Article Type
Changed
Mon, 01/14/2019 - 11:24
Display Headline
What screening tests should you use to evaluate a man with low testosterone?
EVIDENCE-BASED ANSWER

Obtain a repeat morning testosterone level, as well as levels of follicle-stimulating hormone (FSH), luteinizing hormone (LH), and prolactin to help understand the cause of low testosterone when there is a lack of adequate empiric evidence to guide evaluation, advise the experts. When low or normal FSH and LH levels accompany low testosterone, evaluation of the pituitary gland is recommended.

Chromosomal studies are indicated in prepubertal males with low testosterone and elevated FSH and LH levels to assess for Klinefelter syndrome. Perform a semen analysis if fertility is an issue. Bone densitometry is indicated in men with chronic hypogonadism to identify increased risk of hip fracture (strength of all recommendations: C, consensus guidelines and disease-oriented evidence).

Clinical commentary

Diagnosis is often straightforward, but treatment…not so much
Pamela A. Williams, MD
Uniformed Services University of the Health Sciences, Bethesda, Md

The causes of low testosterone are diverse and vary across the life span (TABLE).1,2

Although screening tests are integral to the evaluation, a successful diagnostic approach must begin with a detailed history and physical exam. Clinical clues coupled with judiciously selected tests typically lead to a straightforward diagnosis.

The decision whether or not to treat a patient diagnosed with partial androgen deficiency of aging is often less clear, especially when clinical symptoms are minimal or absent. The benefits of testosterone replacement therapy are significant, but so are the potential risks. Shared decision making with the patient is key to this dilemma.

Evidence summary

Our search retrieved no randomized controlled clinical trials evaluating the screening tests required to work-up a male with low testosterone. We therefore examined 2 consensus guidelines, 9 review articles, and disease-oriented evidence. The recommendations discussed here are based primarily on consensus guidelines and disease-oriented evidence.

Hypogonadism increases with age

Hypogonadism is a common endocrinologic disorder in men. Advancing age, increased life expectancy, and a rising prevalence of obesity and type 2 diabetes may increase the occurrence of hypogonadism.3 Many cases result from partial androgen deficiency in the aging male, because testosterone levels decline an estimated 1% to 2% per year in adult men.1,3 A focused, cost-effective work-up will become ever more critical because an estimated 19% of men will be 65 years or older by 2050.4

TABLE
Causes of hypogonadism

CLASSLOCATIONCAUSES
Primary (low testosterone, elevated FSH)TestesCongenital
Biosynthesis and chromosomal disorders (rare)
Klinefelter syndrome (most common, 1:500-1000 males)
Acquired
Chemotherapeutic agents
Autoimmune disorders
Aging
Drugs
Toxins (eg, alcohol)
Infection
Trauma
Radiation
Idiopathic causes
Secondary (low testosterone, normal or low FSH)Pituitary glandCongenital
Kallmann syndrome (1:10,000 male births)
Idiopathic causes
Abnormal structural hormone defects
Acquired
Chronic disease
Drugs (eg, chronic opioids)
Infection (eg, HIV)
Trauma
Tumors
Idiopathic causes
Age-related (low testosterone, normal or elevated FSH)Testes/hypothalamus
Aging (common; 1%-2% per year after 65 years of age, 30%-70% at 60-80 years of age)
FSH, follicle-stimulating hormone; HIV, human immunodeficiency virus.
Sources: Darby E et al1 and Badar F et al.2
 

Serum testosterone: The first-choice test

Serum testosterone measurements are considered the initial test of choice be-cause they’re reliable, inexpensive, and widely available. Testosterone levels vary from hour to hour and diurnally, so a repeat morning measurement is recommended to confirm subnormal levels.3,5

In some cases—including patients with obesity, type 2 diabetes, or hypothyroidism—the total testosterone level can be misleading; tests for free testosterone and sex hormone-binding globulin levels should be ordered. These tests can also help evaluate men with low-normal total testosterone levels (200-400 ng/dL).6,7

 

 

Is the patient pre- or postpubertal?

