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[Review of] Luvenia A. George. Teaching the Music of Six Different Cultures

Author: Giugliano Constance C.
Publication venue: VCU Scholars Compass
Publication date: 01/01/1988
Field of study

With the recent appearance of more authentic ethnic music in music curriculum series, as well as the spreading influence of the Orff approach to music education based on indigenous and primitive musics and even the proliferation of commercial music influenced by non-Western styles, the appetite of music teachers has been well-whetted for additional source material on ethnic music. In this revised edition of Luvenia George\u27s 1976 book, we have an extraordinary resource that now makes it inexcusable not to have an enriched music program in our schools

VCU Scholars Compass

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
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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
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Brandon P
Braun-dullaeus R
Braunwald E
Bray C
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Breakwell L
Brennan G
Brenner S
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Brettschneider B
Breunig M
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Brigden G
Briggs S
Brilloff S
Brink-kjaer T
Broadway K
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Brown D
Brown E
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Buckley C
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Buesing M
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Bunn D
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Butler R
Butman S
Byng-hollander E
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Börjesson M
Cai J
Cakir M
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Call T
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CARIDAD HERNANDEZ JOSE MANUEL
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Casey MAEVE ANN
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Cha L
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Chai X
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Chen G
Chen L
Chen Minghe
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Chen Y
Chen Z
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Cherian G
Cherrico M
Chi L
Chidambara H
Childs A
Chiodi Riccardo
Chirio C
Chmilewski S
Christensen A
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Christensen S
Chu Y
Chun-furlong D
Chung K
Chung R
Ciampanelli E
Ciuica S
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Claxton E. Jr
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Collis W
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Crivellari ADAM MARIA ROMANO
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Cusner H
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D'Antuono C
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Dagher E
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Darlington H
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Davis M
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Dawkins Hughes S
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De Boer I
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De Donno O
De La Garza J
De Lorenzi E
De Matteis C
De Servi S
De Silva R
Dechert M
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Defraia C
Del Mastro E
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Delgado T
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Demets D
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Deslongchamp F
Desousa C
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Di Pasquale G
Di Ruocco M
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Dickinson RONALD CELESTE
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Diget H
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Ding S
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Dixon L
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Domercant J
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Dong Yingtian
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Donà P
Doty B
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Du N
Du W
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Dubal S
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Edwards M
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Egstrup K
Eiben P
Eichinger G
Einhorn D
Eisen A
Eisenberg D
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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
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Eubanks C
Euler K
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Falco M
Fam M
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Finney
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Ford-tarlton M
Forsberg K
Forster S
Fortney T
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Fox B
Fox C
Fox H
Fox L
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Frank S
Fraser E
Frattini Sabrina
Frederick K
Freeman R
French H
Fresco C
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Fritsch S
Fritschka M
Froberg L
Frost L
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Fullerton D
Fulton J
Gabbert E
Gaede L
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Galindo M
Galla A
Gallegos D
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Gammon R
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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
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Gerber G
German M
Gervasio B
Gesla J
Gessler A
Ghitis A
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Giagnoni E
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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
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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
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Griffiths M
Grimes Y
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Grosseto D
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Grödal K
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Gu Y
Guan X
Gudeman D
Gudmundsdottir S
Guerocak O
Guerra Deborah
Guest C
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He M
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Heldmann M
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Higginson E
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Hilltout P
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Hiltunen P
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Hislop A
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Hockett D
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Hofmann U
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Holbrook V
Holcomb R
Holde I
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Holland M
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Holmstrom P
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Hoopes D
Hopewell Jc
Horacek T
Horner J
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Hou L
House K
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Hovland A
Hovland R
Hovland S
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Howe S
Hrusecka R
Hsi D
Hu L
Huang H
Huang L
Huang M
Huang X
Huang Z
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Huehnergarth K
Huemmelgen M
Huffman L
Hughes E
Hughes S
Hull A
Humberger C
Humbert J
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Hutchesson A
Huth M
Hysing J
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Hårdhammar P
Hårsmar K
Iaquaniello A
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Ince H
Inkrot S
Iqbal S
Iselt M
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Isserman S
Iversen H
Iverson R
Jabs N
Jackson D
Jackson M
Jackson S
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Jain J
James J
James M
Janout M
Jansson Jh
Jasinska E
Jawari A
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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
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Johansen T
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Johansson M
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Johansson S
Johnson E
Johnson M
Johnson S
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Jones CLAIRE LOUISE
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Jones M
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Jones U
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Jonsson L
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Karlsson G
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Kasson A
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Kastarinen H
Kaster S
Kato E
Katopodis J
Kaur J
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Keegan R
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Keiran S
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Kelley E
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Kempe A
Kenegos G
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Khan T
Khan W
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Klundt R
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Koen J
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Kotila M
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Krantzler J
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Lam N
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Langeng T
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Larsby K
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Lecci A
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Lv F
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Lytken Larsen M
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Ma L
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Maas M
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Madden H
Madgwick Z
Madsen L
Mafham M
Maggioni Ap
Magloire V
Mahabir N
Mahal S
Mahan A
Mahlmann A
Mahnkopf C
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Major L
Malak T
Mallari E
Malone M
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Manga S
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Marquez D
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Mcclean G
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Miccoli M
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Zhang Wen
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Zhao JIAYI STELLA
Zhao L
Zhao P
Zhao R
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Zheng Y
Zheng Z
Zhi Y
Zhong H
Zhong R
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Zhou Juan
Zhou Xingyu
Zhou Yingyuan
Zhu Wangqin
Zhu X
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Ziefle S
Zilz N
Zineldine A
Zlatewa R
Zoghbi J
Zong C
Zong D
Zong X
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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Addition of clopidogrel to aspirin and fibrinolytic therapy for myocardial infarction with ST-segment elevation

