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189Male Hypogonadism
GUIDELINES ON
Male Hypogonadism
G.R. Dohle, S. Arver, C. Bettocchi, S. Kliesch, M. Punab,
W. de Ronde
Introduction
Male hypogonadism is a clinical syndrome caused by andro-
gen deficiency. It may adversely affect multiple organ func-
tions and quality of life. Androgens play a crucial role in
the development and maintenance of male reproductive and
sexual functions. Low levels of circulating androgens can
cause disturbances in male sexual development, resulting
in congenital abnormalities of the male reproductive tract.
Later in life, this may cause reduced fertility, sexual dysfunc-
tion, decreased muscle formation and bone mineralisation,
disturbances of fat metabolism, and cognitive dysfunction.
Testosterone levels decrease as a process of ageing: signs and
symptoms caused by this decline can be considered a nor-
mal part of ageing. However, low testosterone levels are also
associated with several chronic diseases, and symptomatic
patients may benefit from testosterone treatment.
Androgen deficiency increases with age; an annual decline
in circulating testosterone of 0.4-2.0% has been reported. In
middle-aged men, the incidence was found to be 6%. It is
more prevalent in older men, in men with obesity, those with
co-morbidities, and in men with a poor health status.
190 Male Hypogonadism
Aetiology and forms
Male hypogonadism can be classified in 4 forms:
1.	 Primary forms caused by testicular insufficiency;
2.	Secondary forms caused by hypothalamic-pituitary dys-
function;
3.	 Late onset hypogonadism;
4.	Male hypogonadism due to androgen receptor insensitiv-
ity.
The main causes of these different forms of hypogonadism
are highlighted in Table 1.
The type of hypogonadism has to be differentiated, as this
has implications for patient evaluation and treatment and
enables identification of patients with associated health
problems.
Table 1: Different forms of male hypogonadism and
main causes
Primary forms
(testicular insufficiency)
Main causes
Congenital forms Klinefelter syndrome
Testicular dysgenesis
(cryptorchidism)
Congenital anorchia
Acuired forms Testicular malignancy
Orchitis
Medications (chemotherapy)
Systemic diseases
Acuired anorchia
191Male Hypogonadism
Secondary forms
(hypothalamic-pituitary
dysfunctions)
Main causes
Congenital forms Kallmann syndrome
Idiopathic
hypogonadotrophic
hypogonadism (IHH)
Acuired forms Pituitary tumour
(prolactinoma)
Drugs
Systemic disease (renal
failure, hemochromatosis,
hypothyroidism, trauma,
infections)
Abuse of anabolic steroids
Morbid obesity
Radiotherapy
Late onset hypogonadism Ageing
(Combined testicular and
hypothalamic pituitary
insucfficiency)
Obesity
Chronic diseases
Poor health status
Androgen receptor
insensitivity
Partial androgen insensitivity
syndrome (PAIS)
Diagnosis
The diagnosis of male hypogonadism is based on clinical
symptoms and signs of androgen deficiency (Table 2 and 3),
together with consistently low serum testosterone levels.
192 Male Hypogonadism
Table 2: Signs and symptoms suggesting prepubertal-
onset hypogonadism
Small testes
Cryptorchidism
Gynaecomastia
High voice
Unclosed epiphyses
Linear growth into adulthood
Eunuchoid habitus
Sparse body/facial hair
Infertility
Low bone mass
Sarcopenia
Reduced sexual desire/activity
Table 3: Signs and symptoms associated with late-
onset hypogonadism
Loss of libido
Erectile dysfunction
Sarcopenia
Low bone mass
Depressive thoughts
Changes in mood, fatigue and anger
Sleep disturbances
Loss of body hair
Hot flushes
Loss of vigour
Insulin resistance
Metabolic syndrome
193Male Hypogonadism
Visceral obesity
Gynaecomastia
Diminished cognitive functions
Routine screening for testosterone deficiency is not indicated.
However, testosterone assessment should be done in men
with:
•	 Pituitary mass, following radiation involving the sellar
region and other diseases in the hypothalamic and sellar
region;
•	 End-stage renal disease receiving haemodialysis;
•	 Treatment with medications that cause suppression of tes-
tosterone levels e.g. corticosteroids and opiates;
•	 Moderate to severe chronic obstructive lung disease;
•	 Infertility;
•	 Osteoporosis or low-trauma fractures;
•	 Human immunodeficiency virus (HIV) infection with sar-
copenia;
•	 Type 2 diabetes.