Assessment of low testosterone should distinguish between pre- and postpubertal males. In prepubertal males, chromosomal analysis is indicated because hypothalamic-pituitary-gonadal axis defects are common—especially Klinefelter syndrome (1 in 500 males).6,8

Men with very low testosterone levels (<150 ng/dL) or signs and symptoms suggesting pituitary pathology warrant pituitary imaging and measurement of thyroxine, cortisol, and prolactin levels.6 Both pre- and postpubertal males with low testosterone should have FSH, LH, and prolactin levels tested to differentiate primary from secondary hypogonadism.6,9

Be alert for hemochromatosis and low bone density

Order biopsy or ultrasound examination of testicular masses and iron studies if hemochromatosis is suspected. Hemochromatosis is the most common single gene disorder of Caucasian Americans (1 in 250-300 are homozygous; 1 in 10 are heterozygous) and is associated with hypogonadotrophic hypogonadism.5,10 In a series of 3 studies, 30% (26 of 89) of men with hemochromatosis had hypogonadism.11 The prevalence of hemochromatosis in males with hypogonadism hasn’t been reported.

 

Because chronic hypogonadism leads to low bone density and increased risk of fracture, baseline bone densitometry may be prudent.12 A chart review study of nursing home residents found that 66% of men with hip fractures and 20% of men with vertebral fractures had low testosterone.13 Notably, 50% of men in their 80s have testosterone levels in the hypogonadal range (<300 ng/dL), compared with 12% of men <50 years.1,14

Recommendations

Scant guidance is available concerning what screening tests to order for a male with low testosterone. The United States Preventive Services Task Force and Canadian Task Force on Preventive Health Care make no recommendations; the Cochrane collaboration has no reviews on the topic. The American Association of Clinical Endocrinologists’ (AACE) guidelines are based on expert opinion.3

The AACE consensus guideline used peer review for validation and didn’t specify the method used to assess the quality and strength of the evidence used to write the statement. The AACE guideline recommends a history and physical exam, obtaining repeat morning testosterone levels, prolactin, FSH, LH, bone densitometry, and a semen analysis if fertility is an issue.

In acquired hypogonadism, pituitary imaging is recommended along with thyroid, adrenal, and growth hormone axis testing. Prepubertal males should undergo chromosome analysis, and men with a suspected mass should have a testicular ultrasound examination.

References

1. Darby E, Anawalt BD. Male hypogonadism: an update on diagnosis and treatment. Treat Endocrinol. 2005;4:293-309.

2. Badar F, Mirmira V, Hemady N. Hypogonadism in men: underdiagnosed and undertreated. Resid Staff Physician. 2006;52(6):6-12.

3. American Association of Clinical Endocrinologists American Association of Clinical Endocrinologists medical guidelines for clinical practice for the evaluation and treatment of hypogonadism in adult male patients—2002 update. Endocr Prac. 2002;8:440-456.

4. Smyth CM, Bremner WJ. Klinefelter syndrome. Arch Intern Med. 1998;158:1309-1314.

5. Spratt DI, O’Dea LS, Schoenfeld D, et al. Neuroendocrine-gonadal axis in men: frequent sampling of LH, FSH, and testosterone. Am J Physiol. 1988;254(5 Part 1):E658-E666.

6. Seftel AD. Male hypogonadism. Part I: epidemiology of hypogonadism. Int J Impot Res. 2006;18:115-120.

7. Sadovsky R, Dhindsa S, Margo K. Testosterone deficiency: which patients should you screen and treat? J Fam Pract. 2007;56(5 suppl):S1-S24.

8. Bhasin S, Jameson DL. Disorders of the testes and male reproductive system. Ch 340. In: Fauci AS, Braunwald E, Kasper DL, et al, eds. Harrison’s Principles of Internal Medicine. 17th ed. New York: McGraw-Hill; 2008.

9. US Census Bureau. US Interim projections by age, sex, race, and Hispanic origin: 2000-2050. Created March 18, 2004. Available at: www.census.gov/ipc/www/usinterimproj/. Accessed March 14, 2006.

