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34 research outputs found

Elevation of plasma phospholipid transfer protein in transgenic mice increases VLDL secretion

Author: Crom M.P.G. (Rini) de
Gent T. (Teus) van
Haperen M.J. (Rien) van
Lankhuizen I.M. (Inge)
Lie J. (Jessica)
Scheek L. (Leo)
Tol A. (Arie) van
Publication venue
Publication date: 01/01/2002
Field of study

Two lipid transfer proteins are active in human plasma, cholesteryl ester transfer protein (CETP), and phospholipid transfer protein (PLTP). Mice by nature do not express CETP. Additional inactivation of the PLTP gene resulted in reduced secretion of VLDL and subsequently in decreased susceptibility to diet-induced atherosclerosis. The aim of this study is to assess possible effects of differences in PLTP expression on VLDL secretion in mice that are proficient in CETP and PLTP. We compared human CETP transgenic (huCETPtg) mice with mice expressing both human lipid transfer proteins (huCETPtg/huPLTPtg). Plasma cholesterol in huCETPtg mice was 1.5-fold higher compared with huCETPtg/huPLTPtg mice (P < 0.001). This difference was mostly due to a lower HDL level in the huCETPtg/huPLTPtg mice, which subsequently could lead to the somewhat decreased CETP activity and concentration that was found in huCETPtg/huPLTPtg mice (P < 0.05). PLTP activity was 2.8-fold increased in these animals (P < 0.001). The human PLTP concentration was 5 microg/ml. Moderate overexpression of PLTP resulted in a 1.5-fold higher VLDL secretion compared with huCETPtg mice (P < 0.05). The composition of nascent VLDL was similar in both strains. These results indicate that elevated PLTP activity in huCETPtg mice results in an increase in VLDL secretion. In addition, PLTP overexpression decreases plasma HDL cholesterol as well as CETP

EUR Research Repository

Erasmus University Digital Repository

Evaluation of phospholipid transfer protein and cholesteryl ester transfer protein as contributors to the generation of pre beta-high-density lipoproteins

Author: Crom M.P.G. (Rini) de
Ehnholm C. (Christian)
Gent T. (Teus) van
Haperen M.J. (Rien) van
Jansen H. (Hans)
Jauhiainen M.
Lie J. (Jessica)
Scheek L. (Leo)
Tol A. (Arie) van
Publication venue
Publication date: 01/01/2001
Field of study

High-density lipoproteins (HDLs) are considered anti-atherogenic because they mediate peripheral cell cholesterol transport to the liver for excretion and degradation. An important step in this reverse cholesterol-transport pathway is the uptake of cellular cholesterol by a specific subclass of small, lipid-poor apolipoprotein A-I particles designated pre beta-HDL. The two lipid-transfer proteins present in human plasma, cholesteryl ester transfer protein (CETP) and phospholipid transfer protein (PLTP), have both been implicated in the formation of pre beta-HDL. In order to investigate the relative contribution of each of these proteins, we used transgenic mouse models. Comparisons were made between human CETP transgenic mice (huCETPtg), human PLTP transgenic mice (huPLTPtg) and mice transgenic for both lipid-transfer proteins (huCETPtg/huPLTPtg). These animals showed elevated plasma levels of CETP activity, PLTP activity or both activities, respectively. We evaluated the generation of pre beta-HDL in mouse plasma by immunoblotting and crossed immuno-electrophoresis. Generation of pre beta-HDL was equal in huCETPtg and wild-type mice. In contrast, in huPLTPtg and huCETPtg/huPLTPtg mice, pre beta-HDL generation was 3-fold higher than in plasma from either wild-type or huCETPtg mice. Our findings demonstrate that, of the two plasma lipid-transfer proteins, PLTP rather than CETP is responsible for the generation of pre beta-HDL. These data support the hypothesis of a role for PLTP in the initial stage of reverse cholesterol transport

