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The Interface of Medical and Psychiatric Disorders: Focus on Cancer and Heart Disease Presented by: Charles B. Nemeroff, M.D., Ph.D. Matthew P. Nemeroff Professor and Chair Department of Psychiatry and Behavioral Sciences Mulva Clinic for the Neurosciences Director, Institute of Early Life Adversity Research Dell Medical School | The University of Texas at Austin CHARLES B. NEMEROFF, M.D., PH.D. DISCLOSURES Research/Grants: National Institutes of Health (NIH) Consulting (last 12 months): ANeuroTech (division of Anima BV), Taisho Pharmaceutical, Inc., Takeda, Signant Health, Sunovion Pharmaceuticals, Inc., Janssen Research & Development LLC, Magstim, Inc., Navitor Pharmaceuticals, Inc., Intra-Cellular Therapies, Inc., EMA Wellness, Acadia Pharmaceuticals, Corcept Therapeutics, Axsome, Sage, BioXcel Therapeutics, Silo Pharma, XW Pharma, Neuritek, Engrail Therapeutics Stockholder: Xhale, Seattle Genetics, Antares, BI Gen Holdings, Inc., Corcept Therapeutics Pharmaceuticals Company, EMA Wellness Scientific Advisory Boards: ANeuroTech (division of Anima BV), Brain and Behavior Research Foundation (BBRF), Anxiety and Depression Association of America (ADAA), Skyland Trail, Signant Health, Laureate Institute for Brain Research (LIBR), Inc., Magnolia CNS Board of Directors: Gratitude America, ADAA, Xhale Smart, Inc. Patents: Method and devices for transdermal delivery of lithium (US 6,375,990B1), Method of assessing antidepressant drug therapy via transport inhibition of monoamine neurotransmitters by ex vivo assay (US 7,148,027B2) Speakers Bureau: None
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The Interface of Medical and Psychiatric Disorders: Focus ...

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Page 1: The Interface of Medical and Psychiatric Disorders: Focus ...

The Interface of Medical and Psychiatric Disorders: Focus on Cancer and Heart Disease

Presented by:

Charles B. Nemeroff, M.D., Ph.D.

Matthew P. Nemeroff Professor and ChairDepartment of Psychiatry and Behavioral Sciences

Mulva Clinic for the Neurosciences

Director, Institute of Early Life Adversity ResearchDell Medical School | The University of Texas at Austin

CHARLES B. NEMEROFF, M.D., PH.D.DISCLOSURES

Research/Grants: National Institutes of Health (NIH)

Consulting (last 12 months): ANeuroTech (division of Anima BV), Taisho Pharmaceutical, Inc., Takeda, Signant Health, Sunovion

Pharmaceuticals, Inc., Janssen Research & Development LLC, Magstim, Inc., Navitor Pharmaceuticals, Inc., Intra-Cellular Therapies, Inc., EMA

Wellness, Acadia Pharmaceuticals, Corcept Therapeutics, Axsome, Sage, BioXcel Therapeutics, Silo Pharma, XW Pharma, Neuritek, Engrail

Therapeutics

Stockholder: Xhale, Seattle Genetics, Antares, BI Gen Holdings, Inc., Corcept Therapeutics Pharmaceuticals Company, EMA Wellness

Scientific Advisory Boards: ANeuroTech (division of Anima BV), Brain and Behavior Research Foundation (BBRF), Anxiety and Depression

Association of America (ADAA), Skyland Trail, Signant Health, Laureate Institute for Brain Research (LIBR), Inc., Magnolia CNS

Board of Directors: Gratitude America, ADAA, Xhale Smart, Inc.

Patents: Method and devices for transdermal delivery of lithium (US 6,375,990B1), Method of assessing antidepressant drug therapy via

transport inhibition of monoamine neurotransmitters by ex vivo assay (US 7,148,027B2)

Speakers Bureau: None

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Is Depression a Risk Factor for Cancer?

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ABSTRACT: Ovarian cancer is the deadliest gynecologic cancer. Chronic stress accelerates tumor

growth in animal models of ovarian cancer. We therefore postulated that posttraumatic stress disorder

(PTSD) may be associated with increased risk of ovarian cancer. We used data from the Nurses' Health

Study II, a longitudinal cohort study with 26 years of follow-up, conducted from 1989 to 2015 with

54,710 subjects. During follow-up, 110 ovarian cancers were identified. Women with high PTSD

symptoms had 2-fold greater risk of ovarian cancer versus women with no trauma exposure [age-adjusted

HR ¼ 2.10; 95% confidence interval (CI), 1.12–3.95]. Adjustment for health and ovarian cancer risk

factors moderately attenuated this association (HR ¼ 1.86; 95% CI, 0.98–3.51). Associations were similar

or moderately stronger in fully prospective analyses (age-adjusted HR ¼ 2.38; 95% CI, 0.98–5.76, N

cases ¼ 50) and in premenopausal women (HR ¼ 3.42; 95% CI, 1.08–10.85). In conclusion, we show

that PTSD symptoms are associated with increased risk of ovarian cancer.