10. Schrier SL, Bacon BR. Clinical manifestations of hereditary hemochromatosis. Up to Date [online database]. Version 15.1. Waltham, Mass: UpToDate; 2008.

11. Harman SM, Metter EJ, Tobin JD, et al. Longitudinal effects of aging on serum total and free testosterone levels in healthy men. Baltimore Longitudinal Study of Aging. J Clin Endocrinol Metab. 2001;86:724-731.

12. Kaufman JM, Johnell O, Abadie E, et al. Background for studies on the treatment of male osteoporosis: state of the art. Ann Rheum Dis. 2000;59:765-772.

13. Abbasi AA, Rudman D, Wilson CR, et al. Observations on nursing home residents with a history of hip fracture. Am J Med Sci. 1995;310:229-234.

14. Pietrangelo A. Hereditary hemochromatosis—a new look at an old disease. N Engl J Med. 2004;350:2383-2397.

Article PDF
Author and Disclosure Information

Robert P. Jackman, MD
Cascades East Family Medicine Residency, Oregon Health and Science University, Klamath Falls, Ore

Dolores Zegar Judkins, MLS
Oregon Health and Science University, Portland, Ore

Issue
The Journal of Family Practice - 57(11)
Publications
Topics
Page Number
756-758
Legacy Keywords
Robert P. Jackman; hypogonadism; follicle-stimulating hormone; luteinizing hormone; prolactin
Sections
Author and Disclosure Information

Robert P. Jackman, MD
Cascades East Family Medicine Residency, Oregon Health and Science University, Klamath Falls, Ore

Dolores Zegar Judkins, MLS
Oregon Health and Science University, Portland, Ore

Author and Disclosure Information

Robert P. Jackman, MD
Cascades East Family Medicine Residency, Oregon Health and Science University, Klamath Falls, Ore

Dolores Zegar Judkins, MLS
Oregon Health and Science University, Portland, Ore

Article PDF
Article PDF
EVIDENCE-BASED ANSWER

Obtain a repeat morning testosterone level, as well as levels of follicle-stimulating hormone (FSH), luteinizing hormone (LH), and prolactin to help understand the cause of low testosterone when there is a lack of adequate empiric evidence to guide evaluation, advise the experts. When low or normal FSH and LH levels accompany low testosterone, evaluation of the pituitary gland is recommended.

Chromosomal studies are indicated in prepubertal males with low testosterone and elevated FSH and LH levels to assess for Klinefelter syndrome. Perform a semen analysis if fertility is an issue. Bone densitometry is indicated in men with chronic hypogonadism to identify increased risk of hip fracture (strength of all recommendations: C, consensus guidelines and disease-oriented evidence).

Clinical commentary

Diagnosis is often straightforward, but treatment…not so much
Pamela A. Williams, MD
Uniformed Services University of the Health Sciences, Bethesda, Md

The causes of low testosterone are diverse and vary across the life span (TABLE).1,2

Although screening tests are integral to the evaluation, a successful diagnostic approach must begin with a detailed history and physical exam. Clinical clues coupled with judiciously selected tests typically lead to a straightforward diagnosis.

The decision whether or not to treat a patient diagnosed with partial androgen deficiency of aging is often less clear, especially when clinical symptoms are minimal or absent. The benefits of testosterone replacement therapy are significant, but so are the potential risks. Shared decision making with the patient is key to this dilemma.

Evidence summary

Our search retrieved no randomized controlled clinical trials evaluating the screening tests required to work-up a male with low testosterone. We therefore examined 2 consensus guidelines, 9 review articles, and disease-oriented evidence. The recommendations discussed here are based primarily on consensus guidelines and disease-oriented evidence.

