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Effect of rosiglitazone on survival in patients with diabetes mellitus treated for coronary artery disease

Choy-Shan, Alana; Zinn, Andrew; Shah, Binita; Danoff, Ann; Donnino, Robert; Schwartzbard, Arthur Z; Lorin, Jeffrey D; Grossi, Eugene; Sedlis, Steven P
OBJECTIVES: The purpose of this study was to assess the impact of rosiglitazone on survival in patients with diabetes mellitus (DM) and coronary artery disease (CAD). METHODS: We carried out a drug-exposure analysis in 801 patients with DM and CAD in a cardiac catheterization laboratory registry (490 patients treated with a percutaneous coronary intervention, 224 patients treated with coronary artery bypass grafting, and 87 patients treated with medication alone). RESULTS: A total of 193 patients (24.1%) were exposed to rosiglitazone. The median survival from the date of cardiac catheterization in the rosiglitazone group was 146.7 months versus 109.1 months in the unexposed group (P<0.001). At 5 years, the unadjusted survival was 82% in the rosiglitazone-exposed group versus 69% in the unexposed group (P<0.001). There was no difference in survival between rosiglitazone-exposed and rosiglitazone-unexposed patients in the groups treated with coronary artery bypass grafting or medical therapy (P=0.37 and 0.11, respectively). In a multivariable model, rosiglitazone exposure had no effect on mortality (hazard ratio=0.737; 95% confidence interval: 0.521-1.044, P=0.86). CONCLUSION: We conclude that exposure to rosiglitazone is not associated with increased mortality in diabetics who are treated for CAD. These findings support the notion that insulin sensitization with a thiazolidinedione is safe in carefully selected and treated patients with DM and CAD.
PMID: 22750913
ISSN: 0954-6928
CID: 171132

Alternative approach to insulin-like growth factor-1 inhibition for treatment of breast cancer

Ameri, Pietro; Danoff, Ann; Kleinberg, David L
PMID: 22393094
ISSN: 0732-183x
CID: 165608

DIABETES IN OLDER ADULTS: RESULTS FROM NHANES 2003-2008 [Meeting Abstract]

Strauss, S. M.; Danoff, A.; Deren, S.
ISI:000303602000299
ISSN: 0016-9013
CID: 167730

Energy, evolution, and human diseases: an overview

Roth, Jesse; Szulc, Alessandra L; Danoff, Ann
In the symposium entitled 'Transcriptional controls of energy sensing,' the authors presented recent advances on 1) AMP kinase, an intracellular energy sensor; 2) PGC-1alpha (peroxisome proliferator-activated receptor gamma co-activator 1alpha), a transcriptional co-activator that has powerful effects on mitochondria; 3) methylation and demethylation in response to metabolic fluctuations; and 4) FGF21 (fibroblast growth factor 21) as an emerging hormone-like intercellular metabolic coordinator. This introduction places these advances within a broad overview of energy sensing and energy balance, with a focus on human evolution and disease. Four key elements of human biology are analyzed: 1) elevated body temperature; 2) complex prolonged reproductive pathways; 3) emergence of 4 large, well-defined fat depots, each with its own functional role; and 4) an immune system that is often up-regulated by nutrition-related signals, independent of the actual presence of a pathogen. We propose that an overactive immune system, including the 'metabolic syndrome,' was adopted evolutionarily in the distant past to help hold out against unconquerable infections such as tuberculosis, malaria, and trypanosomiasis. This immune activation is advantageous in the absence of other disease management methods, especially under conditions in which life expectancy is short. The inflammation has become a major agent of pathology in wealthy populations in whom the pathogens are a minor threat and life expectancy is long. The 'Conclusions' section sketches cautiously how understanding the molecules involved in energy sensing and energy balance may lead to specific therapies for obesity and diabetes and for their complications
PMID: 21289219
ISSN: 1938-3207
CID: 134220

Effect of autoimmune thyroid disease in older euthyroid infertile woman during the first 35 days of an IVF cycle

Reh, Andrea; Chaudhry, Sonal; Mendelsohn, Felicia; Im, Shelly; Rolnitzky, Linda; Amarosa, Alana; Levitz, Mortimer; Srinivasa, Suman; Krey, Lewis; Berkeley, Alan S; Grifo, James A; Danoff, Ann
In this case-control study of euthyroid first-cycle IVF patients >/= 38 years old with singleton baby, miscarriage, biochemical pregnancy, and no pregnancy outcomes from 2005-2008, we assayed frozen serum for autoimmune thyroid disease (AITD) and thyroid function at cycle start, trigger, and 4 and 5 weeks' gestation. AITD prevalence in older infertile women was similar across clinical outcomes, and although AITD was associated with a higher baseline TSH, TSH remained within acceptable ranges, suggesting that T(4) supplementation may not affect maternal outcomes in older euthyroid AITD patients through 5 weeks gestation
PMCID:3059547
PMID: 21047632
ISSN: 1556-5653
CID: 138179