Author: Abud M
Adgey J
Ahlmark H
Ahmed F
Alcocer MA
Alhabaj S
Allaf E
Allall O
Alony I
Alvarado R
Alvarez LV
Amar R
Ambrosio G
Amerena J
Anderson J
Andersson C
Andresen D
Andresen D
Anhalt D
Anhalt D
Appeltants H
Ardissino D
Areses ELD
Arntz H
Aroesty J
Aroesty J
Aso FO
Atar S
Aude Y
Aude Y
Audicana J
Austin M
Avalos V
Averland B
Ayan J
Aylward P
Badenhorst J
Baldini E
Bandh S
Banham N
Barillas O
Barros S
Bartal G
Bass J
Bata I
Batalla A
Bayram E
Bearez E
Becker C
Belras AC
Bennett J
Berger C
Berli MA
Bertrand M
Beruben A
Bethencourt A
Bhargava R
Bishop A
Blomerus P
Blumberg S
Blumenthal M
Blumenthal M
Blumenthal M
Bobak C
Bobak C
Bode C
Boldueva S
Bonneau A
Bosschaart M
Bovak B
Boyarkin M
Braunwald E
Braunwald E
Braunwald E
Braunwald E
Brennan B
Britz A
Brogan G
Budaj A
Burgess L
Buros J
Bustamante F
Bustillos MDB
Caime DG
Cannon C
Cannon C
Cannon C
Cannon CP
Capozi A
Carignan D
Carlaire D
Carrageta M
Carrillo J
Casasnovas J
Casazza F
Caspi A
Castro PT
Caussanel J
Cedergren E
Chadow H
Chandna H
Chandna H
Chandra M
Chandra M
Charlesworth A
Chaves A
Chernov S
Chester L
Chew D
Chiarella F
Chohan A
Ciaglo L
Cicogna A
Claeys M
Claeys MJ
Classon H
Coelho OR
Collberg K
Congreave S
Constance C
Conway B
Cools F
Cools F
Coops G
Coppes A
Coppolino A
Cortes JG
Covelli G
Cragg D
Cruse A
Cunningham N
Cyster H
D'Hooghe G
da Cunha CP
Daly K
Daniels M
Darius H
Darveau C
Datiashvily L
David D
David J
David M
Day L
de Arenaza D
de Belder M
de Blas RC
de Brito MR
De Ferrari G
de Lima AA
De Luca I
De Meester A
deBeer M
Decroly P
Degertekin M
Del Pinto M
Del Pinto M
Delaet I
Delaet I
Delaet I
Delgado L
Dellborg M
Dellborg M
Dieker H
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Dutra O
Ebrahim I
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Fernandez JD
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Fijlstra I
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Wiviott S
Wucherpfennig P
Yedid-Am S
Yoches A
Young J
Yuval R
Zadiontchenko V
Zalevsky G
Zeymer U
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2005
Field of study