Hypogonadism increases with age

Hypogonadism is a common endocrinologic disorder in men. Advancing age, increased life expectancy, and a rising prevalence of obesity and type 2 diabetes may increase the occurrence of hypogonadism.3 Many cases result from partial androgen deficiency in the aging male, because testosterone levels decline an estimated 1% to 2% per year in adult men.1,3 A focused, cost-effective work-up will become ever more critical because an estimated 19% of men will be 65 years or older by 2050.4

TABLE
Causes of hypogonadism

CLASSLOCATIONCAUSES
Primary (low testosterone, elevated FSH)TestesCongenital
Biosynthesis and chromosomal disorders (rare)
Klinefelter syndrome (most common, 1:500-1000 males)
Acquired
Chemotherapeutic agents
Autoimmune disorders
Aging
Drugs
Toxins (eg, alcohol)
Infection
Trauma
Radiation
Idiopathic causes
Secondary (low testosterone, normal or low FSH)Pituitary glandCongenital
Kallmann syndrome (1:10,000 male births)
Idiopathic causes
Abnormal structural hormone defects
Acquired
Chronic disease
Drugs (eg, chronic opioids)
Infection (eg, HIV)
Trauma
Tumors
Idiopathic causes
Age-related (low testosterone, normal or elevated FSH)Testes/hypothalamus
Aging (common; 1%-2% per year after 65 years of age, 30%-70% at 60-80 years of age)
FSH, follicle-stimulating hormone; HIV, human immunodeficiency virus.
Sources: Darby E et al1 and Badar F et al.2
 

Serum testosterone: The first-choice test

Serum testosterone measurements are considered the initial test of choice be-cause they’re reliable, inexpensive, and widely available. Testosterone levels vary from hour to hour and diurnally, so a repeat morning measurement is recommended to confirm subnormal levels.3,5

In some cases—including patients with obesity, type 2 diabetes, or hypothyroidism—the total testosterone level can be misleading; tests for free testosterone and sex hormone-binding globulin levels should be ordered. These tests can also help evaluate men with low-normal total testosterone levels (200-400 ng/dL).6,7

 

 

Is the patient pre- or postpubertal?

Assessment of low testosterone should distinguish between pre- and postpubertal males. In prepubertal males, chromosomal analysis is indicated because hypothalamic-pituitary-gonadal axis defects are common—especially Klinefelter syndrome (1 in 500 males).6,8

Men with very low testosterone levels (<150 ng/dL) or signs and symptoms suggesting pituitary pathology warrant pituitary imaging and measurement of thyroxine, cortisol, and prolactin levels.6 Both pre- and postpubertal males with low testosterone should have FSH, LH, and prolactin levels tested to differentiate primary from secondary hypogonadism.6,9

Be alert for hemochromatosis and low bone density

Order biopsy or ultrasound examination of testicular masses and iron studies if hemochromatosis is suspected. Hemochromatosis is the most common single gene disorder of Caucasian Americans (1 in 250-300 are homozygous; 1 in 10 are heterozygous) and is associated with hypogonadotrophic hypogonadism.5,10 In a series of 3 studies, 30% (26 of 89) of men with hemochromatosis had hypogonadism.11 The prevalence of hemochromatosis in males with hypogonadism hasn’t been reported.

 

Because chronic hypogonadism leads to low bone density and increased risk of fracture, baseline bone densitometry may be prudent.12 A chart review study of nursing home residents found that 66% of men with hip fractures and 20% of men with vertebral fractures had low testosterone.13 Notably, 50% of men in their 80s have testosterone levels in the hypogonadal range (<300 ng/dL), compared with 12% of men <50 years.1,14

Recommendations

Scant guidance is available concerning what screening tests to order for a male with low testosterone. The United States Preventive Services Task Force and Canadian Task Force on Preventive Health Care make no recommendations; the Cochrane collaboration has no reviews on the topic. The American Association of Clinical Endocrinologists’ (AACE) guidelines are based on expert opinion.3

The AACE consensus guideline used peer review for validation and didn’t specify the method used to assess the quality and strength of the evidence used to write the statement. The AACE guideline recommends a history and physical exam, obtaining repeat morning testosterone levels, prolactin, FSH, LH, bone densitometry, and a semen analysis if fertility is an issue.

In acquired hypogonadism, pituitary imaging is recommended along with thyroid, adrenal, and growth hormone axis testing. Prepubertal males should undergo chromosome analysis, and men with a suspected mass should have a testicular ultrasound examination.

