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What measures relieve postherpetic neuralgia?
Tricyclic antidepressants, gabapentin, and pregabalin effectively reduce pain (strength of recommendation [SOR]: A, at least 2 good-quality randomized controlled trials [RCTs] and/or meta-analyses). Opioids have demonstrated pain relief in 3 RCTs (SOR: A, consistent RCTs). Capsaicin and the lidocaine 5% patch relieve pain and decrease allodynia (SOR: B, recommendations from meta-analyses and lower-quality RCTs).
Evidence summary
Postherpetic neuralgia (PHN) is defined as pain lasting 1 to 3 months after resolution of acute herpes zoster (shingles) rash. It occurs in approximately 10% to 15% of patients and can cause significant morbidity.
Tricyclic antidepressants provide effective pain relief
Five systematic reviews have concluded that tricyclic antidepressants (TCAs) are effective treatments for PHN.1-5 Amitriptyline, the best studied TCA, provides at least moderate pain relief in two-thirds of patients with a pooled number needed to treat (NNT) for TCAs of 2.64 (95% confidence interval [CI], 2.1-3.54)5 (TABLE).
Selective serotonin reuptake inhibitors—including fluoxetine, paroxetine, citalopram, and sertraline—have been studied in a variety of neuropathic pain syndromes, but not for treating PHN.1
TABLE
What’s the NNT for drugs used to treat postherpetic neuralgia?
| CLASS | DRUG | DOSE | NNT | SIDE EFFECTS |
|---|---|---|---|---|
| Tricyclic antidepressants5 | Amitriptyline | Up to 150 mg/d (mean 120 mg/d) | 2.64 | Sedation, dry mouth, blurred vision, constipation, urinary retention |
| Nortriptyline | Up to 150 mg/d (mean 89 mg/d) | |||
| Desipramine | Up to 150 mg/d (mean 65-73 mg/d) | |||
| Anticonvulsants3,5 | Gabapentin | 1800-3600 mg/d | 2.8-5.3 | Somnolence, dizziness, edema, dry mouth |
| Pregabalin | 150-600 mg/d | 4.93 | ||
| Opioids5 | Oxycodone | Variable | 2.67 | Constipation, nausea, vomiting, sedation, dizziness, dependence |
| Long-acting morphine/methadone | 15-225 mg/d (morphine) (mean 91 mg/d for morphine, 15 mg/d for methadone) | 2.67 | ||
| Tramadol | 100-400 mg/d (mean 275 mg/d) | 4.76 | Dependence | |
| Topicals5 | Capsaicin 0.075% cream | Applied 3-4 times per day | 3.26 | Burning skin |
| Lidocaine 5% extended release patch | Max 3 patches per day | 2.0 | Mild skin reaction | |
| NNT, number needed to treat. | ||||
Anticonvulsants help, too
Five systematic reviews found gabapentin to be effective, with a range of NNT from 2.8 to 5.3 for as much as 50% pain reduction based on the visual analog score (VAS).2-6 Pregabalin is also effective, with an NNT of 4.93 (95% CI, 3.34-6.07) for up to 50% pain reduction.7,8 Limited data are available concerning the effectiveness of valproate.5
A look at the role of narcotics
Four systematic reviews found that controlled-release oxycodone reduced pain by 50%, based on the VAS.2-5 Another systematic review reported only limited evidence of effectiveness.6 In pooled results from systematic reviews, opioids decreased pain by 50% on the VAS (NNT=2.67; 95% CI, 2.10-3.77).6
An RCT of 76 patients demonstrated that morphine, with methadone as backup, both reduced the intensity of pain and relieved pain more than placebo.9
Tramadol, a selective opioid agonist, showed moderate effectiveness in a small RCT (N=125), with an NNT of 4.76 (95% CI, 2.61-26.97).3,5,6 The mean pain intensity, degree of pain relief, and amount of rescue medication required were all better in the tramadol group than the placebo group.
Evidence for topical therapy is limited
The anesthetic lidocaine patch 5% has shown efficacy in PHN with allodynia based on 3 RCTs of lower quality (short duration, recruitment of patients who had improved on lidocaine previously, no report of baseline levels of pain); the NNT was 2 (95% CI, 1.4-3.3).10 A systematic review of these 3 RCTs concluded that evidence is insufficient to recommend the lidocaine patch as treatment for PHN.10
Capsaicin, a topical counterirritant, reduced pain in fewer than 20% of patients in 2 RCTs reported in systematic reviews, with an NNT of 3.26 (95% CI, 2.26-5.85).2-6 Blinding was limited in these studies because of the stinging associated with treatment.