Acquired hypogonadotropic hypogonadism (secondary
forms) can be caused by some drugs, hormones, anabolic
steroids and by tumours of the pituitary gland. Imaging (CT
scan or MRI) of the sellar region and complete endocrine
work-up is requested when a pituitary tumour is suspected.
Recommendations for screening GR
Screening for testosterone deficiency is only recom-
mended in adult men with consistent and preferably
multiple signs and symptoms, listed in Tables 2 and 3.
C
194 Male Hypogonadism
Adult men with established severe hypogonadism
should be screened for concomitant osteoporosis.
B
Total testosterone assessment should be repeated at
least on two occasions with a reliable method.
A
- In men with total testosterone levels close to the
lower normal range (8-12 nmol/l), the free testo-
sterone level should be measured to strengthen the
laboratory assessment.
- In men with suspected or known abnormal sex
hormone-binding globulin (SHBG) levels, free testo-
sterone should also be included.
Treatment
The aim of treatment is to restore testosterone levels to the
physiological range and thereby improve the patient’s quality
of life. Indications and contraindications are listed in Tables
4 and 5.
Table 4: Indications for testosterone treatment
Adult men with consistent and preferably multiple signs
and symptoms of hypogonadism (listed in Tables 2 and 3)
and low testosterone
Delayed puberty (idiopathic, Kallmann syndrome)
Klinefelter syndrome with hypogonadism
Sexual dysfunction and low testosterone
Low muscle strength and bone mass in hypogonadism
Hypopituitarism
Testicular insufficiency and symptomatic hypogonadism
195Male Hypogonadism
Table 5: Contraindications against testosterone
treatment
Prostate cancer
Prostate-specific antigen (PSA)  4 ng/mL
Male breast cancer
Severe sleep apnoea
Male infertility
Haematocrit  50%
Severe lower urinary tract symptoms due to benign pros-
tatic enlargement
Choice of treatment
Testosterone replacement therapy (TRT) is safe and effective
and the agents are available as oral preparations, intramuscu-
lar injections, and transdermal gel or patches (Table 6).
Table 6: Testosterone preparations for replacement
therapy
Formulation Administration Advantages Disadvantages
Testosterone
undecanoate
Oral; 2-6 cps
every 6 h
Absorbed
through the
lymphatic
system, with
consequent
reduction of
liver involve-
ment
Variable levels
of testosterone
above and
below the
mid-range.
Need for
several doses
per day with
intake of fatty
food
196 Male Hypogonadism
Testosterone
cypionate
Intramuscular;
one injec-
tion every 2-3
weeks
Short-acting
preparation
that allows
drug with-
drawal in case
of onset of
side effects
Possible fluc-
tuation of
testosterone
levels
Testosterone
enanthate
Intramuscular;
one injec-
tion every 2-3
weeks
Short-acting
preparation
that allows
drug with-
drawal in case
of onset of
side effects
Possible fluc-
tuation of
testosterone
levels
Testosterone
undecanoate
Intramuscular;
one injection
every 10-14
weeks
Steady-state
testosterone
levels without
fluctuation
Long-acting
preparation
that cannot
allow drug
withdrawal in
case of onset
of side effects
Transdermal
testosterone
Gel or skin
patches; daily
application
Steady-state
testosterone
level without
fluctuation
Skin irritation
at the site of
application
and risk of
interpersonal
transfer
Sublingual
testosterone
Sublingual;
daily doses
Rapid absorp-
tion and
achievement
of physiologi-
cal serum level
of testosterone
Local irritation
197Male Hypogonadism
Buccal testo-
sterone
Buccal tablet;
two doses per
day
Rapid absorp-
tion and
achievement
of physiologi-
cal serum level
of testosterone
Irritation and
pain at the site
of application
Subdermal
depots
Subdermal
implant every
5-7 months
Long duration
and constant
serum testo-
sterone level
Risk of infec-
tion and
extrusion of
the implants
In patients with secondary hypogonadism, anti-oestrogens
or hormonal stimulation with hCG and FSH or alternatively
GnRH can restore testosterone production.
