AU - Zimmermann, Georg

N1 - Geroldinger, Thiel, Zimmermann: Team Biostatistics and Big Medical Data, IDA Lab Salzburg, Paracelsus Medical University, Strubergasse 21, Salzburg, 5020, Austria; Geroldinger: Department of Neurology, Christian Doppler Medical Centre, Full Member of European Reference Network on Rare and Complex Epilepsies EpiCARE, Paracelsus Medical University, Ignaz-Harrer Straße 79, Salzburg, 5020, Austria; Bauer, Laimer:Department of Dermatology and Allergology, Paracelsus Medical University, Salzburg, 5020, Austria; Bauer, Laimer, Wally:B House Austria, Research Program for Molecular Therapy of Genodermatoses, Department of Dermatology and Allergology, University Hospital of the Paracelsus Medical University Salzburg, Salzburg, 5020, Austria;

PY - 2023/12/19

Y1 - 2023/12/19

N2 - BACKGROUND: Recommendations for statistical methods in rare disease trials are scarce, especially for cross-over designs. As a result various state-of-the-art methodologies were compared as neutrally as possible using an illustrative data set from epidermolysis bullosa research to build recommendations for count, binary, and ordinal outcome variables. For this purpose, parametric (model averaging), semiparametric (generalized estimating equations type [GEE-like]) and nonparametric (generalized pairwise comparisons [GPC] and a marginal model implemented in the R package nparLD) methods were chosen by an international consortium of statisticians.RESULTS: It was found that there is no uniformly best method for the aforementioned types of outcome variables, but in particular situations, there are methods that perform better than others. Especially if maximizing power is the primary goal, the prioritized unmatched GPC method was able to achieve particularly good results, besides being appropriate for prioritizing clinically relevant time points. Model averaging led to favorable results in some scenarios especially within the binary outcome setting and, like the GEE-like semiparametric method, also allows for considering period and carry-over effects properly. Inference based on the nonparametric marginal model was able to achieve high power, especially in the ordinal outcome scenario, despite small sample sizes due to separate testing of treatment periods, and is suitable when longitudinal and interaction effects have to be considered.CONCLUSION: Overall, a balance has to be found between achieving high power, accounting for cross-over, period, or carry-over effects, and prioritizing clinically relevant time points.

AB - BACKGROUND: Recommendations for statistical methods in rare disease trials are scarce, especially for cross-over designs. As a result various state-of-the-art methodologies were compared as neutrally as possible using an illustrative data set from epidermolysis bullosa research to build recommendations for count, binary, and ordinal outcome variables. For this purpose, parametric (model averaging), semiparametric (generalized estimating equations type [GEE-like]) and nonparametric (generalized pairwise comparisons [GPC] and a marginal model implemented in the R package nparLD) methods were chosen by an international consortium of statisticians.RESULTS: It was found that there is no uniformly best method for the aforementioned types of outcome variables, but in particular situations, there are methods that perform better than others. Especially if maximizing power is the primary goal, the prioritized unmatched GPC method was able to achieve particularly good results, besides being appropriate for prioritizing clinically relevant time points. Model averaging led to favorable results in some scenarios especially within the binary outcome setting and, like the GEE-like semiparametric method, also allows for considering period and carry-over effects properly. Inference based on the nonparametric marginal model was able to achieve high power, especially in the ordinal outcome scenario, despite small sample sizes due to separate testing of treatment periods, and is suitable when longitudinal and interaction effects have to be considered.CONCLUSION: Overall, a balance has to be found between achieving high power, accounting for cross-over, period, or carry-over effects, and prioritizing clinically relevant time points.

KW - Guidance

KW - Repeated measures

KW - Model averaging

KW - Small sample size

KW - NparLD

KW - Rare Diseases

KW - GEE-like semiparametric model

KW - Epidermolysis bullosa simplex

KW - Cross-over

KW - Generalized pairwise comparison (GPC)

KW - Recommendation

U2 - 10.1186/s13023-023-02990-1

DO - 10.1186/s13023-023-02990-1

M3 - Original Article

C2 - 38115074

SN - 1750-1172

VL - 18

SP - 391

JO - ORPHANET JOURNAL OF RARE DISEASES

JF - ORPHANET JOURNAL OF RARE DISEASES

IS - 1

ER -

Statistical recommendations for count, binary, and ordinal data in rare disease cross-over trials

Abstract

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State-of-the-art statistical design and analysis for maximal success with minimal patient burden in Epidermolysis bullosa trials

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