Aromatase inhibitors may protect against prostate cancer but promote nasty (but reversible once the drug is stopped) joint problems.
Hmm. I guess resveratrol should be added to the list of autoimmune risk supplements like aminoguanidine and lipoic acid.
J Rheumatol. 2007 Oct 15
Joint Pain with Aromatase Inhibitors: Abnormal Frequency of Sjögren's Syndrome.
Laroche M, Borg S, Lassoued S, De Lafontan B, Roché H.
From the Service de Rhumatologie, CHU Rangueil; and the Service de Cancérologie, Institut Claudius Regaud, Toulouse, France.
OBJECTIVE: Since the results of the ATAC study, women who have undergone surgery for breast cancer and who require adjuvant hormone therapy are often treated with aromatase inhibitors. With these treatments, joint pain is frequent (30% to 40%) and quite often disabling (5% to 10%). Our objective was to investigate the origin of the pain induced by the anti-aromatases. METHODS: Twenty-four women of mean age 59 years with joint pain of > 5/10 on a visual analog scale underwent a rheumatological consultation and systematic laboratory tests. RESULTS: In 5 patients, pain was considered to have a well defined cause: osteoarthritis, shoulder tendinitis, or paraneoplastic aponeurositis. The other 19 patients had inflammatory pain of the fingers, wrists, shoulders, forefeet, ankles, or knees, with slight synovial thickening of the PIP and MCP joints. Two had an inflammatory syndrome on laboratory tests. Nine of these patients had antinuclear antibodies (ANA > 1/160 on HEp-2 cells) and 4 had rheumatoid factors (> 20 U). Ten patients had sicca syndrome of the eyes or mouth, 7 had probable Sjögren's syndrome according to the San Diego criteria, and one had definite Sjögren's syndrome. One had rheumatoid arthritis, one had Hashimoto thyroiditis, and 2 had positive hepatitis C serology. CONCLUSION: Is the almost total estrogen depletion induced by aromatase inhibitors conducive to the development of sicca syndromes with ANA? Our results should be considered in relation to the Sjögren-like syndromes occurring in aromatase knock-out mice as recently reported.
PMID: 17937464
Gastroenterology. 2003 Dec;125(6):1705-13.
Autoreactivity to lipoate and a conjugated form of lipoate in primary biliary cirrhosis.
Bruggraber SF, Leung PS, Amano K, Quan C, Kurth MJ, Nantz MH, Benson GD, Van de Water J, Luketic V, Roche TE, Ansari AA, Coppel RL, Gershwin ME.
Division of Rheumatology, Allergy and Clinical Immunology, University of California at Davis Medical School, 95616, USA.
BACKGROUND & AIMS: Although considerable effort has been directed toward the mapping of peptide epitopes by autoantibodies, the role of nonprotein molecules has been less well studied. The immunodominant autoantigen in primary biliary cirrhosis (PBC), E2 components of pyruvate dehydrogenase complexes (PDC-E2), has a lipoate molecule bonded to the domain to which autoantibodies are directed. METHODS: We examined sera from patients with PBC (n = 105), primary sclerosing cholangitis (n = 70), and rheumatoid arthritis (n = 28) as well as healthy volunteers (n = 43) for reactivity against lipoic acid. The lipoic acid hapten specificity of the reactive antibodies in PBC sera was determined following incubation of aliquots of the sera with human serum albumin (HSA), lipoylated HSA (HSA-LA), PDC-E2, lipoylated PDC-E2, polyethylene glycol (PEG), lipoylated PEG, free lipoic acid, and synthetic molecular mimics of lipoic acid. RESULTS: Anti-lipoic acid specific antibodies were detected in 81% (79 of 97) of antimitochondrial antibody (AMA)-positive patients with PBC but not in controls. Two previously unreported specificities in AMA-positive sera that recognize free lipoic acid and a carrier-conjugated form of lipoic acid were also identified. CONCLUSIONS: We hypothesize that conjugated form(s) of native or xenobiotic lipoic acid mimics contribute to the initiation and perpetuation of autoimmunity by at first breaking self-tolerance and participating in subsequent determinant spreading. The variability in the immunoreactive carrier/lipoate conjugates provides an experimental framework on which potential mechanisms for the breakdown of self-tolerance following exposure to xenobiotics can be investigated. The data have implications for patients taking lipoic acid as a dietary supplement.
PMID: 14724823
http://www.medscape....ticle/460902_21These are the summary results of the aminoguanidine (pimagedine) studies of diabetic nephropathy. A substantial number of patients with type 1 and type 2 diabetes with clinical nephropathy, proteinuria, and creatinine up to 2 mg/dL were studied at 2 different dose levels and compared with placebo.
The studies were troubled by issues with regards to safety, with flu-like syndrome being present in both type 1 and type 2 diabetes patients, and moderate anemia being an issue for another subset of patients. But most disturbing was a problem with elevated antinuclear antibodies and antineutrophil cytoplasm autoantibodies (ANCA) vasculitis, resulting in glomerulonephritis and stroke in a handful of patients.
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