Erasmus University Digital Repository

Biological and clinical insights from genetics of insomnia symptoms

Author: Anderson Simon G.
Aragam Krishna G.
Beaumont Robin N.
Bechtold David A.
Bowden Jack
Bragantini Daniela
Brumpton Ben
Cade Brian E.
Dashti Hassan S.
Engstrom Morten
Frayling Timothy M.
Fritsche Lars
Gabrielsen Maiken E.
Guzey Ismail C.
Haas Mary
Hees Vincent T. van
Hveem Kristian
Janszky Imre
Johnsen Marianne B.
Jones Samuel E.
Kallestad Havard
Kathiresan Sekar
Kyle Simon D.
Lane Jacqueline M.
Lawlor Deborah A.
Lie Marie U.
Little Max A.
Loudon Andrew S.
Luik Annemarie I
Martinsen Amy E.
Nielsen Jonas B.
Nilsen Kristian B.
Patel Krunal
Pedersen Linda M.
Purcell Shaun
Ray David W.
Redline Susan
Richmond Rebecca C.
Rutter Martin K.
Sand Trond
Saxena Richa
Scheer Frank A. J. L.
Schormair Barbara
Sivertsen Borge
Skogholt Anne H.
Song Yanwei
Spiegelhalder Kai
Strand Linn B.
Tyrrell Jessica
Wang Heming
Weedon Michael N.
Willer Cristen J.
Winkelman John W.
Winkelmann Juliane
Winsvold Bendik S.
Wood Andrew R.
Zhao Chen
Zhou Wei
Zwart John-Anker
Publication venue: Ludwig-Maximilians-Universität München
Publication date: 01/01/2019
Field of study

Insomnia is a common disorder linked with adverse long-term medical and psychiatric outcomes. The underlying pathophysiological processes and causal relationships of insomnia with disease are poorly understood. Here we identified 57 loci for self-reported insomnia symptoms in the UK Biobank (n = 453,379) and confirmed their effects on self-reported insomnia symptoms in the HUNT Study (n = 14,923 cases and 47,610 controls), physician-diagnosed insomnia in the Partners Biobank (n = 2,217 cases and 14,240 controls), and accelerometer-derived measures of sleep efficiency and sleep duration in the UK Biobank (n = 83,726). Our results suggest enrichment of genes involved in ubiquitin-mediated proteolysis and of genes expressed in multiple brain regions, skeletal muscle, and adrenal glands. Evidence of shared genetic factors was found between frequent insomnia symptoms and restless legs syndrome, aging, and cardiometabolic, behavioral, psychiatric, and reproductive traits. Evidence was found for a possible causal link between insomnia symptoms and coronary artery disease, depressive symptoms, and subjective well-being

