Chemical structure of lovastatin
Find information on thousands of medical conditions and prescription drugs.

Advicor

Lovastatin, mevastatin is a member of the drug class of statins, used for lowering cholesterol and preventing cardiovascular disease (hypolipidemic agents). The mode of action of statins is HMG-CoA reductase enzyme inhibition. more...

Home
Diseases
Medicines
A
8-Hour Bayer
Abacavir
Abamectin
Abarelix
Abciximab
Abelcet
Abilify
Abreva
Acamprosate
Acarbose
Accolate
Accoleit
Accupril
Accurbron
Accure
Accuretic
Accutane
Acebutolol
Aceclidine
Acepromazine
Acesulfame
Acetaminophen
Acetazolamide
Acetohexamide
Acetohexamide
Acetylcholine chloride
Acetylcysteine
Acetyldigitoxin
Aciclovir
Acihexal
Acilac
Aciphex
Acitretin
Actifed
Actigall
Actiq
Actisite
Actonel
Actos
Acular
Acyclovir
Adalat
Adapalene
Adderall
Adefovir
Adrafinil
Adriamycin
Adriamycin
Advicor
Advil
Aerobid
Aerolate
Afrinol
Aggrenox
Agomelatine
Agrylin
Airomir
Alanine
Alavert
Albendazole
Alcaine
Alclometasone
Aldomet
Aldosterone
Alesse
Aleve
Alfenta
Alfentanil
Alfuzosin
Alimta
Alkeran
Alkeran
Allegra
Allopurinol
Alora
Alosetron
Alpidem
Alprazolam
Altace
Alteplase
Alvircept sudotox
Amantadine
Amaryl
Ambien
Ambisome
Amfetamine
Amicar
Amifostine
Amikacin
Amiloride
Amineptine
Aminocaproic acid
Aminoglutethimide
Aminophenazone
Aminophylline
Amiodarone
Amisulpride
Amitraz
Amitriptyline
Amlodipine
Amobarbital
Amohexal
Amoxapine
Amoxicillin
Amoxil
Amphetamine
Amphotec
Amphotericin B
Ampicillin
Anafranil
Anagrelide
Anakinra
Anaprox
Anastrozole
Ancef
Android
Anexsia
Aniracetam
Antabuse
Antitussive
Antivert
Apidra
Apresoline
Aquaphyllin
Aquaphyllin
Aranesp
Aranesp
Arava
Arestin
Arestin
Argatroban
Argatroban
Argatroban
Argatroban
Arginine
Arginine
Aricept
Aricept
Arimidex
Arimidex
Aripiprazole
Aripiprazole
Arixtra
Arixtra
Artane
Artane
Artemether
Artemether
Artemisinin
Artemisinin
Artesunate
Artesunate
Arthrotec
Arthrotec
Asacol
Ascorbic acid
Asmalix
Aspartame
Aspartic acid
Aspirin
Astemizole
Atacand
Atarax
Atehexal
Atenolol
Ativan
Atorvastatin
Atosiban
Atovaquone
Atridox
Atropine
Atrovent
Augmentin
Aureomycin
Avandia
Avapro
Avinza
Avizafone
Avobenzone
Avodart
Axid
Axotal
Azacitidine
Azahexal
Azathioprine
Azelaic acid
Azimilide
Azithromycin
Azlocillin
Azmacort
Aztreonam
B
C
D
E
F
G
H
I
J
K
L
M
N
O
P
Q
R
S
T
U
V
W
X
Y
Z

Lovastatin was isolated from a strain of Aspergillus terreus and it was the first statin approved by the FDA (August 1987).

Lovastatin is also naturally produced by certain higher fungii such as Pleurotus ostreatus (oyster mushroom) and closely related Pleurotus spp. (Bobek et al., 1998)

In 1998, the US FDA placed a ban on the sale of dietary supplements derived from red yeast rice, which naturally contains lovastatin, arguing that products containing prescription agents require drug approval.

Brand names

  • Mevacor®
  • Advicor® (as a combination with niacin)
  • Altocor®
  • Altoprev®

Reference

  • Bobek P, Ozdin L, Galbavy S. Dose- and time-dependent hypocholesterolemic effect of oyster mushroom (Pleurotus ostreatus) in rats. Nutrition 1998;14:282-6. PMID 9583372.


Read more at Wikipedia.org


[List your site here Free!]


Of death, drugs, recalls, and arrogance
From Alternative Medicine Review, 3/1/05 by Al Czap

To pique your interest, first let's start with the arrogance.