EVIDENCE-BASED ANSWER

Obtain a repeat morning testosterone level, as well as levels of follicle-stimulating hormone (FSH), luteinizing hormone (LH), and prolactin to help understand the cause of low testosterone when there is a lack of adequate empiric evidence to guide evaluation, advise the experts. When low or normal FSH and LH levels accompany low testosterone, evaluation of the pituitary gland is recommended.

Chromosomal studies are indicated in prepubertal males with low testosterone and elevated FSH and LH levels to assess for Klinefelter syndrome. Perform a semen analysis if fertility is an issue. Bone densitometry is indicated in men with chronic hypogonadism to identify increased risk of hip fracture (strength of all recommendations: C, consensus guidelines and disease-oriented evidence).

Clinical commentary

Diagnosis is often straightforward, but treatment…not so much
Pamela A. Williams, MD
Uniformed Services University of the Health Sciences, Bethesda, Md

The causes of low testosterone are diverse and vary across the life span (TABLE).1,2

Although screening tests are integral to the evaluation, a successful diagnostic approach must begin with a detailed history and physical exam. Clinical clues coupled with judiciously selected tests typically lead to a straightforward diagnosis.

The decision whether or not to treat a patient diagnosed with partial androgen deficiency of aging is often less clear, especially when clinical symptoms are minimal or absent. The benefits of testosterone replacement therapy are significant, but so are the potential risks. Shared decision making with the patient is key to this dilemma.

Evidence summary

Our search retrieved no randomized controlled clinical trials evaluating the screening tests required to work-up a male with low testosterone. We therefore examined 2 consensus guidelines, 9 review articles, and disease-oriented evidence. The recommendations discussed here are based primarily on consensus guidelines and disease-oriented evidence.

Hypogonadism increases with age

Hypogonadism is a common endocrinologic disorder in men. Advancing age, increased life expectancy, and a rising prevalence of obesity and type 2 diabetes may increase the occurrence of hypogonadism.3 Many cases result from partial androgen deficiency in the aging male, because testosterone levels decline an estimated 1% to 2% per year in adult men.1,3 A focused, cost-effective work-up will become ever more critical because an estimated 19% of men will be 65 years or older by 2050.4

TABLE
Causes of hypogonadism

CLASSLOCATIONCAUSES
Primary (low testosterone, elevated FSH)TestesCongenital
Biosynthesis and chromosomal disorders (rare)
Klinefelter syndrome (most common, 1:500-1000 males)
Acquired
Chemotherapeutic agents
Autoimmune disorders
Aging
Drugs
Toxins (eg, alcohol)
Infection
Trauma
Radiation
Idiopathic causes
Secondary (low testosterone, normal or low FSH)Pituitary glandCongenital
Kallmann syndrome (1:10,000 male births)
Idiopathic causes
Abnormal structural hormone defects
Acquired
Chronic disease
Drugs (eg, chronic opioids)
Infection (eg, HIV)
Trauma
Tumors
Idiopathic causes
Age-related (low testosterone, normal or elevated FSH)Testes/hypothalamus
Aging (common; 1%-2% per year after 65 years of age, 30%-70% at 60-80 years of age)
FSH, follicle-stimulating hormone; HIV, human immunodeficiency virus.
Sources: Darby E et al1 and Badar F et al.2
 

Serum testosterone: The first-choice test

Serum testosterone measurements are considered the initial test of choice be-cause they’re reliable, inexpensive, and widely available. Testosterone levels vary from hour to hour and diurnally, so a repeat morning measurement is recommended to confirm subnormal levels.3,5

In some cases—including patients with obesity, type 2 diabetes, or hypothyroidism—the total testosterone level can be misleading; tests for free testosterone and sex hormone-binding globulin levels should be ordered. These tests can also help evaluate men with low-normal total testosterone levels (200-400 ng/dL).6,7

 

 

Is the patient pre- or postpubertal?