Recommendations
A 2004 practice parameter of the American Academy of Neurology recommends TCAs (amitriptyline, nortriptyline, desipramine, and maprotiline), gabapentin, pregabalin, opioids, topical lidocaine, and capsaicin to treat PHN (level of evidence: A), but notes that amitriptyline has significant cardiac effects in the elderly compared with nortriptyline and desipramine.3
In 2006, the European Federation of Neurological Societies determined that TCAs, gabapentin, pregabalin, and opioids had established efficacy (level of evidence: A), but recommended opioids as second-line therapy because of potential adverse events with long-term use.4 The federation’s guidelines designate capsaicin, tramadol, topical lidocaine, and valproate as drugs with lower efficacy or limited strength of evidence (level of evidence: B). Nevertheless, they recommend considering topical lidocaine for elderly patients with allodynia and small areas of pain.4
1. saarto T, Wiffen PJ. Antidepressants for neuropathic pain. Cochrane Database Syst Rev. 2007;(4):CD005454.-
2. Alper BS, Lewis PR. Treatment of postherpetic neuralgia: a systematic review of the literature. J Fam Pract. 2002;51:121-128.
3. Dubinsky RM, Kabbani H, El-Chami Z, et al. Practice parameter: treatment of postherpetic neuralgia: an evidence-based report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology. 2004;63:959-965.
4. Attal N, Cruccu G, Haanpaa M, et al. EFNS guidelines on pharmacological treatment of neuropathic pain. Eur J Neurol. 2006;13:1153-1169.
5. Hempenstall K, Nurmikko TJ, Johnson RW, et al. Analgesic therapy in postherpetic neuralgia: a quantitative systematic review. PLoS Med. 2005;2:e164.-
6. Wareham DW. Postherpetic neuralgia. BMJ Clin Evid. 2007;12:905-918.
7. van Seventer R, Feister HA, Young JP, et al. efficacy and tolerability of twice-daily pregabalin for treating pain and related sleep interference in postherpetic neuralgia: a 13-week, randomized trial. Curr Med Res Opin. 2006;22:375-384.
8. Dworkin RH, Corbin AE, Young JP, Jr, et al. Pregabalin for the treatment of postherpetic neuralgia; a randomized, placebo-controlled trial. Neurology. 2003;60:1274-1283.
9. Raja SN, Haythornwaite JA, Pappagallo M, et al. Opioids versus antidepressants in postherpetic neuralgia: a randomized, placebo-controlled trial. Neurology. 2002;59:1015-1021.
10. Khaliq W, Alam S, Puri N. Topical lidocaine for the treatment of postherpetic neuralgia. Cochrane Database Syst Rev. 2007;(2):CD004846.-
Tricyclic antidepressants, gabapentin, and pregabalin effectively reduce pain (strength of recommendation [SOR]: A, at least 2 good-quality randomized controlled trials [RCTs] and/or meta-analyses). Opioids have demonstrated pain relief in 3 RCTs (SOR: A, consistent RCTs). Capsaicin and the lidocaine 5% patch relieve pain and decrease allodynia (SOR: B, recommendations from meta-analyses and lower-quality RCTs).
Evidence summary
Postherpetic neuralgia (PHN) is defined as pain lasting 1 to 3 months after resolution of acute herpes zoster (shingles) rash. It occurs in approximately 10% to 15% of patients and can cause significant morbidity.
Tricyclic antidepressants provide effective pain relief
Five systematic reviews have concluded that tricyclic antidepressants (TCAs) are effective treatments for PHN.1-5 Amitriptyline, the best studied TCA, provides at least moderate pain relief in two-thirds of patients with a pooled number needed to treat (NNT) for TCAs of 2.64 (95% confidence interval [CI], 2.1-3.54)5 (TABLE).
Selective serotonin reuptake inhibitors—including fluoxetine, paroxetine, citalopram, and sertraline—have been studied in a variety of neuropathic pain syndromes, but not for treating PHN.1
TABLE
What’s the NNT for drugs used to treat postherpetic neuralgia?