BACKGROUND: A substantial proportion of patients receiving fibrinolytic therapy for myocardial infarction with ST-segment elevation have inadequate reperfusion or reocclusion of the infarct-related artery, leading to an increased risk of complications and death. METHODS: We enrolled 3491 patients, 18 to 75 years of age, who presented within 12 hours after the onset of an ST-elevation myocardial infarction and randomly assigned them to receive clopidogrel (300-mg loading dose, followed by 75 mg once daily) or placebo. Patients received a fibrinolytic agent, aspirin, and when appropriate, heparin (dispensed according to body weight) and were scheduled to undergo angiography 48 to 192 hours after the start of study medication. The primary efficacy end point was a composite of an occluded infarct-related artery (defined by a Thrombolysis in Myocardial Infarction flow grade of 0 or 1) on angiography or death or recurrent myocardial infarction before angiography. RESULTS: The rates of the primary efficacy end point were 21.7 percent in the placebo group and 15.0 percent in the clopidogrel group, representing an absolute reduction of 6.7 percentage points in the rate and a 36 percent reduction in the odds of the end point with clopidogrel therapy (95 percent confidence interval, 24 to 47 percent; P<0.001). By 30 days, clopidogrel therapy reduced the odds of the composite end point of death from cardiovascular causes, recurrent myocardial infarction, or recurrent ischemia leading to the need for urgent revascularization by 20 percent (from 14.1 to 11.6 percent, P=0.03). The rates of major bleeding and intracranial hemorrhage were similar in the two groups. CONCLUSIONS: In patients 75 years of age or younger who have myocardial infarction with ST-segment elevation and who receive aspirin and a standard fibrinolytic regimen, the addition of clopidogrel improves the patency rate of the infarct-related artery and reduces ischemic complications

Lirias

Archivio istituzionale della Ricerca - Università degli Studi di Parma

Evolocumab and clinical outcomes in patients with cardiovascular disease

Author: Abelson M.
Aboufakher R.
Abrahamsen T. E.
Accini Mendoza J. L.
Acheatel R.
Ackermann D.
Adamkova V.
Adams M.
Adlam D.
Aggarwal R.
Aggarwal S.
Ahsan A.
Ainsworth P.
Airody Govinda R.
Akai A.
Ako J.
Al-Bahrani A.
Al-Joundi T.
Aldegather J.
Aldrete Velasco J. A.
Alfieri A.
Alt I.
Alzohaili O.
Amerena J.
Amin J.
Amoedo R.
Amuchastegui M.
Anderson T.
Andreka P.
Andreotti F.
Angoulvant D.
Ansell B.
Antalik L.
Antkowiak-Piatyszek K.
Appel K.
Arakawa T.
Arana Londoño C.
Ardissino D.
Ardito W. R.
Arkhipov M.
Arsenescu-Georgescu C.
Asamoah N.
Ascaso Gimilio J. F.
Atar S.
Atassi K.
Athyros V.
Auerbach E.
Awtry E.
Baass A.
Badariene J.
Badat A.
Badila E.
Bae J.
Baigent C.
Bain S.
Baird I.
Baker J.
Balbay Y.
Baldari D.
Ballantyne C.
Bammert A.
Banach M.
Bandh S.
Banerjee S.
Banik M.
Banikova A.
Barbarash O.
Barcinas R.
Barnum O.
Barroso de Souza W. K.
Bart B.
Barton J.
Bata I.
Batalla E.
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Bazzoni Ruiz A. E.
Bednarkiewicz Z.
Beer H. J.
Begg A.
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Bendermacher P.
Benton R.
Berger C.
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Berglund S.
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Bertolet B.
Bertolim Precoma D.
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Östergren J.
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2017
Field of study