Open Access LMU

Effects of Anacetrapib in Patients with Atherosclerotic Vascular Disease

Author: Aaltonen M
Abdur Rahman M
Abell T
Abide W. Jr
Acheatel R
Achiri P
Acon J
Adams T
Affinito S
Agarwal S
Aggarwal K
Aggarwal R
Ahlström P
Ahmad A
Ahmed M
Aillon C
Airaksinen A
Ait-sadi R
Akers J
Al-jumaily J
Albers C
Albert M
Alberti A
Alexander T
Alford C
Algotsson L
Allen T
Allworth M
Almond E
Aloisi A
Alternburg C
Alton M
Amin J
Amundson A
Andersen K
Andersen M
Anderson E
Anderson G
Anderson R
Anderson T
Andersson H
Andersson L
Andreo J
Andres C
Andresen D
Andrews G
Andrews L
Andrews R
Andrioli V
Angermann Ce
Annas T
Ansell V
Antonio-drabek C
Antonishen D
Antonishen M
Anuschek V
Appel Kf
Appel S
Appleyard D
Archer A
Armitage J
Armstrong L
Armstrong M
Arnesson K
Arnold M
Arora P
Arp H
Asbill B
Ashbrook-raby C
Ashton L
Assarsson E
Audet K
Augenbraun C
Aung HNIN THANDA
Auscher S
Ausner J
Aviles R
Awasty V
Axelsson U
Ayers S
Ayub H
Babar G
Babington G
Backlund M
Badal B
Baggiore C
Baghiana S
Bai H
Bai J
Baigent C
Baillargeon G
Bakbak A
Baker S
Baldin Mg
Baldini E
Baldwin E
Ballantyne C
Baltic A
Banerjee S
Bang Hansen M
Banks K
Bansilal S
Barkley-daughtry S
Barnes D
Barnes E
Barnett S
Baroni Claudio
Barry S
Barter P
Bartolomei Mecatti B
Barton I
Barton J
Baré C
Bashton D
Basler M
Bastani L
Basvi P
Batchlett K
Bateman S
Battistelli E
Baty J
Bauersachs J
Bauman A
Bavendiek U
Baxter A
Bayly G
Bays H
Beasley T
Beck P
Beck S
Becker P
Beebe S
Been M
Begg R
Behm K
Beilker J
Beißner S
Bekfani T
Belanger B
Belew K
Bellaby J
Bellamy C
Bellini S
Beneat Am
Benedetto K
Benoni S
Bentivenga L
Benton R
Berg Schmidt E
Berg-johansen J
Berge C
Bergengen L
Bergmark B
Bergmark C
Bergsten P
Bergström Ml
Bergström O
Bergvall L
Bernardinangeli M
Bernstein R
Berry C
Berry M
Bertoli D
Bertram W
Bescak D
Bescak K
Betzl G
Bhargava A
Bhargava R
Bhatia
Bian B
Bian H
Bian X
Bianchini Filippo
Bibi A
Bies J
Bigelow A
Biggers J
Bilazarian S
Billings C
Binley E
Biondi A
Bird C
Birner C
Bisceglia T
Bittar N
Bittel B
Bitzer V
Biundo V
Bjerge Kaspersen B
Bjergo J
Bjorkas A
Björkman-larnefeldt M
Bjørhovde V
Black L
Blackwood S
Blake J
Blankenberg S
Blaustein R
Blechert Å
Bloksgaard Nilesen S
Blower G
Board J
Boccalandro F
Boccati S
Boelmans K
Boesgaard T
Boggs L
Bohn A
Bohula May E
Bolzani V
Boman K
Bongartz A
Booth J
Borg L
Borucki K
Bosiljanoff E
Bosiljanoff P
Bosnjak B
Bossaers J
Boulware W
Bourhaial H
Bowman L
Bowsher Brown K
Bowsher-brown K
Brachmann J
Bradley A
Brady R
Brandon P
Braun-dullaeus R
Braunwald E
Bray C
Breakspear S
Breakwell L
Brennan G
Brenner S
Bretton E
Brettschneider B
Breunig M
Brewster A
Brian S
Brigden G
Briggs S
Brilloff S
Brink-kjaer T
Broadway K
Broberg M
Bromberger L
Brooks J
Brooks-wolfe A
Brown C
Brown D
Brown E
Brown J
Brown L
Brown M
Brown R
Brown T
Brownlow T
Brueggemann B
Bruney C
Bryan A
Bryan S
Bryson V
Bu Y
Buccolieri M
Buchholz M
Buckley C
Buda M
Buerger M
Buesing M
Bukoski K
Bulbulia R
Bunn D
Buresh R