| CLASS | DRUG | DOSE | NNT | SIDE EFFECTS |
|---|---|---|---|---|
| Tricyclic antidepressants5 | Amitriptyline | Up to 150 mg/d (mean 120 mg/d) | 2.64 | Sedation, dry mouth, blurred vision, constipation, urinary retention |
| Nortriptyline | Up to 150 mg/d (mean 89 mg/d) | |||
| Desipramine | Up to 150 mg/d (mean 65-73 mg/d) | |||
| Anticonvulsants3,5 | Gabapentin | 1800-3600 mg/d | 2.8-5.3 | Somnolence, dizziness, edema, dry mouth |
| Pregabalin | 150-600 mg/d | 4.93 | ||
| Opioids5 | Oxycodone | Variable | 2.67 | Constipation, nausea, vomiting, sedation, dizziness, dependence |
| Long-acting morphine/methadone | 15-225 mg/d (morphine) (mean 91 mg/d for morphine, 15 mg/d for methadone) | 2.67 | ||
| Tramadol | 100-400 mg/d (mean 275 mg/d) | 4.76 | Dependence | |
| Topicals5 | Capsaicin 0.075% cream | Applied 3-4 times per day | 3.26 | Burning skin |
| Lidocaine 5% extended release patch | Max 3 patches per day | 2.0 | Mild skin reaction | |
| NNT, number needed to treat. | ||||
Anticonvulsants help, too
Five systematic reviews found gabapentin to be effective, with a range of NNT from 2.8 to 5.3 for as much as 50% pain reduction based on the visual analog score (VAS).2-6 Pregabalin is also effective, with an NNT of 4.93 (95% CI, 3.34-6.07) for up to 50% pain reduction.7,8 Limited data are available concerning the effectiveness of valproate.5
A look at the role of narcotics
Four systematic reviews found that controlled-release oxycodone reduced pain by 50%, based on the VAS.2-5 Another systematic review reported only limited evidence of effectiveness.6 In pooled results from systematic reviews, opioids decreased pain by 50% on the VAS (NNT=2.67; 95% CI, 2.10-3.77).6
An RCT of 76 patients demonstrated that morphine, with methadone as backup, both reduced the intensity of pain and relieved pain more than placebo.9
Tramadol, a selective opioid agonist, showed moderate effectiveness in a small RCT (N=125), with an NNT of 4.76 (95% CI, 2.61-26.97).3,5,6 The mean pain intensity, degree of pain relief, and amount of rescue medication required were all better in the tramadol group than the placebo group.
Evidence for topical therapy is limited
The anesthetic lidocaine patch 5% has shown efficacy in PHN with allodynia based on 3 RCTs of lower quality (short duration, recruitment of patients who had improved on lidocaine previously, no report of baseline levels of pain); the NNT was 2 (95% CI, 1.4-3.3).10 A systematic review of these 3 RCTs concluded that evidence is insufficient to recommend the lidocaine patch as treatment for PHN.10
Capsaicin, a topical counterirritant, reduced pain in fewer than 20% of patients in 2 RCTs reported in systematic reviews, with an NNT of 3.26 (95% CI, 2.26-5.85).2-6 Blinding was limited in these studies because of the stinging associated with treatment.
Recommendations
A 2004 practice parameter of the American Academy of Neurology recommends TCAs (amitriptyline, nortriptyline, desipramine, and maprotiline), gabapentin, pregabalin, opioids, topical lidocaine, and capsaicin to treat PHN (level of evidence: A), but notes that amitriptyline has significant cardiac effects in the elderly compared with nortriptyline and desipramine.3
In 2006, the European Federation of Neurological Societies determined that TCAs, gabapentin, pregabalin, and opioids had established efficacy (level of evidence: A), but recommended opioids as second-line therapy because of potential adverse events with long-term use.4 The federation’s guidelines designate capsaicin, tramadol, topical lidocaine, and valproate as drugs with lower efficacy or limited strength of evidence (level of evidence: B). Nevertheless, they recommend considering topical lidocaine for elderly patients with allodynia and small areas of pain.4
Tricyclic antidepressants, gabapentin, and pregabalin effectively reduce pain (strength of recommendation [SOR]: A, at least 2 good-quality randomized controlled trials [RCTs] and/or meta-analyses). Opioids have demonstrated pain relief in 3 RCTs (SOR: A, consistent RCTs). Capsaicin and the lidocaine 5% patch relieve pain and decrease allodynia (SOR: B, recommendations from meta-analyses and lower-quality RCTs).
Evidence summary
Postherpetic neuralgia (PHN) is defined as pain lasting 1 to 3 months after resolution of acute herpes zoster (shingles) rash. It occurs in approximately 10% to 15% of patients and can cause significant morbidity.
Tricyclic antidepressants provide effective pain relief
Five systematic reviews have concluded that tricyclic antidepressants (TCAs) are effective treatments for PHN.1-5 Amitriptyline, the best studied TCA, provides at least moderate pain relief in two-thirds of patients with a pooled number needed to treat (NNT) for TCAs of 2.64 (95% confidence interval [CI], 2.1-3.54)5 (TABLE).