peer reviewedBACKGROUND Evolocumab is a monoclonal antibody that inhibits proprotein convertase subtilisin-kexin type 9 (PCSK9) and lowers low-density lipoprotein (LDL) cholesterol levels by approximately 60%. Whether it prevents cardiovascular events is uncertain. METHODS We conducted a randomized, double-blind, placebo-controlled trial involving 27,564 patients with atherosclerotic cardiovascular disease and LDL cholesterol levels of 70 mg per deciliter (1.8 mmol per liter) or higher who were receiving statin therapy. Patients were randomly assigned to receive evolocumab (either 140 mg every 2 weeks or 420 mg monthly) or matching placebo as subcutaneous injections. The primary efficacy end point was the composite of cardiovascular death, myocardial infarction, stroke, hospitalization for unstable angina, or coronary revascularization. The key secondary efficacy end point was the composite of cardiovascular death, myocardial infarction, or stroke. The median duration of follow-up was 2.2 years. RESULTS At 48 weeks, the least-squares mean percentage reduction in LDL cholesterol levels with evolocumab, as compared with placebo, was 59%, from a median baseline value of 92 mg per deciliter (2.4 mmol per liter) to 30 mg per deciliter (0.78 mmol per liter) (P<0.001). Relative to placebo, evolocumab treatment significantly reduced the risk of the primary end point (1344 patients [9.8%] vs. 1563 patients [11.3%]; hazard ratio, 0.85; 95% confidence interval [CI], 0.79 to 0.92; P<0.001) and the key secondary end point (816 [5.9%] vs. 1013 [7.4%]; hazard ratio, 0.80; 95% CI, 0.73 to 0.88; P<0.001). The results were consistent across key subgroups, including the subgroup of patients in the lowest quartile for baseline LDL cholesterol levels (median, 74 mg per deciliter [1.9 mmol per liter]). There was no significant difference between the study groups with regard to adverse events (including new-onset diabetes and neurocognitive events), with the exception of injection-site reactions, which were more common with evolocumab (2.1% vs. 1.6%). CONCLUSIONS In our trial, inhibition of PCSK9 with evolocumab on a background of statin therapy lowered LDL cholesterol levels to a median of 30 mg per deciliter (0.78 mmol per liter) and reduced the risk of cardiovascular events. These findings show that patients with atherosclerotic cardiovascular disease benefit from lowering of LDL cholesterol levels below current targets. © 2017 Massachusetts Medical Society

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Ezetimibe added to statin therapy after acute coronary syndromes

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Aambakk MB
Aase O
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Abdel-Latief A
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Zuidgeest JA
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Zweiker R
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Édes I
Östberg S
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2015
Field of study