Burgess A
Burke A
Burkhardt V
Burns S
Burog W
Bursey E
Burton C
Bushong D
Butler E
Butler R
Butman S
Byng-hollander E
Bönigk H
Börjesson M
Cai J
Cakir M
Caldarola P
Calhoun E
Call T
Camerer M
Campbell A
Campbell Evan
Campey L
Campidonico U
Cannon Cp
Canto J
Cao W
Capponi E
Capps N
Capstraw E
Caranzetti F
Carey C
CARIDAD HERNANDEZ JOSE MANUEL
Carlos S
Carlsen H
Carlsson M
Caro H
Carrington M
Carroll A
Carter L
Carver A
Casey MAEVE ANN
Casey MAEVE ANN
Casolo G
Castedal H
Castro-foskett K
Cathcart C
Cauthren T
Cavender M
Cawley P
Cayler J
Cebe J
Cederholm Ac
Centofante L
Ceresa M
Cesanelli R
Ceseri M
Cha J
Cha L
Chackathayil J
Chai X
Chambers J
Chausse I
Chavagnon T
Che H
Chehayeb R
Chen F
Chen G
Chen L
Chen Minghe
Chen Weipeng
Chen X
Chen Y
Chen Z
Cheng C
Cheng Y
Cherian G
Cherrico M
Chi L
Chidambara H
Childs A
Chiodi Riccardo
Chirio C
Chmilewski S
Christensen A
Christensen B
Christensen S
Chu Y
Chun-furlong D
Chung K
Chung R
Ciampanelli E
Ciuica S
Clark A
Clark S
Clark W
Clarke R
Claxton E. Jr
Clayton-evans L
Clemens L
Clements M
Clemmensen P
Cleveland T
Cleverley P
Cluley C
Coates G
Cobb L
Cochrane H
Cockram L
Cockrell D
Cohen R
Colacone T
Colfer H
Colhoun H
Colicchia J
Collet A
Collins J
Collins R
Collins S
Collis W
Cong H
Connors D
Constance C
Conteh V
Contreras S
Cook T
Cooke B
Coombs V
Cooper I
Cooper J
Cooper L
Cooper M
Corbelli J
Corcoran B
Corneal C
Cosmi F
Cox J
Cox R
Craig M
Craig S
Crandall L
Creamer J
Crescenti C
Crews C
Crisci C
Crivellari ADAM MARIA ROMANO
Crouch S
Crowther J
Cryderman A
Cucchi GIANNI MARIO
Cui G
Cui R
Cui Z
Cummings J
Cureton L
Curless R
Curtis J
Cusner H
Custer C
Cyr J
Czihal M
D'Antuono C
Dabrowski J
Dagher E
Dai H
Dalal P
Dalton P
Danel L
Danesh-pour S
Daniels C
Danish Rizvi M
Darlington H
Darrel-asherel E
Davey P
David M
Davidson A
Davidson S
Davies L
Davies M
Davis A
Davis K
Davis M
Dawe C
Dawkins Hughes S
Dayanandan R
De Boer I
De Burca B
De Donno O
De La Garza J
De Lorenzi E
De Matteis C
De Servi S
De Silva R
Dechert M
Defosse C
Defraia C
Del Mastro E
Dela Cruz C
Delgado T
Delozier A
Delucca P
Demets D
Deng X
Dengler T
Desai N
Desai V
Desantis J
Deslongchamp F
Desousa C
Destefano R
Dettmer M
Dhaliwal M
Di Biase M
DI BUONO Antonio
Di Donato A
Di Matteo C
Di Pasquale G
Di Ruocco M
Diao Q
Diaz L
Dickinson RONALD CELESTE
Dieckheuer U
Dietrich D
Diget H
Dignon C
Dinesen P
Ding S
Dionisopoulos P
Dixon L
Dolan M
Domercant J
Domingue N
Donahoe S
Donaldson D
Dong Yingtian
Donley B
Donlin A
Donà P
Doty B
Doucette W
Doughty A
Douglas J
Downing J
Drephal C
Drexler A
Drexler M
Drouin K
Drösch H
Du N
Du W
Du Y
Duan L
Dubal S
Dugan B
Dulea I
Dumais S
Dungca E
Dunne A
Durì G
Dy J
Dyer H
Dziekonski A
Düngen Hd
Easterling A
Ebert J
Edgell R
Edvardsen L
Edwards M
Edwards S
Edwards T
Egenrieder S
Egresits J
Egstrup K
Eiben P
Eichinger G
Einhorn D
Eisen A
Eisenberg D
Ek I
Ekholm L
Elberg B
Eld M
Elliot K
Eloranta E
Emberson J
Emery P
Emmens K
Enebakk T
Engbjerg Andersen M