Selective serotonin reuptake inhibitors—including fluoxetine, paroxetine, citalopram, and sertraline—have been studied in a variety of neuropathic pain syndromes, but not for treating PHN.1
TABLE
What’s the NNT for drugs used to treat postherpetic neuralgia?
| CLASS | DRUG | DOSE | NNT | SIDE EFFECTS |
|---|---|---|---|---|
| Tricyclic antidepressants5 | Amitriptyline | Up to 150 mg/d (mean 120 mg/d) | 2.64 | Sedation, dry mouth, blurred vision, constipation, urinary retention |
| Nortriptyline | Up to 150 mg/d (mean 89 mg/d) | |||
| Desipramine | Up to 150 mg/d (mean 65-73 mg/d) | |||
| Anticonvulsants3,5 | Gabapentin | 1800-3600 mg/d | 2.8-5.3 | Somnolence, dizziness, edema, dry mouth |
| Pregabalin | 150-600 mg/d | 4.93 | ||
| Opioids5 | Oxycodone | Variable | 2.67 | Constipation, nausea, vomiting, sedation, dizziness, dependence |
| Long-acting morphine/methadone | 15-225 mg/d (morphine) (mean 91 mg/d for morphine, 15 mg/d for methadone) | 2.67 | ||
| Tramadol | 100-400 mg/d (mean 275 mg/d) | 4.76 | Dependence | |
| Topicals5 | Capsaicin 0.075% cream | Applied 3-4 times per day | 3.26 | Burning skin |
| Lidocaine 5% extended release patch | Max 3 patches per day | 2.0 | Mild skin reaction | |
| NNT, number needed to treat. | ||||
Anticonvulsants help, too
Five systematic reviews found gabapentin to be effective, with a range of NNT from 2.8 to 5.3 for as much as 50% pain reduction based on the visual analog score (VAS).2-6 Pregabalin is also effective, with an NNT of 4.93 (95% CI, 3.34-6.07) for up to 50% pain reduction.7,8 Limited data are available concerning the effectiveness of valproate.5
A look at the role of narcotics
Four systematic reviews found that controlled-release oxycodone reduced pain by 50%, based on the VAS.2-5 Another systematic review reported only limited evidence of effectiveness.6 In pooled results from systematic reviews, opioids decreased pain by 50% on the VAS (NNT=2.67; 95% CI, 2.10-3.77).6
An RCT of 76 patients demonstrated that morphine, with methadone as backup, both reduced the intensity of pain and relieved pain more than placebo.9
Tramadol, a selective opioid agonist, showed moderate effectiveness in a small RCT (N=125), with an NNT of 4.76 (95% CI, 2.61-26.97).3,5,6 The mean pain intensity, degree of pain relief, and amount of rescue medication required were all better in the tramadol group than the placebo group.
Evidence for topical therapy is limited
The anesthetic lidocaine patch 5% has shown efficacy in PHN with allodynia based on 3 RCTs of lower quality (short duration, recruitment of patients who had improved on lidocaine previously, no report of baseline levels of pain); the NNT was 2 (95% CI, 1.4-3.3).10 A systematic review of these 3 RCTs concluded that evidence is insufficient to recommend the lidocaine patch as treatment for PHN.10
Capsaicin, a topical counterirritant, reduced pain in fewer than 20% of patients in 2 RCTs reported in systematic reviews, with an NNT of 3.26 (95% CI, 2.26-5.85).2-6 Blinding was limited in these studies because of the stinging associated with treatment.
Recommendations
A 2004 practice parameter of the American Academy of Neurology recommends TCAs (amitriptyline, nortriptyline, desipramine, and maprotiline), gabapentin, pregabalin, opioids, topical lidocaine, and capsaicin to treat PHN (level of evidence: A), but notes that amitriptyline has significant cardiac effects in the elderly compared with nortriptyline and desipramine.3
In 2006, the European Federation of Neurological Societies determined that TCAs, gabapentin, pregabalin, and opioids had established efficacy (level of evidence: A), but recommended opioids as second-line therapy because of potential adverse events with long-term use.4 The federation’s guidelines designate capsaicin, tramadol, topical lidocaine, and valproate as drugs with lower efficacy or limited strength of evidence (level of evidence: B). Nevertheless, they recommend considering topical lidocaine for elderly patients with allodynia and small areas of pain.4
1. saarto T, Wiffen PJ. Antidepressants for neuropathic pain. Cochrane Database Syst Rev. 2007;(4):CD005454.-
2. Alper BS, Lewis PR. Treatment of postherpetic neuralgia: a systematic review of the literature. J Fam Pract. 2002;51:121-128.
3. Dubinsky RM, Kabbani H, El-Chami Z, et al. Practice parameter: treatment of postherpetic neuralgia: an evidence-based report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology. 2004;63:959-965.