Recommendations GR
The patient should be fully informed about expected
benefits and side effects of each treatment option. The
selection of the preparation should be a joint decision
by an informed patient and the physician.
A
Short-acting preparations may initially be preferred to
long-acting depot administration when starting treat-
ment. Patients can switch to a long-acting depot if
preferred and side effects are absent or minimal.
B
Human chorionic gonadotrophin (hCG) treatment
can only be recommended for hypogonadal patients
who are receiving simultaneous fertility treatment.
B
Risk factors in testosterone treatment
•	 Case reports and small cohort studies point to a possible
correlation between TRT and the onset of breast cancer,
198 Male Hypogonadism
but there is as yet a lack of strong evidence for this rela-
tionship.
•	 Randomised controlled trials support the hypothesis that
TRT does not result in changes in prostatic histology.
However, there are not yet data available that show long-
term prostatic safety of TRT.
•	 Testosterone therapy is not related to the development
of de novo cardiovascular events. However, patients with
severe cardiovascular diseases should be screened first by
a cardiologist before TRT is initiated.
Recommendations for initiation of treatment GR
Haematological, cardiovascular, breast and prostatic
assessment should be performed before the start of
treatment.
A
Men with severe cardiovascular co-morbidity should
be assessed by a cardiologist before TRT is initiated
and there should be close cardiovascular monitoring
during TRT.
C
Prostate health should be assessed by digital rectal
examination (DRE) and PSA before the start of TRT.
A
In patients treated for localised prostate cancer
and without signs of prostate cancer recurrence,
testosterone therapy should not start before at least 1
year of follow-up.
C
Recommendations for monitoring GR
The response to treatment (symptoms and
testosterone serum levels) should be assessed 3, 6 and
12 months after the onset of treatment, and thereafter
annually.
C
199Male Hypogonadism
In men with an abnormal bone mineral density
(BMD), BMD measurements should be repeated 6
and 12 months after the start of TRT and thereafter
annually.
C
Haematocrit should be monitored at 3, 6 and 12
months and thereafter annually. The testosterone
dosage should be decreased, or therapy discontinued
if the haematocrit increases above normal levels.
C
Prostate health should be monitored by PSA testing at
3, 6 and 12 months and thereafter annually.
C
Routine screening of potential cardiovascular side
effects is not indicated in men receiving TRT.
A
This short booklet text is based on the more comprehensive EAU guidelines
(978-90-79754-83-0), available to all members of the European Association
of Urology at their website, http://www.uroweb.org.

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15 male hypogonadism

  • 1. 189Male Hypogonadism GUIDELINES ON Male Hypogonadism G.R. Dohle, S. Arver, C. Bettocchi, S. Kliesch, M. Punab, W. de Ronde Introduction Male hypogonadism is a clinical syndrome caused by andro- gen deficiency. It may adversely affect multiple organ func- tions and quality of life. Androgens play a crucial role in the development and maintenance of male reproductive and sexual functions. Low levels of circulating androgens can cause disturbances in male sexual development, resulting in congenital abnormalities of the male reproductive tract. Later in life, this may cause reduced fertility, sexual dysfunc- tion, decreased muscle formation and bone mineralisation, disturbances of fat metabolism, and cognitive dysfunction. Testosterone levels decrease as a process of ageing: signs and symptoms caused by this decline can be considered a nor- mal part of ageing. However, low testosterone levels are also associated with several chronic diseases, and symptomatic patients may benefit from testosterone treatment. Androgen deficiency increases with age; an annual decline in circulating testosterone of 0.4-2.0% has been reported. In middle-aged men, the incidence was found to be 6%. It is more prevalent in older men, in men with obesity, those with co-morbidities, and in men with a poor health status.
