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Testosterone- Should we be considering it as a risk factor for CVD?
And should we be measuring & addressing it?
Professor Mike Kirby FRCP University of Hertfordshire & The
Prostate Centre London
Disclosures
• Professor Mike Kirby has received funding for research, conference
attendance, lecturing and advice from the pharmaceutical industry
including Astellas, Pfizer, Takeda, Bayer, Besins, MSD, BI, Lilly,
GSK, AZ, Ipsen and Menarini.
• Editor PCCJ
• Also on several NHS advisory boards including the Prostate cancer
Risk Management Programme and the Prostate Cancer advisory
Group
• Member of the National Prostate Cancer Audit Group
Hodges Kirby et al Int J Clin. Pract 2007;61:2019-25
In half the men there were missed opportunities
to assess CVD risk and treat to goal
“Men with ED should be specifically targeted for CVD
preventative strategies in terms of lifestyle changes and
pharmacological treatments” Nitrates!!
The temporal relationship between ED and CVD & why don’t men talk about it ?
• 207 CVD men attending cardiac rehab
• 165 age matched controls
• ED in 66% with CVD – discussed in 53%
• ED in 37% controls – discussed in 43%
• ED on average 5 years before CVD
Testosterone levels are lower at all ages in
Men with ED
0
5
10
15
20
25
30
18-35 35-55 56-70
Age Group
Te
sto
ste
ron
e (
nm
ol/
l)
Patient Control
Janini Int J Androl 1999 22 385-392
1400 men aged 40-49 ED associated with 50 fold risk of CAD
Age Group ED at baseline No baseline ED
40-49 48.52 (1.23-269.26) 0.94 (0.02-5.21)
50-59 27.15 (7.40-69.56) 5.09 (3.38-7.38)
60-69 23.97 (11.49-44.10) 10.72 (7.62-14.66)
70+ 29.63 (19.37-43.75) 23.30 (17.18-30.89)
Inman et al Mayo Clin Pr 2009
CAD events per 1000 pt years with CI interval
What is the difference between QRISK®3 and QRISK®2?
• QRISK®3 includes more factors than QRISK®2 to help enable doctors
to identify those at most risk of heart disease and stroke. • These are
• Chronic kidney disease, which now includes stage 3 CKD • Migraine • Corticosteroids • Systemic lupus erythematosus (SLE) • atypical antipsychotics • severe mental illness
• erectile dysfunction • a measure of systolic blood pressure variability
Development and validation of QRISK3 risk prediction algorithms to estimate future risk of cardiovascular disease:
prospective cohort study
BMJ 2017;357:j2099 doi: 10.1136/bmj.j2099 (Published 24 May 2017)
• Testosterone Deficiency Syndrome (TDS) is inadequate function of the testes
• Prevalence: Over 8% of men between age 50 and 79 years1
• Characterised by low serum testosterone (total testosterone <12nmol/l) + clinical symptoms2
– <8nmol/l - usually require treatment
– 8-12nmol/l – consider 3 months trial if appropriate or refer to specialist
• Prompt diagnosis, treatment or referral are key factors in avoiding serious long-term consequences for health
1. British Society for Sexual Medicine, Guidelines on the Management of Sexual Problems in Men:
the Role of Androgens 2010.
