Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial

Pierluigi Tricoci; Megan Neely; Michael J. Whitley; Leonard C. Edelstein; Lukas M. Simon; Chad Shaw; Paolo Fortina; David J. Moliterno; Paul W. Armstrong; Philip Aylward; Harvey White; Frans Van de Werf; Lisa K. Jennings; Lars Wallentin; Claes Held; Robert A. Harrington; Kenneth W. Mahaffey; Paul F. Bray

doi:10.1016/j.bcmd.2018.07.004

Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial

Pierluigi Tricoci
, Megan Neely
, Michael J. Whitley
, Leonard C. Edelstein
, Lukas M. Simon
, Chad Shaw
, Paolo Fortina
, David J. Moliterno
, Paul W. Armstrong
, Philip Aylward
, Harvey White
, Frans Van de Werf
, Lisa K. Jennings
, Lars Wallentin
, Claes Held
, Robert A. Harrington
, Kenneth W. Mahaffey
, Paul F. Bray

Producción científica: Article › revisión exhaustiva

11 Citas (Scopus)

Resumen

Variation in platelet response to thrombin may affect the safety and efficacy of PAR antagonism. The Thr120 variant of the common single nucleotide polymorphism (SNP) rs773902 in the protease-activated receptor (PAR) 4 gene is associated with higher platelet aggregation compared to the Ala120 variant. We investigated the relationship between the rs773902 SNP with major bleeding and ischemic events, safety, and efficacy of PAR1 inhibition in 6177 NSTE ACS patients in the TRACER trial. There was a lower rate of GUSTO moderate/severe bleeding in patients with the Thr120 variant. The difference was driven by a lower rate in the smaller homozygous group (recessive model, HR 0.13 [0.02–0.92] P = 0.042). No significant differences were observed in the ischemic outcomes. The excess in bleeding observed with PAR1 inhibition was attenuated in patients with the Thr120 variant, but the interactions were not statistically significant. In summary, lower major bleeding rates were observed in the overall TRACER cohort with the hyperreactive PAR4 Thr120 variant. The increase in bleeding with vorapaxar was attenuated with the Thr120 variant, but we could not demonstrate an interaction with PAR1 inhibition. These findings warrant further exploration, including those of African ancestry where the A allele (Thr120) frequency is ~65%.

Idioma original	English
Páginas (desde-hasta)	37-43
Número de páginas	7
Publicación	Blood Cells, Molecules, and Diseases
Volumen	72
DOI	https://doi.org/10.1016/j.bcmd.2018.07.004
Estado	Published - sept 2018

Nota bibliográfica

Publisher Copyright:
© 2018 Elsevier Inc.

Financiación

This work was supported by the National Institutes of Health [grant number HL102482]; the University of Utah Division of Hematology and Hematologic Malignancies; and the Cardeza Foundation for Hematologic Research. This work was supported by the National Institutes of Health [grant number HL102482 ]; the University of Utah Division of Hematology and Hematologic Malignancies; and the Cardeza Foundation for Hematologic Research.

Financiadores	Número del financiador
Cardeza Foundation for Hematologic Research
University of Utah Division of Hematology and Hematologic Malignancies
National Institutes of Health (NIH)
National Heart, Lung, and Blood Institute (NHLBI)	R01HL102482
University of Utah

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Hematology
Cell Biology

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10.1016/j.bcmd.2018.07.004

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Tricoci, P., Neely, M., Whitley, M. J., Edelstein, L. C., Simon, L. M., Shaw, C., Fortina, P., Moliterno, D. J., Armstrong, P. W., Aylward, P., White, H., Van de Werf, F., Jennings, L. K., Wallentin, L., Held, C., Harrington, R. A., Mahaffey, K. W., & Bray, P. F. (2018). Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial. Blood Cells, Molecules, and Diseases, 72, 37-43. https://doi.org/10.1016/j.bcmd.2018.07.004

@article{519e3dfc70464d079407adc5dc001f4c,

title = "Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial",

abstract = "Variation in platelet response to thrombin may affect the safety and efficacy of PAR antagonism. The Thr120 variant of the common single nucleotide polymorphism (SNP) rs773902 in the protease-activated receptor (PAR) 4 gene is associated with higher platelet aggregation compared to the Ala120 variant. We investigated the relationship between the rs773902 SNP with major bleeding and ischemic events, safety, and efficacy of PAR1 inhibition in 6177 NSTE ACS patients in the TRACER trial. There was a lower rate of GUSTO moderate/severe bleeding in patients with the Thr120 variant. The difference was driven by a lower rate in the smaller homozygous group (recessive model, HR 0.13 [0.02–0.92] P = 0.042). No significant differences were observed in the ischemic outcomes. The excess in bleeding observed with PAR1 inhibition was attenuated in patients with the Thr120 variant, but the interactions were not statistically significant. In summary, lower major bleeding rates were observed in the overall TRACER cohort with the hyperreactive PAR4 Thr120 variant. The increase in bleeding with vorapaxar was attenuated with the Thr120 variant, but we could not demonstrate an interaction with PAR1 inhibition. These findings warrant further exploration, including those of African ancestry where the A allele (Thr120) frequency is \textasciitilde{}65\%.",