Ensminger E
Erickson B
Erie G
Eriksson A
Eriksson K
Eronen S
Erstad O
Ertl G
Ervin J
Ervin W
Esaki J
Eshaghian S
Eskridge L
Eubanks C
Euler K
Evans S
Evans-gay S
Evenson C
Fabbri Giorgio
Fahrig A
Fajardo-moser M
Falco M
Fam M
Fan P
Fang X
Fanola C
Fantony N
Farr S
Fathers S
Fattore L
Feest K
Feger J
Fehling K
Feldmann C
Felici A
Felmeden L
Felten W
Felthaus B
Feng F
Feng J
Feng T
Ferguson D
Fernando D
Ferree L
Ferreira J
Ferruzzi P
Festerling E
Ficarra R
Field A
Filippini E
Filorizzo G
Fink P
Finnegan L
Finney
Fischer L
Fish P
Fisher E
Fisher M
Fisscher D
Fitchet A
Flagstad E
Flanery V
Fleming N
Fleming S
Fletcher L
Fleury C
Flores A
Foley J
Fontaine S
Ford-tarlton M
Forsberg K
Forster S
Fortney T
Foster B
Foster T
Foster V
Fox B
Fox C
Fox H
Fox L
Foxton J
Francis Matthew
Frank S
Fraser E
Frattini Sabrina
Frederick K
Freeman R
French H
Fresco C
Frew S
Fritsch S
Fritschka M
Froberg L
Frost L
Fruge A
Fu Q
Fu X
Fuerst-carter K
Fuller J
Fullerton D
Fulton J
Gabbert E
Gaede L
Galietti M
Galindo M
Galla A
Gallegos D
Gallivan A
Gammelmark A
Gammon R
Gang X
Gao Y
Garceau J
GARCIA MARTIN PATRICIA CAROLINA
Garcia H
Garrison K
Garza A
Gates S
Gattone M
Gault J
Gauthier M
Gauthier T
Gaviani P
Ge Z
Gearld K
Gebauer R
Gebhardt S
Gelernt M
Genest J
Gennusa C
Gent S
George S
Geraldo-abache A
Gerber G
German M
Gervasio B
Gesla J
Gessler A
Ghitis A
GIACOMUZZI MOORE Bianca
Giagnoni E
Gianatti E
Giannuzzi P
Gianonatti C
Gibney K
Gibson A
Gilbert L
Gilbert S
Gilley J
Gilmore R
Girardi A
Gislason G
Giugliano R
Gjellefall B
Gluck J
Gneiting A
Godfrey C
Goebel U
Goeres M
Goetz C
Goldscher D
Goldstein M
Golledge S
GOMEZ MARTINEZ MARIA VALENTINA
Gomez A
Goodenough OLIVER RAMSDELL
Goodwin N
Gordon A
Gordon J
Gordon R
Gordon T
Gorini M
Gorman C
Gorsuch A
Gosselin G
Goto S
Gottschalck H
Gour R
Grabmaier U
Graf E
Graf K
Graf R
Graf T
Grande P
Granger C
Graversen K
Gray A
Gray M
Green E
Green J
Green M
Greenberg D
Greene E
Griffiths H
Griffiths M
Grimes Y
Grimwood-fidler D
Gross C
Grosseto D
Gruensfelder S
Gruhne C
Grundtvig M
Gryl A
Grändås M
Grödal K
Gu X
Gu Y
Guan X
Gudeman D
Gudmundsdottir S
Guerocak O
Guerra Deborah
Guest C
Gunvarsdotter S
Guo C
Guo Lei
Guo M
Guo R
Guo S
Guo W
Guo X
Guo Y
Gupta A
Gupta M
Gutierrez J
Günesli A
Haaraoja A
Haastrup B
Hack T
Haddad T
Hadjikov A
Hage-korban E
Haggenmiller S
Hagmanns M
Halberstadt S
Halestrap M
Hall C
Hall E
Hall J
Hall L
Hallett S
Halter B
Hamburg C
Hames E
Hametz C
Hammer F
Hamroff G
Han D
Han Q
Han Y
Hannibal K
Hanrahan J
Hansen ANNETTE SKOVSTED
Hansen TOBIAS HOLM
Hansen TOBIAS HOLM
Hanzich C
Harder M
Harding P
Hardingham S
Harman D
Harnden S
Harrington A
Harris Sigrid
Harting T
Hartland A
Hartley J
Hartner C
Harwood A
Haskel E
Hass T
Hatch J
Hausleiter K
Hautmann M
Haynes R
Hays R
Haywood S
Hazim S
He G
He M
He Weiran
He Y
Healey M
Heaney L
Hedegaard B
Hedgaard L
Hedin U
Hedlöf L
Heid J
Heiman M
Heineman J
Heins G
Heinsvig S
Held M
Heldmann M
Hellsten S
Helms S
Henderson D