Assessment of low testosterone should distinguish between pre- and postpubertal males. In prepubertal males, chromosomal analysis is indicated because hypothalamic-pituitary-gonadal axis defects are common—especially Klinefelter syndrome (1 in 500 males).6,8

Men with very low testosterone levels (<150 ng/dL) or signs and symptoms suggesting pituitary pathology warrant pituitary imaging and measurement of thyroxine, cortisol, and prolactin levels.6 Both pre- and postpubertal males with low testosterone should have FSH, LH, and prolactin levels tested to differentiate primary from secondary hypogonadism.6,9

Be alert for hemochromatosis and low bone density

Order biopsy or ultrasound examination of testicular masses and iron studies if hemochromatosis is suspected. Hemochromatosis is the most common single gene disorder of Caucasian Americans (1 in 250-300 are homozygous; 1 in 10 are heterozygous) and is associated with hypogonadotrophic hypogonadism.5,10 In a series of 3 studies, 30% (26 of 89) of men with hemochromatosis had hypogonadism.11 The prevalence of hemochromatosis in males with hypogonadism hasn’t been reported.

 

Because chronic hypogonadism leads to low bone density and increased risk of fracture, baseline bone densitometry may be prudent.12 A chart review study of nursing home residents found that 66% of men with hip fractures and 20% of men with vertebral fractures had low testosterone.13 Notably, 50% of men in their 80s have testosterone levels in the hypogonadal range (<300 ng/dL), compared with 12% of men <50 years.1,14

Recommendations

Scant guidance is available concerning what screening tests to order for a male with low testosterone. The United States Preventive Services Task Force and Canadian Task Force on Preventive Health Care make no recommendations; the Cochrane collaboration has no reviews on the topic. The American Association of Clinical Endocrinologists’ (AACE) guidelines are based on expert opinion.3

The AACE consensus guideline used peer review for validation and didn’t specify the method used to assess the quality and strength of the evidence used to write the statement. The AACE guideline recommends a history and physical exam, obtaining repeat morning testosterone levels, prolactin, FSH, LH, bone densitometry, and a semen analysis if fertility is an issue.

In acquired hypogonadism, pituitary imaging is recommended along with thyroid, adrenal, and growth hormone axis testing. Prepubertal males should undergo chromosome analysis, and men with a suspected mass should have a testicular ultrasound examination.

References

1. Darby E, Anawalt BD. Male hypogonadism: an update on diagnosis and treatment. Treat Endocrinol. 2005;4:293-309.

2. Badar F, Mirmira V, Hemady N. Hypogonadism in men: underdiagnosed and undertreated. Resid Staff Physician. 2006;52(6):6-12.

3. American Association of Clinical Endocrinologists American Association of Clinical Endocrinologists medical guidelines for clinical practice for the evaluation and treatment of hypogonadism in adult male patients—2002 update. Endocr Prac. 2002;8:440-456.

4. Smyth CM, Bremner WJ. Klinefelter syndrome. Arch Intern Med. 1998;158:1309-1314.

5. Spratt DI, O’Dea LS, Schoenfeld D, et al. Neuroendocrine-gonadal axis in men: frequent sampling of LH, FSH, and testosterone. Am J Physiol. 1988;254(5 Part 1):E658-E666.

6. Seftel AD. Male hypogonadism. Part I: epidemiology of hypogonadism. Int J Impot Res. 2006;18:115-120.

7. Sadovsky R, Dhindsa S, Margo K. Testosterone deficiency: which patients should you screen and treat? J Fam Pract. 2007;56(5 suppl):S1-S24.

8. Bhasin S, Jameson DL. Disorders of the testes and male reproductive system. Ch 340. In: Fauci AS, Braunwald E, Kasper DL, et al, eds. Harrison’s Principles of Internal Medicine. 17th ed. New York: McGraw-Hill; 2008.

9. US Census Bureau. US Interim projections by age, sex, race, and Hispanic origin: 2000-2050. Created March 18, 2004. Available at: www.census.gov/ipc/www/usinterimproj/. Accessed March 14, 2006.

10. Schrier SL, Bacon BR. Clinical manifestations of hereditary hemochromatosis. Up to Date [online database]. Version 15.1. Waltham, Mass: UpToDate; 2008.