What is a normal thyroid-stimulating hormone (TSH) level? Effects of stricter TSH thresholds on pregnancy outcomes after in vitro fertilization

Reh, Andrea; Grifo, James; Danoff, Ann
Using a thyroid-stimulating hormone (TSH) cutoff of 2.5 mIU/L or 4.5 mIU/L, no differences in the rates of clinical pregnancy, delivery, or miscarriage were observed in this large, retrospective cohort study of first-cycle IVF patients from 2005 through 2008, after controlling for age. Although lowering the TSH threshold to 2.5 mIU/L would result in a nearly fivefold increase in the number of women being classified as hypothyroid, the lack of differences in maternal clinical outcomes must be considered in the current controversy regarding the relative merits of lowering the upper limit of normal of TSH
PMID: 20655528
ISSN: 1556-5653
CID: 149782

WHAT IS A NORMAL THYROID STIMULATING HORMONE (TSH) LEVEL? EFFECTS OF STRICTER TSH THRESHOLDS ON PREGNANCY OUTCOMES AFTER IVF [Meeting Abstract]

Reh, A.; Danoff, A.; Grifo, J.
ISI:000281441000641
ISSN: 0015-0282
CID: 113772

EFFECT OF AUTOIMMUNE THYROID DISEASE (AITD) IN OLDER, EUTHYROID INFERTILE WOMEN UNDERGOING IN VITRO FERTILIZATION (IVF) [Meeting Abstract]

Reh, A.; Im, S.; Amarosa, A.; Rolnitzky, L.; Grifo, J.; Danoff, A.
ISI:000281441000647
ISSN: 0015-0282
CID: 113773

Can 'personalized diagnostics' promote earlier intervention for dysglycaemia? Hypothesis ready for testing [Editorial]

Dankner, Rachel; Danoff, Ann; Roth, Jesse
The risk associated with progression to diabetes as well as for cardiovascular complications increases along a continuum, rather than being threshold-dependent. How can we identify those with glucose levels in the upper reaches of normal who are most in need of a preventive intervention? With present criteria, we are likely excluding many individuals who have heightened risk. We introduce here the possibility of using a 'personalized' glucose profile to encourage early intervention in subjects in whom glucose metabolism is deteriorating (on an individual level) but not yet abnormal on a population-based norm. We further suggest that 'personalized profiles' of hemoglobin A1c and basal plasma insulin may also help encourage appropriately early intervention. That the first line therapies are so effective, safe and simple make these more sensitive approaches very attractive
PMID: 20101654
ISSN: 1520-7560
CID: 149789

Glycated haemoglobin in diabetic women with and without HIV infection: data from the Women's Interagency HIV Study

Glesby, Marshall J; Hoover, Donald R; Shi, Qiuhu; Danoff, Ann; Howard, Andrea; Tien, Phyllis; Merenstein, Dan; Cohen, Mardge; Golub, Elizabeth; Dehovitz, Jack; Nowicki, Marek; Anastos, Kathryn
BACKGROUND: Limited data suggest that glycated haemoglobin (haemoglobin A1c; A1C) values might not reflect glycaemic control accurately in HIV-infected individuals with diabetes. METHODS: We evaluated repeated measures of paired fasting glucose and A1C values in 315 HIV-infected and 109 HIV-uninfected diabetic participants in the Women's Interagency HIV Study. Generalized estimating equations used log A1C as the outcome variable, with adjustment for log fasting glucose concentration in all models. RESULTS: An HIV-infected woman on average had 0.9868 times as much A1C (that is, 1.32% lower; 95% confidence interval 0.9734-0.9904) as an HIV-uninfected woman with the same log fasting glucose concentration. In multivariate analyses, HIV serostatus was not associated, but White, other non-Black race, and higher red blood cell mean corpuscular volume (MCV) were statistically associated with lower A1C values. Use of diabetic medication was associated with higher A1C values. In multivariate analyses restricted to HIV-infected women, White and other race, higher MCV, and HCV viraemia were associated with lower A1C values, whereas older age, use of diabetic medications and higher CD4(+) T-cell count were associated with higher A1C values. Use of combination antiretroviral therapy, protease inhibitors, zidovudine, stavudine or abacavir was not associated with A1C values. CONCLUSIONS: A1C values were modestly lower in HIV-infected diabetic women relative to HIV-uninfected diabetic women after adjustment for fasting glucose concentration. The difference was abrogated by adjustment for MCV, race and diabetic medication use. Our data suggest that in clinical practice A1C gives a reasonably accurate refection of glycaemic control in HIV-infected diabetic women
PMCID:2943237
PMID: 20587850
ISSN: 2040-2058
CID: 119249