keywords = "Bleeding, PAR1, PAR4, Pharmacogenetics, Platelets",

author = "Pierluigi Tricoci and Megan Neely and Whitley, \{Michael J.\} and Edelstein, \{Leonard C.\} and Simon, \{Lukas M.\} and Chad Shaw and Paolo Fortina and Moliterno, \{David J.\} and Armstrong, \{Paul W.\} and Philip Aylward and Harvey White and \{Van de Werf\}, Frans and Jennings, \{Lisa K.\} and Lars Wallentin and Claes Held and Harrington, \{Robert A.\} and Mahaffey, \{Kenneth W.\} and Bray, \{Paul F.\}",

note = "Publisher Copyright: {\textcopyright} 2018 Elsevier Inc.",

year = "2018",

month = sep,

doi = "10.1016/j.bcmd.2018.07.004",

language = "English",

volume = "72",

pages = "37--43",

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Tricoci, P, Neely, M, Whitley, MJ, Edelstein, LC, Simon, LM, Shaw, C, Fortina, P, Moliterno, DJ, Armstrong, PW, Aylward, P, White, H, Van de Werf, F, Jennings, LK, Wallentin, L, Held, C, Harrington, RA, Mahaffey, KW & Bray, PF 2018, 'Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial', Blood Cells, Molecules, and Diseases, vol. 72, pp. 37-43. https://doi.org/10.1016/j.bcmd.2018.07.004

TY - JOUR

T1 - Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome

T2 - Analysis from the TRACER trial

AU - Tricoci, Pierluigi

AU - Neely, Megan

AU - Whitley, Michael J.

AU - Edelstein, Leonard C.

AU - Simon, Lukas M.

AU - Shaw, Chad

AU - Fortina, Paolo

AU - Moliterno, David J.

AU - Armstrong, Paul W.

AU - Aylward, Philip

AU - White, Harvey

AU - Van de Werf, Frans

AU - Jennings, Lisa K.

AU - Wallentin, Lars

AU - Held, Claes

AU - Harrington, Robert A.

AU - Mahaffey, Kenneth W.

AU - Bray, Paul F.

PY - 2018/9

Y1 - 2018/9

N2 - Variation in platelet response to thrombin may affect the safety and efficacy of PAR antagonism. The Thr120 variant of the common single nucleotide polymorphism (SNP) rs773902 in the protease-activated receptor (PAR) 4 gene is associated with higher platelet aggregation compared to the Ala120 variant. We investigated the relationship between the rs773902 SNP with major bleeding and ischemic events, safety, and efficacy of PAR1 inhibition in 6177 NSTE ACS patients in the TRACER trial. There was a lower rate of GUSTO moderate/severe bleeding in patients with the Thr120 variant. The difference was driven by a lower rate in the smaller homozygous group (recessive model, HR 0.13 [0.02–0.92] P = 0.042). No significant differences were observed in the ischemic outcomes. The excess in bleeding observed with PAR1 inhibition was attenuated in patients with the Thr120 variant, but the interactions were not statistically significant. In summary, lower major bleeding rates were observed in the overall TRACER cohort with the hyperreactive PAR4 Thr120 variant. The increase in bleeding with vorapaxar was attenuated with the Thr120 variant, but we could not demonstrate an interaction with PAR1 inhibition. These findings warrant further exploration, including those of African ancestry where the A allele (Thr120) frequency is ~65%.

AB - Variation in platelet response to thrombin may affect the safety and efficacy of PAR antagonism. The Thr120 variant of the common single nucleotide polymorphism (SNP) rs773902 in the protease-activated receptor (PAR) 4 gene is associated with higher platelet aggregation compared to the Ala120 variant. We investigated the relationship between the rs773902 SNP with major bleeding and ischemic events, safety, and efficacy of PAR1 inhibition in 6177 NSTE ACS patients in the TRACER trial. There was a lower rate of GUSTO moderate/severe bleeding in patients with the Thr120 variant. The difference was driven by a lower rate in the smaller homozygous group (recessive model, HR 0.13 [0.02–0.92] P = 0.042). No significant differences were observed in the ischemic outcomes. The excess in bleeding observed with PAR1 inhibition was attenuated in patients with the Thr120 variant, but the interactions were not statistically significant. In summary, lower major bleeding rates were observed in the overall TRACER cohort with the hyperreactive PAR4 Thr120 variant. The increase in bleeding with vorapaxar was attenuated with the Thr120 variant, but we could not demonstrate an interaction with PAR1 inhibition. These findings warrant further exploration, including those of African ancestry where the A allele (Thr120) frequency is ~65%.

KW - Bleeding

KW - PAR1

KW - PAR4

KW - Pharmacogenetics

KW - Platelets

UR - https://www.scopus.com/pages/publications/85050386628

UR - https://www.scopus.com/pages/publications/85050386628#tab=citedBy

U2 - 10.1016/j.bcmd.2018.07.004

DO - 10.1016/j.bcmd.2018.07.004

M3 - Article

C2 - 30055940

AN - SCOPUS:85050386628

SN - 1079-9796

VL - 72

SP - 37

EP - 43

JO - Blood Cells, Molecules, and Diseases

JF - Blood Cells, Molecules, and Diseases

ER -

Effects of genetic variation in protease activated receptor 4 after an acute coronary syndrome: Analysis from the TRACER trial

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Nota bibliográfica

Financiación

ASJC Scopus subject areas

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