  • 2. 190 Male Hypogonadism Aetiology and forms Male hypogonadism can be classified in 4 forms: 1. Primary forms caused by testicular insufficiency; 2. Secondary forms caused by hypothalamic-pituitary dys- function; 3. Late onset hypogonadism; 4. Male hypogonadism due to androgen receptor insensitiv- ity. The main causes of these different forms of hypogonadism are highlighted in Table 1. The type of hypogonadism has to be differentiated, as this has implications for patient evaluation and treatment and enables identification of patients with associated health problems. Table 1: Different forms of male hypogonadism and main causes Primary forms (testicular insufficiency) Main causes Congenital forms Klinefelter syndrome Testicular dysgenesis (cryptorchidism) Congenital anorchia Acuired forms Testicular malignancy Orchitis Medications (chemotherapy) Systemic diseases Acuired anorchia
  • 3. 191Male Hypogonadism Secondary forms (hypothalamic-pituitary dysfunctions) Main causes Congenital forms Kallmann syndrome Idiopathic hypogonadotrophic hypogonadism (IHH) Acuired forms Pituitary tumour (prolactinoma) Drugs Systemic disease (renal failure, hemochromatosis, hypothyroidism, trauma, infections) Abuse of anabolic steroids Morbid obesity Radiotherapy Late onset hypogonadism Ageing (Combined testicular and hypothalamic pituitary insucfficiency) Obesity Chronic diseases Poor health status Androgen receptor insensitivity Partial androgen insensitivity syndrome (PAIS) Diagnosis The diagnosis of male hypogonadism is based on clinical symptoms and signs of androgen deficiency (Table 2 and 3), together with consistently low serum testosterone levels.
  • 4. 192 Male Hypogonadism Table 2: Signs and symptoms suggesting prepubertal- onset hypogonadism Small testes Cryptorchidism Gynaecomastia High voice Unclosed epiphyses Linear growth into adulthood Eunuchoid habitus Sparse body/facial hair Infertility Low bone mass Sarcopenia Reduced sexual desire/activity Table 3: Signs and symptoms associated with late- onset hypogonadism Loss of libido Erectile dysfunction Sarcopenia Low bone mass Depressive thoughts Changes in mood, fatigue and anger Sleep disturbances Loss of body hair Hot flushes Loss of vigour Insulin resistance Metabolic syndrome
  • 5. 193Male Hypogonadism Visceral obesity Gynaecomastia Diminished cognitive functions Routine screening for testosterone deficiency is not indicated. However, testosterone assessment should be done in men with: • Pituitary mass, following radiation involving the sellar region and other diseases in the hypothalamic and sellar region; • End-stage renal disease receiving haemodialysis; • Treatment with medications that cause suppression of tes- tosterone levels e.g. corticosteroids and opiates; • Moderate to severe chronic obstructive lung disease; • Infertility; • Osteoporosis or low-trauma fractures; • Human immunodeficiency virus (HIV) infection with sar- copenia; • Type 2 diabetes. Acquired hypogonadotropic hypogonadism (secondary forms) can be caused by some drugs, hormones, anabolic steroids and by tumours of the pituitary gland. Imaging (CT scan or MRI) of the sellar region and complete endocrine work-up is requested when a pituitary tumour is suspected. Recommendations for screening GR Screening for testosterone deficiency is only recom- mended in adult men with consistent and preferably multiple signs and symptoms, listed in Tables 2 and 3. C
  • 6. 194 Male Hypogonadism Adult men with established severe hypogonadism should be screened for concomitant osteoporosis. B Total testosterone assessment should be repeated at least on two occasions with a reliable method. A - In men with total testosterone levels close to the lower normal range (8-12 nmol/l), the free testo- sterone level should be measured to strengthen the laboratory assessment. - In men with suspected or known abnormal sex hormone-binding globulin (SHBG) levels, free testo- sterone should also be included. Treatment The aim of treatment is to restore testosterone levels to the physiological range and thereby improve the patient’s quality of life. Indications and contraindications are listed in Tables 4 and 5. Table 4: Indications for testosterone treatment Adult men with consistent and preferably multiple signs and symptoms of hypogonadism (listed in Tables 2 and 3) and low testosterone Delayed puberty (idiopathic, Kallmann syndrome) Klinefelter syndrome with hypogonadism Sexual dysfunction and low testosterone Low muscle strength and bone mass in hypogonadism Hypopituitarism Testicular insufficiency and symptomatic hypogonadism