Henderson J
Hendrix E
Henkel E
Herd V
Hermans P
Hermany P
Hermes M
Hernandez E
Herrington W
Herriott C
Hessing Kobbelgaard L
Heuer H
Heywood J
Hickmann E
Hierons S
Higginson E
Hill J
Hill M
Hillis S
Hilltout P
Hilts T
Hiltunen P
Hindsgaul L
Hirjikaka S
Hislop A
Hjelmaeus L
Hoag G
Hobbs-williams J
Hobrack S
Hochholzer W
Hockett D
Hoekstra J
Hoffmann L
Hofmann U
Hohenleitner-lührßen K
Holbrook V
Holcomb R
Holde I
Holland Clasby S
Holland M
Hollenweger L
Hollis R
Holm Pedersen L
Holmstrom P
Homberg-pinassi E
Hoopes D
Hopewell Jc
Horacek T
Horner J
Hornslet P
Hosbond S
Hou L
House K
Hovdal H
Hovland A
Hovland R
Hovland S
Howard S
Howe S
Hrusecka R
Hsi D
Hu L
Huang H
Huang L
Huang M
Huang X
Huang Z
Hudson K
Huehnergarth K
Huemmelgen M
Huffman L
Hughes E
Hughes S
Hull A
Humberger C
Humbert J
Hummelshoj J
Humphrey K
Hundei W
Hunt G
Hunter J
Huo L
Hussi E
Hutcheon S
Hutcheson K.
Hutchesson A
Huth M
Hysing J
Hyttinen K
Hårdhammar P
Hårsmar K
Iaquaniello A
Ieva R
Ince H
Inkrot S
Iqbal S
Iselt M
Isermann B
Isserman S
Iversen H
Iverson R
Jabs N
Jackson D
Jackson M
Jackson S
Jagodzinski A
Jain J
James J
James M
Janout M
Jansson Jh
Jasinska E
Jawari A
Jayashekaramurthy J
Jayne K
Jeffers H
Jenkins R
Jensen L
Jepsen J
Jerome S
Jeserich M
Jeter W
Jetty P
Jewkes C
Jia Z
Jiang L Landray M. J.
Jiang J
Jiang X
Jiao H
Jin C
Jin P
Jin Y
Jing J
Johansen L
Johansen T
Johansson A
Johansson M
Johansson Pa
Johansson S
Johnson E
Johnson M
Johnson S
Jonassen R
Jonasson L
Jones A
Jones CLAIRE LOUISE
Jones J
Jones M
Jones P
Jones S
Jones U
Jonsson H
Jonsson L
Jordan J
Joyce J
Judex J
Judge P
Juergens A
Jumper R
Jumper S
Junejo S
Jungbauer C
Junge J
Kadel C
Kahn B
Kahrmann G
Kaiser V
Kalra P
Kandath D
Kandola S
Kanegae K
Kantola I
Karagianni A
Karaks M
Karas S
Karlsberg R
Karlsson Ac
Karlsson G
Karunaratne H
Kask A
Kassa Y
Kasson A
Kastanis D
Kastarinen H
Kaster S
Kato E
Katopodis J
Kaur J
Kayner K
Kazanjian P
Keegan R
Keenan S
Keiran S
Kelley A
Kelley E
Kemala E
Kempe A
Kenegos G
Kent J
Keppel E
Kereiakes D
Kesäniemi A
Ketis C
Key A
Khachab S
Khalifa M
Khan T
Khan W
Kim C
Kimball L
Kimmel S
Kinateder A
Kinder M
King J
Kirby K
Kissam C
Kitamura S
Kiuru P
Kiviniemi T
Kizhakekuttu T
Kjaergaard Danö M
Kjekshus J
Kjellberg-eriksson J
Kjærnli T
Klaus Clark M
Klausen I
Klements D
Klemsdal T
Kleve R
Kline J
Klinger C
Klinkhammer LUTZ HUBER
Klintberg L
Klundt R
Kmetzo J
Knap P
Knoppe A
Knott C
Knutson T
Knutsson A
Koen J
Koopmann K
Koren M
Korn A
Korn D
Koskinen N
Kostedt G
Kotila M
Kouz S
Kovach J
Kozlowski C
Kozlowski L
Krantzler J
Kraus Barbara
Kremerskothen R
Krenk S
Kress K
Kreuzpointner R
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Zhao JIAYI STELLA
Zhao L
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Zhou Juan
Zhou Xingyu
Zhou Yingyuan
Zhu Wangqin
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Zuchelkowski A
Zulauf N
Ågårdh A
Öner A
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2017
Field of study