4. Attal N, Cruccu G, Haanpaa M, et al. EFNS guidelines on pharmacological treatment of neuropathic pain. Eur J Neurol. 2006;13:1153-1169.
5. Hempenstall K, Nurmikko TJ, Johnson RW, et al. Analgesic therapy in postherpetic neuralgia: a quantitative systematic review. PLoS Med. 2005;2:e164.-
6. Wareham DW. Postherpetic neuralgia. BMJ Clin Evid. 2007;12:905-918.
7. van Seventer R, Feister HA, Young JP, et al. efficacy and tolerability of twice-daily pregabalin for treating pain and related sleep interference in postherpetic neuralgia: a 13-week, randomized trial. Curr Med Res Opin. 2006;22:375-384.
8. Dworkin RH, Corbin AE, Young JP, Jr, et al. Pregabalin for the treatment of postherpetic neuralgia; a randomized, placebo-controlled trial. Neurology. 2003;60:1274-1283.
9. Raja SN, Haythornwaite JA, Pappagallo M, et al. Opioids versus antidepressants in postherpetic neuralgia: a randomized, placebo-controlled trial. Neurology. 2002;59:1015-1021.
10. Khaliq W, Alam S, Puri N. Topical lidocaine for the treatment of postherpetic neuralgia. Cochrane Database Syst Rev. 2007;(2):CD004846.-
1. saarto T, Wiffen PJ. Antidepressants for neuropathic pain. Cochrane Database Syst Rev. 2007;(4):CD005454.-
2. Alper BS, Lewis PR. Treatment of postherpetic neuralgia: a systematic review of the literature. J Fam Pract. 2002;51:121-128.
3. Dubinsky RM, Kabbani H, El-Chami Z, et al. Practice parameter: treatment of postherpetic neuralgia: an evidence-based report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology. 2004;63:959-965.
4. Attal N, Cruccu G, Haanpaa M, et al. EFNS guidelines on pharmacological treatment of neuropathic pain. Eur J Neurol. 2006;13:1153-1169.
5. Hempenstall K, Nurmikko TJ, Johnson RW, et al. Analgesic therapy in postherpetic neuralgia: a quantitative systematic review. PLoS Med. 2005;2:e164.-
6. Wareham DW. Postherpetic neuralgia. BMJ Clin Evid. 2007;12:905-918.
7. van Seventer R, Feister HA, Young JP, et al. efficacy and tolerability of twice-daily pregabalin for treating pain and related sleep interference in postherpetic neuralgia: a 13-week, randomized trial. Curr Med Res Opin. 2006;22:375-384.
8. Dworkin RH, Corbin AE, Young JP, Jr, et al. Pregabalin for the treatment of postherpetic neuralgia; a randomized, placebo-controlled trial. Neurology. 2003;60:1274-1283.
9. Raja SN, Haythornwaite JA, Pappagallo M, et al. Opioids versus antidepressants in postherpetic neuralgia: a randomized, placebo-controlled trial. Neurology. 2002;59:1015-1021.
10. Khaliq W, Alam S, Puri N. Topical lidocaine for the treatment of postherpetic neuralgia. Cochrane Database Syst Rev. 2007;(2):CD004846.-
Evidence-based answers from the Family Physicians Inquiries Network
What is the best workup for hypocalcemia?
Unexplained hypocalcemia can usually be diagnosed by a limited number of serum tests when the cause isn’t obvious from the history (recent neck surgery or renal failure):
- calcium (corrected for serum albumin)
- creatinine
- phosphorus
- magnesium
- parathyroid hormone (PTH).
The most common causes, categorized according to the results of these tests, are (strength of recommendation: C, expert opinion, case series, and physiologic principles):
- high PTH, high phosphorus, and high creatinine: renal failure
- high PTH, low or normal phosphorus, and normal creatinine: vitamin D deficiency or pancreatitis
- low PTH, high phosphorus, and normal creatinine: inadequate parathyroid gland function or hypomagnesemia.
Important supporting tests—serum albumin, phosphorus, magnesium
Grant Hoekzema, MD
Mercy Family Medicine Residency, St. Louis, Mo
Serious abnormal laboratory results often are encountered in outpatient testing using multitest panels such as basic and comprehensive metabolic profiles. Hypocalcemia found on a basic metabolic panel is a good example of such a result.
Given the broad differential diagnosis outlined by the authors of this Clinical Inquiry, we must interpret abnormal results with the proper supporting tests. In this case, the most important is serum albumin, which can be a critical indicator of whether the patient truly has hypocalcemia. That is why I tend to order a comprehensive metabolic panel when disorders of calcium metabolism are part of the differential.
