Treatment drop-in in a contemporary cohort used to derive cardiovascular risk prediction equations

Jingyuan Liang; Rodney T Jackson; Romana Pylypchuk; Yeunhyang Choi; Claris Chung; Sue Crengle; Pei Gao; Corina Grey; Matire Harwood; Anders Holt; Andrew Kerr; Suneela Mehta; Susan Wells; Katrina Poppe

doi:10.1136/heartjnl-2024-324179

Treatment drop-in in a contemporary cohort used to derive cardiovascular risk prediction equations

Jingyuan Liang, Rodney T Jackson, Romana Pylypchuk, Yeunhyang Choi, Claris Chung, Sue Crengle, Pei Gao, Corina Grey, Matire Harwood, Anders Holt, Andrew Kerr, Suneela Mehta, Susan Wells, Katrina Poppe

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1 Citationer (Scopus)

Abstract

BACKGROUND: No routinely recommended cardiovascular disease (CVD) risk prediction equations have adjusted for CVD preventive medications initiated during follow-up (treatment drop-in) in their derivation cohorts. This will lead to underestimation of risk when equations are applied in clinical practice if treatment drop-in is common. We aimed to quantify the treatment drop-in in a large contemporary national cohort to determine whether equations are likely to require adjustment.

METHODS: Eight de-identified individual-level national health administrative datasets in Aotearoa New Zealand were linked to establish a cohort of almost all New Zealanders without CVD and aged 30-74 years in 2006. Individuals dispensing blood-pressure-lowering and/or lipid-lowering medications between 1 July 2006 and 31 December 2006 (baseline dispensing), and in each 6-month period during 12 years' follow-up to 31 December 2018 (follow-up dispensing), were identified. Person-years of treatment drop-in were determined.

RESULTS: A total of 1 399 348 (80%) out of the 1 746 695 individuals in the cohort were not dispensed CVD medications at baseline. Blood-pressure-lowering and/or lipid-lowering treatment drop-in accounted for 14% of follow-up time in the group untreated at baseline and increased significantly with increasing predicted baseline 5-year CVD risk (12%, 31%, 34% and 37% in <5%, 5-9%, 10-14% and ≥15% risk groups, respectively) and with increasing age (8% in 30-44 year-olds to 30% in 60-74 year-olds).

CONCLUSIONS: CVD preventive treatment drop-in accounted for approximately one-third of follow-up time among participants typically eligible for preventive treatment (≥5% 5-year predicted risk). Equations derived from cohorts with long-term follow-up that do not adjust for treatment drop-in effect will underestimate CVD risk in higher risk individuals and lead to undertreatment. Future CVD risk prediction studies need to address this potential flaw.

Originalsprog	Engelsk
Tidsskrift	Heart (British Cardiac Society)
Vol/bind	110
Udgave nummer	17
Sider (fra-til)	1083-1089
Antal sider	7
ISSN	1355-6037
DOI	https://doi.org/10.1136/heartjnl-2024-324179
Status	Udgivet - 14 aug. 2024

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@article{e143df90c6c4484daccac0d996682a21,

title = "Treatment drop-in in a contemporary cohort used to derive cardiovascular risk prediction equations",

abstract = "BACKGROUND: No routinely recommended cardiovascular disease (CVD) risk prediction equations have adjusted for CVD preventive medications initiated during follow-up (treatment drop-in) in their derivation cohorts. This will lead to underestimation of risk when equations are applied in clinical practice if treatment drop-in is common. We aimed to quantify the treatment drop-in in a large contemporary national cohort to determine whether equations are likely to require adjustment.METHODS: Eight de-identified individual-level national health administrative datasets in Aotearoa New Zealand were linked to establish a cohort of almost all New Zealanders without CVD and aged 30-74 years in 2006. Individuals dispensing blood-pressure-lowering and/or lipid-lowering medications between 1 July 2006 and 31 December 2006 (baseline dispensing), and in each 6-month period during 12 years' follow-up to 31 December 2018 (follow-up dispensing), were identified. Person-years of treatment drop-in were determined.RESULTS: A total of 1 399 348 (80%) out of the 1 746 695 individuals in the cohort were not dispensed CVD medications at baseline. Blood-pressure-lowering and/or lipid-lowering treatment drop-in accounted for 14% of follow-up time in the group untreated at baseline and increased significantly with increasing predicted baseline 5-year CVD risk (12%, 31%, 34% and 37% in <5%, 5-9%, 10-14% and ≥15% risk groups, respectively) and with increasing age (8% in 30-44 year-olds to 30% in 60-74 year-olds).CONCLUSIONS: CVD preventive treatment drop-in accounted for approximately one-third of follow-up time among participants typically eligible for preventive treatment (≥5% 5-year predicted risk). Equations derived from cohorts with long-term follow-up that do not adjust for treatment drop-in effect will underestimate CVD risk in higher risk individuals and lead to undertreatment. Future CVD risk prediction studies need to address this potential flaw.",

keywords = "Humans, Middle Aged, Male, Female, Cardiovascular Diseases/epidemiology, Aged, Risk Assessment/methods, Adult, New Zealand/epidemiology, Heart Disease Risk Factors, Hypolipidemic Agents/therapeutic use, Antihypertensive Agents/therapeutic use",

author = "Jingyuan Liang and Jackson, {Rodney T} and Romana Pylypchuk and Yeunhyang Choi and Claris Chung and Sue Crengle and Pei Gao and Corina Grey and Matire Harwood and Anders Holt and Andrew Kerr and Suneela Mehta and Susan Wells and Katrina Poppe",

note = "{\textcopyright} Author(s) (or their employer(s)) 2024. No commercial re-use. See rights and permissions. Published by BMJ.",

year = "2024",

month = aug,

day = "14",

doi = "10.1136/heartjnl-2024-324179",

language = "English",

volume = "110",

pages = "1083--1089",

journal = "Heart (British Cardiac Society)",

issn = "1355-6037",

publisher = "BMJ Publishing Group",

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TY - JOUR

T1 - Treatment drop-in in a contemporary cohort used to derive cardiovascular risk prediction equations