BACKGROUND: Patients with atherosclerotic vascular disease remain at high risk for cardiovascular events despite effective statin-based treatment of low-density lipoprotein (LDL) cholesterol levels. The inhibition of cholesteryl ester transfer protein (CETP) by anacetrapib reduces LDL cholesterol levels and increases high-density lipoprotein (HDL) cholesterol levels. However, trials of other CETP inhibitors have shown neutral or adverse effects on cardiovascular outcomes. METHODS: We conducted a randomized, double-blind, placebo-controlled trial involving 30,449 adults with atherosclerotic vascular disease who were receiving intensive atorvastatin therapy and who had a mean LDL cholesterol level of 61 mg per deciliter (1.58 mmol per liter), a mean non-HDL cholesterol level of 92 mg per deciliter (2.38 mmol per liter), and a mean HDL cholesterol level of 40 mg per deciliter (1.03 mmol per liter). The patients were assigned to receive either 100 mg of anacetrapib once daily (15,225 patients) or matching placebo (15,224 patients). The primary outcome was the first major coronary event, a composite of coronary death, myocardial infarction, or coronary revascularization. RESULTS: During the median follow-up period of 4.1 years, the primary outcome occurred in significantly fewer patients in the anacetrapib group than in the placebo group (1640 of 15,225 patients [10.8%] vs. 1803 of 15,224 patients [11.8%]; rate ratio, 0.91; 95% confidence interval, 0.85 to 0.97; P=0.004). The relative difference in risk was similar across multiple prespecified subgroups. At the trial midpoint, the mean level of HDL cholesterol was higher by 43 mg per deciliter (1.12 mmol per liter) in the anacetrapib group than in the placebo group (a relative difference of 104%), and the mean level of non-HDL cholesterol was lower by 17 mg per deciliter (0.44 mmol per liter), a relative difference of -18%. There were no significant between-group differences in the risk of death, cancer, or other serious adverse events. CONCLUSIONS: Among patients with atherosclerotic vascular disease who were receiving intensive statin therapy, the use of anacetrapib resulted in a lower incidence of major coronary events than the use of placebo. (Funded by Merck and others; Current Controlled Trials number, ISRCTN48678192 ; ClinicalTrials.gov number, NCT01252953 ; and EudraCT number, 2010-023467-18 .)

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