  • 7. 195Male Hypogonadism Table 5: Contraindications against testosterone treatment Prostate cancer Prostate-specific antigen (PSA) 4 ng/mL Male breast cancer Severe sleep apnoea Male infertility Haematocrit 50% Severe lower urinary tract symptoms due to benign pros- tatic enlargement Choice of treatment Testosterone replacement therapy (TRT) is safe and effective and the agents are available as oral preparations, intramuscu- lar injections, and transdermal gel or patches (Table 6). Table 6: Testosterone preparations for replacement therapy Formulation Administration Advantages Disadvantages Testosterone undecanoate Oral; 2-6 cps every 6 h Absorbed through the lymphatic system, with consequent reduction of liver involve- ment Variable levels of testosterone above and below the mid-range. Need for several doses per day with intake of fatty food
  • 8. 196 Male Hypogonadism Testosterone cypionate Intramuscular; one injec- tion every 2-3 weeks Short-acting preparation that allows drug with- drawal in case of onset of side effects Possible fluc- tuation of testosterone levels Testosterone enanthate Intramuscular; one injec- tion every 2-3 weeks Short-acting preparation that allows drug with- drawal in case of onset of side effects Possible fluc- tuation of testosterone levels Testosterone undecanoate Intramuscular; one injection every 10-14 weeks Steady-state testosterone levels without fluctuation Long-acting preparation that cannot allow drug withdrawal in case of onset of side effects Transdermal testosterone Gel or skin patches; daily application Steady-state testosterone level without fluctuation Skin irritation at the site of application and risk of interpersonal transfer Sublingual testosterone Sublingual; daily doses Rapid absorp- tion and achievement of physiologi- cal serum level of testosterone Local irritation
  • 9. 197Male Hypogonadism Buccal testo- sterone Buccal tablet; two doses per day Rapid absorp- tion and achievement of physiologi- cal serum level of testosterone Irritation and pain at the site of application Subdermal depots Subdermal implant every 5-7 months Long duration and constant serum testo- sterone level Risk of infec- tion and extrusion of the implants In patients with secondary hypogonadism, anti-oestrogens or hormonal stimulation with hCG and FSH or alternatively GnRH can restore testosterone production. Recommendations GR The patient should be fully informed about expected benefits and side effects of each treatment option. The selection of the preparation should be a joint decision by an informed patient and the physician. A Short-acting preparations may initially be preferred to long-acting depot administration when starting treat- ment. Patients can switch to a long-acting depot if preferred and side effects are absent or minimal. B Human chorionic gonadotrophin (hCG) treatment can only be recommended for hypogonadal patients who are receiving simultaneous fertility treatment. B Risk factors in testosterone treatment • Case reports and small cohort studies point to a possible correlation between TRT and the onset of breast cancer,
  • 10. 198 Male Hypogonadism but there is as yet a lack of strong evidence for this rela- tionship. • Randomised controlled trials support the hypothesis that TRT does not result in changes in prostatic histology. However, there are not yet data available that show long- term prostatic safety of TRT. • Testosterone therapy is not related to the development of de novo cardiovascular events. However, patients with severe cardiovascular diseases should be screened first by a cardiologist before TRT is initiated. Recommendations for initiation of treatment GR Haematological, cardiovascular, breast and prostatic assessment should be performed before the start of treatment. A Men with severe cardiovascular co-morbidity should be assessed by a cardiologist before TRT is initiated and there should be close cardiovascular monitoring during TRT. C Prostate health should be assessed by digital rectal examination (DRE) and PSA before the start of TRT. A In patients treated for localised prostate cancer and without signs of prostate cancer recurrence, testosterone therapy should not start before at least 1 year of follow-up. C Recommendations for monitoring GR The response to treatment (symptoms and testosterone serum levels) should be assessed 3, 6 and 12 months after the onset of treatment, and thereafter annually. C
  • 11. 199Male Hypogonadism In men with an abnormal bone mineral density (BMD), BMD measurements should be repeated 6 and 12 months after the start of TRT and thereafter annually. C Haematocrit should be monitored at 3, 6 and 12 months and thereafter annually. The testosterone dosage should be decreased, or therapy discontinued if the haematocrit increases above normal levels. C Prostate health should be monitored by PSA testing at 3, 6 and 12 months and thereafter annually. C Routine screening of potential cardiovascular side effects is not indicated in men receiving TRT. A This short booklet text is based on the more comprehensive EAU guidelines (978-90-79754-83-0), available to all members of the European Association of Urology at their website, http://www.uroweb.org.