This Clinical Inquiry also highlights the important role of phosphorus and magnesium in calcium metabolism. It’s important to note that these tests are no longer a regular component of many multitest blood panels and must be ordered when hypocalcemia is found.
Evidence summary
Normal values for total or corrected serum calcium are 8.5-10.2 mg/dL and for ionized calcium, 4.4-5.4 mg/dL. Because total serum calcium is approximately 50% free (ionized) and 50% bound, primarily to albumin, the serum level must be “corrected” if hypoalbuminemia exists. Because serum calcium comprises less than 1% of body stores, severe total body deficiency of calcium can exist without hypocalcemia.1,2
Ionized calcium is under tight physiologic control, monitored by calcium-sensing proteins in the parathyroid gland; low ionized calcium augments PTH secretion, which in turn has 3 primary actions:
- decreased calcium excretion by the kidneys
- increased activity of osteoclasts, leading to calcium release from bone
- increased activity of renal 25-OH vitamin D hydroxylase, resulting in elevated serum levels of calcitriol, the active form of vitamin D; elevated calcitriol in turn augments gastrointestinal absorption of calcium.
An adequate supply of 25-OH vitamin D to the kidneys requires adequate gastrointestinal absorption or sun-induced skin production of vitamin D and sufficient liver function to carry out the first of the 2 hydroxylation steps.1,3
Common causes of hypocalcemia
We found no studies that established the frequency of various causes of hypocalcemia in the general population, but reviewers concurred that the most common specific causes, in order of frequency, are (TABLE):2,3
- renal failure
- vitamin D deficiency
- hypomagnesemia
- pancreatitis
- hypoparathyroidism.
It is not surprising that renal failure is a common cause of hypocalcemia, given the high prevalence of chronic kidney disease in adults—11.2% of the total United States population older than 20 years has at least a mildly reduced glomerular filtration rate (stage 2, chronic kidney disease, with glomerular filtration rate <90 cc/min).4 Despite elevated PTH, serum calcium may be slightly reduced (and osteomalacia present) even in mild chronic kidney disease.5,6 Only severe or end-stage chronic kidney disease (glomerular filtration rate <30 cc/min, 5.8% of population) is often associated with actual hypocalcemia.5,6 Likewise, the prevalence of vitamin D deficiency (<15 ng/mL of 25-OH vitamin D) is 35% to 55% in the general population,7,8 and 95% in institutionalized elderly patients.9
Chronic kidney disease (66%) and vitamin D deficiency (24%) were the most common causes of hypocalcemia in a study of 594 elderly general medicine inpatients.10 In a study of 62 hypocalcemic patients in a medical intensive care unit, the cause of the hypocalcemia could be determined in only 28 (45%); most of the cases were caused by hypomagnesemia (28%), renal insufficiency (8%), and pancreatitis (3%).11
TABLE
Causes of hypocalcemia by key test results
| TEST RESULTS | COMMON CAUSES | LESS COMMON CAUSES |
|---|---|---|
| High PTH, high phosphorus | Renal failure |
|
| High PTH, low phosphorus | Vitamin D deficiency (with low bone calcium) caused by:
|
|
| Low PTH, high phosphorus | Hypoparathyroidism and hypomagnesemia |
|
| PTH, parathyroid hormone. | ||
Serious causes of hypocalcemia
The usual cause of critically low serum calcium (<7 mg/dL “corrected” or <3.2 mg/dL ionized) is parathyroidectomy or acute renal failure. Hypocalcemia resulting from partial parathyroidectomy or thyroidectomy (with inadvertent parathyroidectomy) occurs in approximately 5% of these surgeries; 99.5% of cases resolve completely within a year.12
Recommendations
Several reviewers recommend a similar workup and differential diagnosis for hypocalcemia. Unfortunately, none cites quantitative data on the prevalence of hypocalcemia and its causes.2,13
Some authors recommend measuring 25-OH vitamin D in all hypocalcemia patients with elevated PTH without hyperphosphatemia to confirm vitamin D deficiency.1,2 Others emphasize the importance of measuring ionized calcium to detect hypocalcemia, especially in critically ill patients, in whom many acute variables can decrease ionized calcium (alkalosis can increase protein binding, for example).1,3,14
Although several reviewers present an algorithmic approach to determining the cause of hypocalcemia,3 we could find no data on the derivation or validation of the diagnostic effectiveness of these algorithms.
1. Fukugawa M, Kurokawa K. Calcium homeostasis and imbalance. Nephron. 2002;92(suppl 1):41-45.
2. Ruppe M. Hypocalcemia. In: American College of Physicians (ACP) Physician’s Information and Education Resource (PIER) database. Available at: http://pier.acponline.org/index.html. Accessed October 30, 2007.