AU - Liang, Jingyuan

AU - Jackson, Rodney T

AU - Pylypchuk, Romana

AU - Choi, Yeunhyang

AU - Chung, Claris

AU - Crengle, Sue

AU - Gao, Pei

AU - Grey, Corina

AU - Harwood, Matire

AU - Holt, Anders

AU - Kerr, Andrew

AU - Mehta, Suneela

AU - Wells, Susan

AU - Poppe, Katrina

N1 - © Author(s) (or their employer(s)) 2024. No commercial re-use. See rights and permissions. Published by BMJ.

PY - 2024/8/14

Y1 - 2024/8/14

N2 - BACKGROUND: No routinely recommended cardiovascular disease (CVD) risk prediction equations have adjusted for CVD preventive medications initiated during follow-up (treatment drop-in) in their derivation cohorts. This will lead to underestimation of risk when equations are applied in clinical practice if treatment drop-in is common. We aimed to quantify the treatment drop-in in a large contemporary national cohort to determine whether equations are likely to require adjustment.METHODS: Eight de-identified individual-level national health administrative datasets in Aotearoa New Zealand were linked to establish a cohort of almost all New Zealanders without CVD and aged 30-74 years in 2006. Individuals dispensing blood-pressure-lowering and/or lipid-lowering medications between 1 July 2006 and 31 December 2006 (baseline dispensing), and in each 6-month period during 12 years' follow-up to 31 December 2018 (follow-up dispensing), were identified. Person-years of treatment drop-in were determined.RESULTS: A total of 1 399 348 (80%) out of the 1 746 695 individuals in the cohort were not dispensed CVD medications at baseline. Blood-pressure-lowering and/or lipid-lowering treatment drop-in accounted for 14% of follow-up time in the group untreated at baseline and increased significantly with increasing predicted baseline 5-year CVD risk (12%, 31%, 34% and 37% in <5%, 5-9%, 10-14% and ≥15% risk groups, respectively) and with increasing age (8% in 30-44 year-olds to 30% in 60-74 year-olds).CONCLUSIONS: CVD preventive treatment drop-in accounted for approximately one-third of follow-up time among participants typically eligible for preventive treatment (≥5% 5-year predicted risk). Equations derived from cohorts with long-term follow-up that do not adjust for treatment drop-in effect will underestimate CVD risk in higher risk individuals and lead to undertreatment. Future CVD risk prediction studies need to address this potential flaw.

AB - BACKGROUND: No routinely recommended cardiovascular disease (CVD) risk prediction equations have adjusted for CVD preventive medications initiated during follow-up (treatment drop-in) in their derivation cohorts. This will lead to underestimation of risk when equations are applied in clinical practice if treatment drop-in is common. We aimed to quantify the treatment drop-in in a large contemporary national cohort to determine whether equations are likely to require adjustment.METHODS: Eight de-identified individual-level national health administrative datasets in Aotearoa New Zealand were linked to establish a cohort of almost all New Zealanders without CVD and aged 30-74 years in 2006. Individuals dispensing blood-pressure-lowering and/or lipid-lowering medications between 1 July 2006 and 31 December 2006 (baseline dispensing), and in each 6-month period during 12 years' follow-up to 31 December 2018 (follow-up dispensing), were identified. Person-years of treatment drop-in were determined.RESULTS: A total of 1 399 348 (80%) out of the 1 746 695 individuals in the cohort were not dispensed CVD medications at baseline. Blood-pressure-lowering and/or lipid-lowering treatment drop-in accounted for 14% of follow-up time in the group untreated at baseline and increased significantly with increasing predicted baseline 5-year CVD risk (12%, 31%, 34% and 37% in <5%, 5-9%, 10-14% and ≥15% risk groups, respectively) and with increasing age (8% in 30-44 year-olds to 30% in 60-74 year-olds).CONCLUSIONS: CVD preventive treatment drop-in accounted for approximately one-third of follow-up time among participants typically eligible for preventive treatment (≥5% 5-year predicted risk). Equations derived from cohorts with long-term follow-up that do not adjust for treatment drop-in effect will underestimate CVD risk in higher risk individuals and lead to undertreatment. Future CVD risk prediction studies need to address this potential flaw.

KW - Humans

KW - Middle Aged

KW - Male

KW - Female

KW - Cardiovascular Diseases/epidemiology

KW - Aged

KW - Risk Assessment/methods

KW - Adult

KW - New Zealand/epidemiology

KW - Heart Disease Risk Factors

KW - Hypolipidemic Agents/therapeutic use

KW - Antihypertensive Agents/therapeutic use

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U2 - 10.1136/heartjnl-2024-324179

DO - 10.1136/heartjnl-2024-324179

M3 - Journal article

C2 - 38960588

SN - 1355-6037

VL - 110

SP - 1083

EP - 1089

JO - Heart (British Cardiac Society)

JF - Heart (British Cardiac Society)

IS - 17

ER -

Treatment drop-in in a contemporary cohort used to derive cardiovascular risk prediction equations

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