BACKGROUND: Statin therapy reduces low-density lipoprotein (LDL) cholesterol levels and the risk of cardiovascular events, but whether the addition of ezetimibe, a nonstatin drug that reduces intestinal cholesterol absorption, can reduce the rate of cardiovascular events further is not known. METHODS: We conducted a double-blind, randomized trial involving 18,144 patients who had been hospitalized for an acute coronary syndrome within the preceding 10 days and had LDL cholesterol levels of 50 to 100 mg per deciliter (1.3 to 2.6 mmol per liter) if they were receiving lipid-lowering therapy or 50 to 125 mg per deciliter (1.3 to 3.2 mmol per liter) if they were not receiving lipid-lowering therapy. The combination of simvastatin (40 mg) and ezetimibe (10 mg) (simvastatin-ezetimibe) was compared with simvastatin (40 mg) and placebo (simvastatin monotherapy). The primary end point was a composite of cardiovascular death, nonfatal myocardial infarction, unstable angina requiring rehospitalization, coronary revascularization ( 6530 days after randomization), or nonfatal stroke. The median follow-up was 6 years. RESULTS: The median time-weighted average LDL cholesterol level during the study was 53.7 mg per deciliter (1.4 mmol per liter) in the simvastatin-ezetimibe group, as compared with 69.5 mg per deciliter (1.8 mmol per liter) in the simvastatin-monotherapy group (P<0.001). The Kaplan-Meier event rate for the primary end point at 7 years was 32.7% in the simvastatin-ezetimibe group, as compared with 34.7% in the simvastatin-monotherapy group (absolute risk difference, 2.0 percentage points; hazard ratio, 0.936; 95% confidence interval, 0.89 to 0.99; P = 0.016). Rates of pre-specified muscle, gallbladder, and hepatic adverse effects and cancer were similar in the two groups. CONCLUSIONS: When added to statin therapy, ezetimibe resulted in incremental lowering of LDL cholesterol levels and improved cardiovascular outcomes. Moreover, lowering LDL cholesterol to levels below previous targets provided additional benefit

Archivio istituzionale della ricerca - Università di Genova

Archivio della ricerca- Università di Roma La Sapienza

Archivio istituzionale della ricerca - Università di Modena e Reggio Emilia

Edoxaban versus warfarin in patients with atrial fibrillation

Author: Abdullakutty J
Abi-Mansour P
Abril SB
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Acikel M
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Adler J
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Ahuad Guerrero R
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Albert L. Waldo
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Östberg S
Ŝpinar J
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2013
Field of study

Contains fulltext : 125374.pdf (publisher's version ) (Open Access)BACKGROUND: Edoxaban is a direct oral factor Xa inhibitor with proven antithrombotic effects. The long-term efficacy and safety of edoxaban as compared with warfarin in patients with atrial fibrillation is not known. METHODS: We conducted a randomized, double-blind, double-dummy trial comparing two once-daily regimens of edoxaban with warfarin in 21,105 patients with moderate-to-high-risk atrial fibrillation (median follow-up, 2.8 years). The primary efficacy end point was stroke or systemic embolism. Each edoxaban regimen was tested for noninferiority to warfarin during the treatment period. The principal safety end point was major bleeding. RESULTS: The annualized rate of the primary end point during treatment was 1.50% with warfarin (median time in the therapeutic range, 68.4%), as compared with 1.18% with high-dose edoxaban (hazard ratio, 0.79; 97.5% confidence interval [CI], 0.63 to 0.99; P<0.001 for noninferiority) and 1.61% with low-dose edoxaban (hazard ratio, 1.07; 97.5% CI, 0.87 to 1.31; P=0.005 for noninferiority). In the intention-to-treat analysis, there was a trend favoring high-dose edoxaban versus warfarin (hazard ratio, 0.87; 97.5% CI, 0.73 to 1.04; P=0.08) and an unfavorable trend with low-dose edoxaban versus warfarin (hazard ratio, 1.13; 97.5% CI, 0.96 to 1.34; P=0.10). The annualized rate of major bleeding was 3.43% with warfarin versus 2.75% with high-dose edoxaban (hazard ratio, 0.80; 95% CI, 0.71 to 0.91; P<0.001) and 1.61% with low-dose edoxaban (hazard ratio, 0.47; 95% CI, 0.41 to 0.55; P<0.001). The corresponding annualized rates of death from cardiovascular causes were 3.17% versus 2.74% (hazard ratio, 0.86; 95% CI, 0.77 to 0.97; P=0.01), and 2.71% (hazard ratio, 0.85; 95% CI, 0.76 to 0.96; P=0.008), and the corresponding rates of the key secondary end point (a composite of stroke, systemic embolism, or death from cardiovascular causes) were 4.43% versus 3.85% (hazard ratio, 0.87; 95% CI, 0.78 to 0.96; P=0.005), and 4.23% (hazard ratio, 0.95; 95% CI, 0.86 to 1.05; P=0.32). CONCLUSIONS: Both once-daily regimens of edoxaban were noninferior to warfarin with respect to the prevention of stroke or systemic embolism and were associated with significantly lower rates of bleeding and death from cardiovascular causes. (Funded by Daiichi Sankyo Pharma Development; ENGAGE AF-TIMI 48 ClinicalTrials.gov number, NCT00781391.)