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BACKGROUND: Few previous studies investigating depression before the diagnosis of breast cancer and breast cancer–

specific mortality have examined depression measured at more than 1 time point. This study investigated the effect of

depression (combining depressive symptoms alone with antidepressant use) measured at 2 time points before the diagnosis of

breast cancer on all-cause mortality and breast cancer–specific mortality among older postmenopausal women. METHODS: A

large prospective cohort, the Women’s Health Initiative, was used. The study included 3095 women with incident breast cancer

who had measures of depressive symptoms and antidepressant use before their diagnosis at the baseline and at year 3.

Multivariate Cox proportional hazards regression was used to estimate adjusted hazard ratios (HRs) between depression at the

baseline, depression at year 3, and combinations of depression at these time points and all-cause mortality and breast cancer–

specific mortality. RESULTS: Depression at year 3 before a breast cancer diagnosis was associated with higher all-cause

mortality after adjustments for multiple covariates (HR, 1.35; 95% confidence interval [CI], 1.02-1.78. In women with late-

stage (regional- or distant-stage) breast cancer, newly developed depression at year 3 was significantly associated with both

all-cause mortality (HR, 2.00; 95%CI, 1.13-3.56) and breast cancer–specific mortality (HR, 2.42; 95% CI, 1.24-4.70).

CONCLUSIONS: Women with newly developed depression before the diagnosis of breast cancer had a modestly but

significantly increased risk for death from any cause and for death from breast cancer at a late stage.

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Our purpose is to identify cancer patients at highest risk of suicide compared to the general

population and other cancer patients. This is a retrospective, population-based study using

nationally representative data from the Surveillance, Epidemiology, and End Results program,

1973-2014. Among 8,651,569 cancer patients, 13,311 committed suicide; the rate of suicide was

28.58/ 100,000-person years, and the standardized mortality ratio (SMR) of suicide was 4.44

(95% CI, 4.33, 4.55). The predominant patients who committed suicide were male (83%) and

white (92%). Cancers of the lung, head and neck, testes, bladder, and Hodgkin lymphoma had

the highest SMRs ( > 5-10) through the follow up period. Elderly, white, unmarried males with

localized disease are at highest risk vs other cancer patients. Among those diagnosed at < 50

years of age, the plurality of suicides is from hematologic and testicular tumors; if > 50, from

prostate, lung, and colorectal cancer patients.

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Musselman et al

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PLoS ONE 7(8): e42324, 2012

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* P < .05, 60 mg vs placebo. HRSD = Hamilton Rating Scale for Depression.van Heeringen K, Zivkov M. Br J Psychiatry. 1996;169:440-443.

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Let no one persuade you to

cure the headache until he

has given you his soul to be

cured. For this is the great

error of our day in the

treatment of the human body,

that physicians separate the

soul from the body.

--Hippocrates 2000BC

NOTHING VIVIFIES AND NOTHING KILLS LIKE THE EMOTIONS.--Joseph Roux 1886

“Grief is Mortal…that is to say deadly”

— Shakespeare (1599)

Every affectation of the mind that is attended with either pain or pleasure, hope or fear, is the cause of an agitation whose influence extends to the heart.--William Harvey 1628

Depression And Cardiovascular Disease

• ↑ rate of depression in ischemic heart disease (IHD)

• Depression is a risk factor for morbidity/mortality post-Ml

• Depression is a risk factor for development of coronary artery disease

• Depression associated with increased platelet activation, platelet reactivity, cardiac events

• SSRIs effective antidepressants in lHD without adverse effects of TCAs

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Previously Identified Risk Factors for

Coronary Artery Disease

Genetic Factors

Diabetes

Hypertension

Thrombocyte Dysfunction

Hyperlipidemia

Smoking

Obesity

Photograph: Davies MJ.Circulation 94:2013-2020, 1996

Relationship Between Depression and

Ischemic Heart Disease (IHD)• 2,832 participants in the National Health Examination Follow-up study

- Ages 45-77 with no IHD

• Baseline assessment with General Well-Being Schedule

- Depressed affect 11.5%

- Moderate hopelessness 10.8%

- Severe hopelessness 2.9%

• Follow-up

- Mean 12.4 years

- 189 cases of fatal IHD

• Depressed affect and hopelessness were associated with fatal and non-fatal IHD

Anda et al., Epidemiology 4:285, 1993

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Fatal and Nonfatal Ischemic Heart Disease (IHD)

over 12.4 Years’ Follow-up

Anda et al. Epidemiology. 1993;4:285-294.