11. Harman SM, Metter EJ, Tobin JD, et al. Longitudinal effects of aging on serum total and free testosterone levels in healthy men. Baltimore Longitudinal Study of Aging. J Clin Endocrinol Metab. 2001;86:724-731.

12. Kaufman JM, Johnell O, Abadie E, et al. Background for studies on the treatment of male osteoporosis: state of the art. Ann Rheum Dis. 2000;59:765-772.

13. Abbasi AA, Rudman D, Wilson CR, et al. Observations on nursing home residents with a history of hip fracture. Am J Med Sci. 1995;310:229-234.

14. Pietrangelo A. Hereditary hemochromatosis—a new look at an old disease. N Engl J Med. 2004;350:2383-2397.

References

1. Darby E, Anawalt BD. Male hypogonadism: an update on diagnosis and treatment. Treat Endocrinol. 2005;4:293-309.

2. Badar F, Mirmira V, Hemady N. Hypogonadism in men: underdiagnosed and undertreated. Resid Staff Physician. 2006;52(6):6-12.

3. American Association of Clinical Endocrinologists American Association of Clinical Endocrinologists medical guidelines for clinical practice for the evaluation and treatment of hypogonadism in adult male patients—2002 update. Endocr Prac. 2002;8:440-456.

4. Smyth CM, Bremner WJ. Klinefelter syndrome. Arch Intern Med. 1998;158:1309-1314.

5. Spratt DI, O’Dea LS, Schoenfeld D, et al. Neuroendocrine-gonadal axis in men: frequent sampling of LH, FSH, and testosterone. Am J Physiol. 1988;254(5 Part 1):E658-E666.

6. Seftel AD. Male hypogonadism. Part I: epidemiology of hypogonadism. Int J Impot Res. 2006;18:115-120.

7. Sadovsky R, Dhindsa S, Margo K. Testosterone deficiency: which patients should you screen and treat? J Fam Pract. 2007;56(5 suppl):S1-S24.

8. Bhasin S, Jameson DL. Disorders of the testes and male reproductive system. Ch 340. In: Fauci AS, Braunwald E, Kasper DL, et al, eds. Harrison’s Principles of Internal Medicine. 17th ed. New York: McGraw-Hill; 2008.

9. US Census Bureau. US Interim projections by age, sex, race, and Hispanic origin: 2000-2050. Created March 18, 2004. Available at: www.census.gov/ipc/www/usinterimproj/. Accessed March 14, 2006.

10. Schrier SL, Bacon BR. Clinical manifestations of hereditary hemochromatosis. Up to Date [online database]. Version 15.1. Waltham, Mass: UpToDate; 2008.

11. Harman SM, Metter EJ, Tobin JD, et al. Longitudinal effects of aging on serum total and free testosterone levels in healthy men. Baltimore Longitudinal Study of Aging. J Clin Endocrinol Metab. 2001;86:724-731.

12. Kaufman JM, Johnell O, Abadie E, et al. Background for studies on the treatment of male osteoporosis: state of the art. Ann Rheum Dis. 2000;59:765-772.

13. Abbasi AA, Rudman D, Wilson CR, et al. Observations on nursing home residents with a history of hip fracture. Am J Med Sci. 1995;310:229-234.

14. Pietrangelo A. Hereditary hemochromatosis—a new look at an old disease. N Engl J Med. 2004;350:2383-2397.

Issue
The Journal of Family Practice - 57(11)
Issue
The Journal of Family Practice - 57(11)
Page Number
756-758
Page Number
756-758
Publications
Publications
Topics
Article Type
Display Headline
What screening tests should you use to evaluate a man with low testosterone?
Display Headline
What screening tests should you use to evaluate a man with low testosterone?
Legacy Keywords
Robert P. Jackman; hypogonadism; follicle-stimulating hormone; luteinizing hormone; prolactin
Legacy Keywords
Robert P. Jackman; hypogonadism; follicle-stimulating hormone; luteinizing hormone; prolactin
Sections
PURLs Copyright

Evidence-based answers from the Family Physicians Inquiries Network

Disallow All Ads
Alternative CME
Article PDF Media