3. Carlstedt F, Lind L. Hypocalcemic syndromes. Crit Care Clin. 2001;17:139, 53, vii-viii.
4. Centers for Disease Control and Prevention (CDC). Prevalence of chronic kidney disease and associated risk factors—United States, 1999-2004. MMWR Morb Mortal Wkly Rep. 2007;56:161-165.
5. National Kidney Foundation. K/DOQI clinical practice guidelines for bone metabolism and disease in chronic kidney disease. Am J Kidney Dis. 2003;42(4 suppl 3):S1-S201.
6. Rix M, Andreassen H, Eskildsen P, Langdahl B, Olgaard K. Bone mineral density and biochemical markers of bone turnover in patients with predialysis chronic renal failure. Kidney Int. 1999;56:1084-1093.
7. Thomas MK, Lloyd-Jones DM, Thadhani RI, et al. Hypovitaminosis D in medical inpatients. N Engl J Med. 1998;338:777-783.
8. Tangpricha V, Pearce EN, Chen TC, Holick MF. Vitamin D insufficiency among free-living healthy young adults. Am J Med. 2002;112:659-662.
9. Fardellone P, Sebert JL, Garabedian M, et al. Prevalence and biological consequences of vitamin D deficiency in elderly institutionalized subjects. Rev Rhum Engl Ed. 1995;62:576-581.
10. Hodkinson HM. Serum calcium in a geriatric inpatient population. Age Ageing. 1973;2:157-162.
11. Desai TK, Carlson RW, Geheb MA. Prevalence and clinical implications of hypocalcemia in acutely ill patients in a medical intensive care setting. Am J Med. 1988;84:209-214.
12. Pattou F, Combemale F, Fabre S, et al. Hypocalcemia following thyroid surgery: incidence and prediction of outcome. World J Surg. 1998;22:718-724.
13. Guise TA, Mundy GR. Clinical review 69: evaluation of hypocalcemia in children and adults. J Clin Endocrinol Metab. 1995;80:1473-1478.
14. Hastbacka J, Pettila V. Prevalence and predictive value of ionized hypocalcemia among critically ill patients. Acta Anaesthesiol Scand. 2003;47:1264-1269.
Unexplained hypocalcemia can usually be diagnosed by a limited number of serum tests when the cause isn’t obvious from the history (recent neck surgery or renal failure):
- calcium (corrected for serum albumin)
- creatinine
- phosphorus
- magnesium
- parathyroid hormone (PTH).
The most common causes, categorized according to the results of these tests, are (strength of recommendation: C, expert opinion, case series, and physiologic principles):
- high PTH, high phosphorus, and high creatinine: renal failure
- high PTH, low or normal phosphorus, and normal creatinine: vitamin D deficiency or pancreatitis
- low PTH, high phosphorus, and normal creatinine: inadequate parathyroid gland function or hypomagnesemia.
Important supporting tests—serum albumin, phosphorus, magnesium
Grant Hoekzema, MD
Mercy Family Medicine Residency, St. Louis, Mo
Serious abnormal laboratory results often are encountered in outpatient testing using multitest panels such as basic and comprehensive metabolic profiles. Hypocalcemia found on a basic metabolic panel is a good example of such a result.
Given the broad differential diagnosis outlined by the authors of this Clinical Inquiry, we must interpret abnormal results with the proper supporting tests. In this case, the most important is serum albumin, which can be a critical indicator of whether the patient truly has hypocalcemia. That is why I tend to order a comprehensive metabolic panel when disorders of calcium metabolism are part of the differential.
This Clinical Inquiry also highlights the important role of phosphorus and magnesium in calcium metabolism. It’s important to note that these tests are no longer a regular component of many multitest blood panels and must be ordered when hypocalcemia is found.
Evidence summary
Normal values for total or corrected serum calcium are 8.5-10.2 mg/dL and for ionized calcium, 4.4-5.4 mg/dL. Because total serum calcium is approximately 50% free (ionized) and 50% bound, primarily to albumin, the serum level must be “corrected” if hypoalbuminemia exists. Because serum calcium comprises less than 1% of body stores, severe total body deficiency of calcium can exist without hypocalcemia.1,2
Ionized calcium is under tight physiologic control, monitored by calcium-sensing proteins in the parathyroid gland; low ionized calcium augments PTH secretion, which in turn has 3 primary actions:
- decreased calcium excretion by the kidneys
- increased activity of osteoclasts, leading to calcium release from bone
- increased activity of renal 25-OH vitamin D hydroxylase, resulting in elevated serum levels of calcitriol, the active form of vitamin D; elevated calcitriol in turn augments gastrointestinal absorption of calcium.