2. Wang C et al. Eur J Endocrinol 2008;159:507-514.
20%
31%
49%
Total T<8 nmol/L
Total T 8.0-12 nmol/L
Total T>12 nmol/L
T; Testosterone
1. Kapoor D et al. Diabetes Care 2007;30:911-917.
• 355 UK men (mean age, 58 yrs) with type 2 diabetes
51%
Testosterone
≤12 nmol/L
Less than 8nmol/L
8-12nmol/L
A self-perpetuating pathogenic cycle
Metabolic syndrome
Insulin resistance
Dyslipidemia
Arterial hypertension
Obesity
Hypogonadism
Depression
Other adverse
psychotropic effects
Osteoporosis
Anaemia
Late outcomes
Hyperinsulinemia/disturbed
Endothelial function
Type 2 diabetes mellitus
Cardiovascular events
Stroke
Erectile dysfunction
Hypothalamic-pituitary-
gonadal axis
Testicular
function Visceral
adipose tissue
+
+
+
+
+
-
+
Zitzmann Nature Endo Rev 2009
Insulin Inflammatory
cytokines
Leptin
Probability of Symptoms on the Basis of Levels of Total Testosterone
and Free Testosterone
Wu FCW et al. N Engl J Med 2010;363:123-135
0.75
0.50
0.25
0.00
Pro
babili
ty
0 10 20 30 40
Total testosterone (nmol/L)
Sexual symptoms and total testosterone
Decreased frequency of
morning erection Erectile dysfunction Decreased frequency of
sexual thoughts 11 nmol/L
8.5 nmol/L 8 nmol/L
0.75
0.50
0.25
0.00
Pro
babili
ty
0 10 20 30 40
Total testosterone (nmol/L)
Physical symptoms and total testosterone
Decreased vigerous
activity Difficulty walking >1km Decreased bending
13 nmol/L
0.75
0.50
0.25
0.00
Pro
babili
ty
0 10 20 30 40
Total testosterone (nmol/L)
Psychological symptoms and total testosterone
Fatigue Loss of energy Sadness
Hypogonadism – A combination of abnormal biochemistry and clinical symptoms
•DIMINISHED SEXUAL DESIRE
•ED
LOSS OF MORNING ERECTIONS
•Diminished energy
•Reduced vitality /well-being
•Increased fatigue
•Depressed mood
•Impaired cognition
•Diminished muscle mass and
Strength (3Kg of lean muscle/decade over 30)
•Diminished bone density
•Anaemia
•PATIENTS EXPECT BOTHERSOME
•SYMPTOMS TO BE TREATED!
•(NOT JUST STATISTICAL RISK)
Circadian rhythm of testosterone
1. Adapted from Diver M et al. Clin Endocrinol 2003;58:710-717.
15
12
10
8
0
Loss of libido p<0.001
Loss of vigour p<0.001
Obesity p<0.001
Feeling depressed p=0.001
Disturbed sleep p=0.004
Lack concentration p=0.002
Type 2 diabetes p<0.001
Hot flushes p<0.001
Erectile dysfunction p=0.003
N
84
65
67
75
Increasing
prevalence of
symptoms with
decreasing
androgen
concentrations
Zitzmann M et al. JCEM 2006;91:4335-4343.
Total testosterone nmol/L
MM Shores Arch Int Med 2006 166 1660-5
Testosterone and Survival
Benefits of Testosterone Replacement
• Increases lean body mass
• Decreases fat mass
• Increases muscle strength
• Increases libido
• Increases well being
• Decreased total cholesterol, LDL cholesterol and triglycerides
• Increases bone mineral density
• (Restores fertility)
The estimated mortality probability and 95% CI from the fitted logistic regression: Men on all and none of the above treatments
Not on any treatment Not on any treatment + 95% CI Not on any treatment – 95% CI All 3 treatments All 3 treatments + 95% CI All 3 treatments – 95% CI
World Journal of Diabetes 2017 March 15; 8(3): 104-111
Multivariate Regression model for risk of mortality (N=7860): (Anderson et al Heart 2016 )
21
Adjusted HRs and 95% CIs for the association between treatment for erectile
dysfunction, compared with no treatment for erectile dysfunction, and
outcomes after a first myocardial infarction in : 43,145 men.
Daniel P Andersson et al. Heart doi:10.1136/heartjnl-2016-
310746
Copyright © BMJ Publishing Group Ltd & British Cardiovascular Society. All rights reserved.
Dose dependent effect
How would the recognition of ED and low T work when integrated into current screening regimes?
• Matthew is 52 and has not seen a doctor for 22 years. He has become tired and lethargic and has given up physical activity, for over 5 years because of reduced strength and endurance.
• He is now longer engaging in any sort of physical activity. He feels tired at work as a factory worker and often needs to sleep in the afternoon. He falls asleep easily and has not initiated sex for 3 years and has lost his morning erections.
• His wife Tracy is concerned and makes an appointment for him to have an over-40 medical check
• He sees his GP, who takes his history • but does not ask about his erections or sexual function. • Matthew is too embarrassed to raise the issue as his doctor is running late and seems stressed. Some routine measurements and blood tests are arranged.
Matthew - Results • Weight 101 Kg, BMI 28kg/m2. Waist 102cms
• Total Cholesterol 6.6 LDL-Cholesterol 5.4, HDL-cholesterol 0.95 mmol/l TGs 2.78mmol/l. HbA1c 46mmol/mol.
• The data used in the JBS3 calculator confirms that he has a heart age 60 with a 4.7% 10 year risk of a cardiovascular event. He has metabolic syndrome and pre-diabetes.
• An exercise and dietary regime is advised with follow up in 3 months.
• Matthew returns home and tells his wife that the doctor said that he is “overweight”, but his heart is not too bad.