"Niacin (nicotinic acid) comes in prescription form and as 'dietary supplements.' Dietary supplement niacin is not regulated by the U.S. Food and Drug Administration (FDA) the same way that prescription niacin is. It may contain widely variable amounts of niacin--from none to much more than the label states. The amount of niacin may even vary from lot to lot of the same brand. Dietary, supplement niacin must not be used as a substitute for prescription niacin. It should not be used for lowering cholesterol because of potential very serious side effects." (My italics)

Quoted from "Cholesterol-Lowering Drugs" webpage of the American Heart Association (AHA). There is a complete lack of any alternatives to the drugs they recommend, including no mention of inositol hexaniacinate, pantethine, policosanol, or red yeast rice powder.

http://www.americanheart.org/presenter.jhtml?identifier=163

Listing all the drug forms for controlling cholesterol levels, this pharmaceutical model promotion by the AHA appears highly suspect in light of product recalls and problems in the pharmaceutical industry. More on AHA arrogance later.

David Graham is the FDA reviewer who warned the arthritis drug Vioxx had been linked to an increased risk of heart attack and stroke. He testified before the U.S. Senate Finance Committee that there were at least five other drugs on the market today that should be seriously scrutinized to determine whether they should remain there. Dr. Graham cited the ache drug Accutane, the weight loss drug Meridia, the anti-cholesterol drug Crestor, the pain reliever Bextra, and the asthma drug Serevent. Accutane and Crestor continue to come under heavy fire from industry watchdogs calling for their recall. Another editorial alone could be written about antidepressants and the court cases involving suicide and murder.

Product recalls over the past few years include the diabetes drug Rezulin and the painkiller Duract--both for causing liver failure--and the cholesterol-lowering statin Baycol, hitting a home run with fatal rhabdomyolysis, a condition that results in muscle cell breakdown and release of the contents of muscle cells into the bloodstream. Symptoms of rhabdomyolysis include muscle pain, weakness, tenderness, malaise, fever, dark urine, nausea, and vomiting. At the time of recall, the FDA had received reports of 31 deaths in the United States due to severe rhabdomyolysis associated with the use of Baycol, 12 of which involved concomitant use of gemfibrozil. Gemfibrozil currently remains listed on the AHA webpage quoted above, as one of the AHA's magic bullets.

In a February 2004 love-fest press release, KOS Pharmaceuticals, the manufacturer of Niaspan and Advicor (prescription niacin products), strongly commended the AHA for its stand that dietary supplement niacin should not be used. The press release included KOS product information that includes the following warning--Niaspan preparations should not be substituted for equivalent doses of immediate-release (crystalline) niacin because "Cases of severe toxicity, including fulminant hepatic necrosis, have occurred in patients who have substituted sustained-release (modified release, timed-release) niacin products for immediate-release niacin at equivalent doses."

So let's get this straight: substituting the AHA-endorsed pharmaceutical, timed-release niacin, for the same dose of the demonic "dietary supplement" niacin, can cause liver toxicity, while the "dietary supplement" niacin does not. Darn those pesky livers; we should cut them all out and make the AHA happy. A review of the literature readily reveals how some sustained-release forms of niacin have caused significant liver toxicity and in some cases liver failure. (1-5)

So let's come back to the AHA arrogance again:

The following quotation is from an FDA warning letter to the aforementioned KOS Pharmaceuticals, the manufacturer of the AHA-endorsed, pharmaceutical timed-release niacin:

"The inspection revealed your firm's Quality and Laboratory systems employed during the manufacture, processing, packing, or holding of Niaspan (niacin extended-release tablets) and Advicor (niacin extended-release tablet cores/lovastatin tablets) do not conform to cGMP.

"For example, your firm's QCU failed to thoroughly investigate dissolution failures in multiple lots of your Niaspan Extended Release tablets and content uniformity failures found in multiple lots of Advicor tablets." http://www.fda.gov/foi/warningletters/g4502d.htm

Get out your scissors (watch out for that liver) and cut out the quote from the AHA webpage above. You can then paste the pertinent parts adjacent to the actual facts in the rest of this editorial. You will find nothing left, much like the arrogant argument of the AHA, a vacuous condemnation of everything they have not blessed.

Al Czap Publisher

(1.) McKenney JM, Proctor JD. Harris S, Chinchili VM. A comparison of the efficacy and toxic effects of sustained versus immediate-release niacin in hypercholesterolemic patients. JAMA 1994:271:672-677.

(2.) Knopp RH, Ginsberg J, Albers JJ, et al. Contrasting effects of unmodified and time-release forms of niacin on lipoproteins in hyperlipidemic subjects: clues to mechanism of action of niacin. Metabolism 1985:34:642-650.

(3.) Gray DR, Morgan T. Chretien SD, Kashyap ML. Efficacy and safety of controlled-release niacin in dyslipoproteinemic veterans. Am; Intern Med 1994; 121:252-258.

(4.) Rader JI. Calvert RJ, Hathcock JN. Hepatic toxicity of unmodified and time-release preparations of niacin. Am J Med 1992:92:77-81.

(5.) Knopp RH. Niacin and hepatic failure. Ann Intern Med 1989:111:769.

COPYRIGHT 2005 Thorne Research Inc.
COPYRIGHT 2005 Gale Group

Return to Advicor
Home Contact Resources Exchange Links ebay