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Evolocumab and clinical outcomes in patients with cardiovascular disease

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Aboufakher R
Abrahamsen Te
Accini Mendoza Jl
Acheatel R
Ackermann D
Adamkova V
Adams M
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Ahsan A
Ainsworth P
Airody Govinda R
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Al-Bahrani A
Al-Joundi T
Aldegather J
Aldrete Velasco Ja
Alfieri A
Alt I
Alzohaili O
Amerena J
Amin J
Amoedo R
Amuchastegui M
Anderson T
Andreka P
Andreotti F
Angoulvant D
Ansell B
Antalik L
Antkowiak-Piatyszek K
Appel K
Arakawa T
Arana Londoño C
Ardissino D
Ardito Wr
Arkhipov M
Arsenescu-Georgescu C
Asamoah N
Ascaso Gimilio Jf
Atar S
Atassi K
Athyros V
Auerbach E
Awtry E
Baass A
Badariene J
Badat A
Badila E
Bae J
Baigent C
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Baird I
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Balbay Y
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Ballantyne C
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Bandh S
Banerjee S
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Barroso de Souza Wk
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Bertolim Precoma D
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Bhargava R
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Bilianou H
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Östergren J
Publication venue: 'Massachusetts Medical Society'
Publication date: 01/01/2017
Field of study

BACKGROUND Evolocumab is a monoclonal antibody that inhibits proprotein convertase subtilisin-kexin type 9 (PCSK9) and lowers low-density lipoprotein (LDL) cholesterol levels by approximately 60%. Whether it prevents cardiovascular events is uncertain. METHODS We conducted a randomized, double-blind, placebo-controlled trial involving 27,564 patients with atherosclerotic cardiovascular disease and LDL cholesterol levels of 70 mg per deciliter (1.8 mmol per liter) or higher who were receiving statin therapy. Patients were randomly assigned to receive evolocumab (either 140 mg every 2 weeks or 420 mg monthly) or matching placebo as subcutaneous injections. The primary efficacy end point was the composite of cardiovascular death, myocardial infarction, stroke, hospitalization for unstable angina, or coronary revascularization. The key secondary efficacy end point was the composite of cardiovascular death, myocardial infarction, or stroke. The median duration of follow-up was 2.2 years. RESULTS At 48 weeks, the least-squares mean percentage reduction in LDL cholesterol levels with evolocumab, as compared with placebo, was 59%, from a median baseline value of 92 mg per deciliter (2.4 mmol per liter) to 30 mg per deciliter (0.78 mmol per liter) (P<0.001). Relative to placebo, evolocumab treatment significantly reduced the risk of the primary end point (1344 patients [9.8%] vs. 1563 patients [11.3%]; hazard ratio, 0.85; 95% confidence interval [CI], 0.79 to 0.92; P<0.001) and the key secondary end point (816 [5.9%] vs. 1013 [7.4%]; hazard ratio, 0.80; 95% CI, 0.73 to 0.88; P<0.001). The results were consistent across key subgroups, including the subgroup of patients in the lowest quartile for baseline LDL cholesterol levels (median, 74 mg per deciliter [1.9 mmol per liter]). There was no significant difference between the study groups with regard to adverse events (including new-onset diabetes and neurocognitive events), with the exception of injection-site reactions, which were more common with evolocumab (2.1% vs. 1.6%). CONCLUSIONS In our trial, inhibition of PCSK9 with evolocumab on a background of statin therapy lowered LDL cholesterol levels to a median of 30 mg per deciliter (0.78 mmol per liter) and reduced the risk of cardiovascular events. These findings show that patients with atherosclerotic cardiovascular disease benefit from lowering of LDL cholesterol levels below current targets

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