• He decides not to attend for the follow-up visit
Highest risk of mortality
• Had the GP asked about his erections, she would have found that he had severe ED with a SHIM score of 7.
• This would have led to mandatory measurement of his testosterone level which would have shown a level of 7.2 nmol/l with SHBG 19nmol/l. LH 2.0 iu/l.
• This would have led to the recognition that his multiple symptoms were due to testosterone deficiency.
• Traditional teaching that men such as Matthew should be managed by weight loss in the first instance
• A recent RCT showed that men treated with diet alone lose lean substantial lean muscle mass compared with men
treated with diet plus testosterone.
Fui MNT, Prendergast LA, Dupuis P. et al Effects of testosterone treatment on body fat and lean mass in obese men on a hypocaloric diet: a randomised controlled trial BMC Medicine 2016; 14:153 DOI: 10.1186/s12916-016-0700-9
Preservation of lean muscle is an important component in cardiovascular performance and in the prevention of frailty in ageing
men (Kloner).
As loss of physical strength was a major complaint, the optimal treatment for George would be lifestyle advice, testosterone therapy
plus a PDE5 inhibitor and a statin, as the presence of ED increases risk by 50% ( Araujo).
Recognition and treatment of his ED would also guarantee attendance at follow –up medical assessments.
Kloner RA, Carson C 3rd, Dobs A, Kopecky S, Mohler ER 3rd. Testosterone and Cardiovascular Disease. J Am Coll Cardiol. 2016; 67 (5): 545-57. Araujo AB, Hall SA, Ganz P, et al. Does erectile dysfunction contribute to cardiovascular disease risk prediction beyond the Framingham Risk Score? J Am Coll Cardiol. 2010; 55(4): 350-356.
The Pleomorphic effects of testosterone on Cardiovascular risk and Frailty.
Total T Free T
Consider trial of treatment if other causes
of symptoms have been excluded
8 nmol/L*
12 nmol/L* 225 pmol/L*
180 pmol/L*
Testosterone substitution required
Testosterone substitution not required
BSSM and ISSM 2017
Thresholds for T Therapy
Regarding the thresholds for treatment intervention in symptomatic men, BSSM and ISSM guidelines recommend the following:
• TT level <8 nmol/L or FT <180 pmol/L (<0.180nmol/L) (based on two separate 8–11 am levels), usually requires T Therapy • TT level >12 nmol/L, or FT of >225 pmol/L (>0.225nmol/L), does not require T Therapy • Levels between 8-12nmol/L may require a trial of T Therapy for a minimum of 6 months, based on symptoms (LoE = 3, Grade = C )
Additional recommendations include:
• Raised LH levels and testosterone below normal or in the lower quartile range, indicates testicular failure, so T Therapy should be considered
• Raised LH levels in men with normal testosterone levels but symptoms of TD, should be considered as TD
• Recent data from EMAS found that clinical symptoms were more closely related to calculated free testosterone (cFT). (LoE 2 Grade = B)
• T Calc for Free T
Treatment Risks • Serious adverse events related to T Therapy are relatively rare. They are more
significant in elderly patients and often dependent on the method of delivery.
• The intramuscular injections , (monthly or 3 monthly) are associated with pain at the injection site, changes in mood, energy and sexual desire, and rarely, coughing straight after the injection
• Transdermal gels carry a risk of interpersonal transfer, skin irritation and fluctuations in absorption.
Follow Up
For risk reduction programmes to be practical, consideration should be given to factors that are relevant, easily assessed and measured, be quantifiable and be modifiable.
There is now strong evidence that both ED and testosterone deficiency fulfil these
criteria and that both should, at the very least, now be considered as predisposing risk factors for cardiovascular disease.
ED and low testosterone are symptomatic conditions that patients would expect to be fully assessed and treated. Motivation to comply with ED and T therapy is relatively high, in contrast with other risk factors modification regimes. The reality is that, unless risk “markers” are not reclassified as “risk factors” then they will not be seen as relevant in every day practice. These issues are particularly important in younger men where current risk calculators are
of less value.
Conclusions
Less heart attacks & less strokes
Lower pulse rate
Lower BP
Longer marriage & Less divorce
Longer life
Take Home Message
Sexual activity
Global CV Risk Perspective
Vascular Disease is an Interplay of Risk Factors
Poulter N. Am J Hypertens. 1999;12:92S-95S.
age sex
Lipids BP
DM
smoking
ED LOW
T
Welcome to the World of the
Cardiac Sexologist
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