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Mortality and Depression Post-MI

N = 222 post-MI

7 days post MI

Interview and DIS performed to determine if DSM-III-R criteria met

6 months f/u

Determination of survivalFrasure-Smith et al., JAMA 270:1819-1825, 1993

Cumulative Mortality for Depressed and Nondepressed Patients Following Heart Attack

Frasure-Smith et al., JAMA 270:1819-1825, 1993

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6-Month and 18-Month

Coronary Fatalities After Acute MI

Frasure-Smith et al., JAMA 270(15):1819−1825, 1993

Frasure-Smith et al., Circulation 91:999−1005, 1995

Long-term survival after MI in relation to Beck Depression Inventory Score during hospitalization

Lespérance et al., Circulation 105: 1049-1053, 2002

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Depression and Anxiety as Predictors of 2-Year Cardiac

Events in Patients With Stable Coronary Artery Disease

Frasure-Smith and Lesperance (2008) Arch Gen Psychiatry 65:62-71.

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• Results: Baseline depressive symptoms were not related to subsequent events; however, an increase in depression was prognostic. Cox proportional hazards regression analyses with the CES-D scale as a time-dependent variable, controlling for multiple covariates, indicated a 25% increased risk of death per 5-unit increase in the CES-D score (relative risk (RR), 1.25; 95% confidence interval (CI), 1.15 to 1.36).

The RR for stroke or myocardial infarction was 1.18 (95% CI, 1.08 to 1.30). Increase in CES-D score was an independent predictor in both placebo and active drug groups, and it was strongest as a risk factor for stroke among women (RR, 1.29; 95% CI, 1.07 to 1.34).

• Conclusions: Among elderly persons, a significant and substantial excess risk of death and stroke or myocardial infarction was associated with an increase in depressive symptoms over time, which may be a marker for subsequent major disease events and warrants the attention of physicians to such mood changes. However, further

studies of causal pathways are needed before widespread screening for depression in clinical practice is to be recommended.

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Exaggerated Platelet Reactivity in Major DepressionBefore and After Orthostatic Challenge

Musselman et al., Am J Psychiatry 153: 1313-1317, 1996

Platelet Activation

Ischemic heart disease and depression

IHD = ischemic heart disease; D = depression.

Biol Psychiatry 42: 290-295, 1997

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Antidepressant may block heart attacks

Zoloft alleviates sticky situation in blood

USA TODAY – WEDNESDAY, MARCH 17, 1999

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Sertraline Treatment of Major Depression

in Patients With Acute MI or Unstable AnginaSADHART Principal Investigators

Brian Baker, MD; David Barton, MD; Bradley Bart, MD; Peter

Berman, MD; David Brewer, MD; Kevin Browne, MD; John Burks, MD; Robert Campagna, MD; Peter Clemmensen, MD; David Colquhoun,

MD; Clinton Corder, MD; Eric Eichhorn, MD; Mitchell Finkel, MD; Les Forman. MD; Andrew Gaffney, MD; Alexander Glassman, MD; David Goldberg, MD; Veeraindar Goli, MD; Wayne Goodman, MD; Richard

Gray, MD; John Griffin, MD; Torben Haghfelt, MD; Mark Kelemen, MD; Helmut Klein, MD; Michael Koren, MD; Charles Landau, MD; Lidia

Lidagoster,MD; Frank McGrew, MD; Andre Natale, MD; Frank Navetta, MD; Charles Nemeroff, MD; Gerard O’Donnell, MD; Sebastian Palmeri,

MD; Kevin Rapepport, MD; David Sane, MD; Peter Schwartz, MD; Dennis Sprecher, MD; Joshua Straus, MD; J. Robert Swenson, MD; Karl

Swedberg, MD; Louis Van Zyl, MD; Richard Veith, MD; William Wainwright, MD; Richard Weisler, MD; Tom Wise, MD

Risk of Serious Cardiovascular Events

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Cognitive behavior therapy and supportive stress management are efficacious for treating depression after

coronary artery bypass surgery, relative to usual care.

CBT had greater and more

durable effects than SSM on

depression and several

secondary psychological

outcomes.

Cognitive Behavior Therapy (CBT), Supportive Stress Management (SSM), Usual Care (UC).

Freedland et al (2009) Arch Gen Psychiatry 66:387-396.

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UGI Bleeding:

Risk of SSRIs Compared With Others

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