An adequate supply of 25-OH vitamin D to the kidneys requires adequate gastrointestinal absorption or sun-induced skin production of vitamin D and sufficient liver function to carry out the first of the 2 hydroxylation steps.1,3
Common causes of hypocalcemia
We found no studies that established the frequency of various causes of hypocalcemia in the general population, but reviewers concurred that the most common specific causes, in order of frequency, are (TABLE):2,3
- renal failure
- vitamin D deficiency
- hypomagnesemia
- pancreatitis
- hypoparathyroidism.
It is not surprising that renal failure is a common cause of hypocalcemia, given the high prevalence of chronic kidney disease in adults—11.2% of the total United States population older than 20 years has at least a mildly reduced glomerular filtration rate (stage 2, chronic kidney disease, with glomerular filtration rate <90 cc/min).4 Despite elevated PTH, serum calcium may be slightly reduced (and osteomalacia present) even in mild chronic kidney disease.5,6 Only severe or end-stage chronic kidney disease (glomerular filtration rate <30 cc/min, 5.8% of population) is often associated with actual hypocalcemia.5,6 Likewise, the prevalence of vitamin D deficiency (<15 ng/mL of 25-OH vitamin D) is 35% to 55% in the general population,7,8 and 95% in institutionalized elderly patients.9
Chronic kidney disease (66%) and vitamin D deficiency (24%) were the most common causes of hypocalcemia in a study of 594 elderly general medicine inpatients.10 In a study of 62 hypocalcemic patients in a medical intensive care unit, the cause of the hypocalcemia could be determined in only 28 (45%); most of the cases were caused by hypomagnesemia (28%), renal insufficiency (8%), and pancreatitis (3%).11
TABLE
Causes of hypocalcemia by key test results
| TEST RESULTS | COMMON CAUSES | LESS COMMON CAUSES |
|---|---|---|
| High PTH, high phosphorus | Renal failure |
|
| High PTH, low phosphorus | Vitamin D deficiency (with low bone calcium) caused by:
|
|
| Low PTH, high phosphorus | Hypoparathyroidism and hypomagnesemia |
|
| PTH, parathyroid hormone. | ||
Serious causes of hypocalcemia
The usual cause of critically low serum calcium (<7 mg/dL “corrected” or <3.2 mg/dL ionized) is parathyroidectomy or acute renal failure. Hypocalcemia resulting from partial parathyroidectomy or thyroidectomy (with inadvertent parathyroidectomy) occurs in approximately 5% of these surgeries; 99.5% of cases resolve completely within a year.12
Recommendations
Several reviewers recommend a similar workup and differential diagnosis for hypocalcemia. Unfortunately, none cites quantitative data on the prevalence of hypocalcemia and its causes.2,13
Some authors recommend measuring 25-OH vitamin D in all hypocalcemia patients with elevated PTH without hyperphosphatemia to confirm vitamin D deficiency.1,2 Others emphasize the importance of measuring ionized calcium to detect hypocalcemia, especially in critically ill patients, in whom many acute variables can decrease ionized calcium (alkalosis can increase protein binding, for example).1,3,14
Although several reviewers present an algorithmic approach to determining the cause of hypocalcemia,3 we could find no data on the derivation or validation of the diagnostic effectiveness of these algorithms.
Unexplained hypocalcemia can usually be diagnosed by a limited number of serum tests when the cause isn’t obvious from the history (recent neck surgery or renal failure):
- calcium (corrected for serum albumin)
- creatinine
- phosphorus
- magnesium
- parathyroid hormone (PTH).
The most common causes, categorized according to the results of these tests, are (strength of recommendation: C, expert opinion, case series, and physiologic principles):
- high PTH, high phosphorus, and high creatinine: renal failure
- high PTH, low or normal phosphorus, and normal creatinine: vitamin D deficiency or pancreatitis
- low PTH, high phosphorus, and normal creatinine: inadequate parathyroid gland function or hypomagnesemia.
Important supporting tests—serum albumin, phosphorus, magnesium
Grant Hoekzema, MD
Mercy Family Medicine Residency, St. Louis, Mo
Serious abnormal laboratory results often are encountered in outpatient testing using multitest panels such as basic and comprehensive metabolic profiles. Hypocalcemia found on a basic metabolic panel is a good example of such a result.
Given the broad differential diagnosis outlined by the authors of this Clinical Inquiry, we must interpret abnormal results with the proper supporting tests. In this case, the most important is serum albumin, which can be a critical indicator of whether the patient truly has hypocalcemia. That is why I tend to order a comprehensive metabolic panel when disorders of calcium metabolism are part of the differential.
This Clinical Inquiry also highlights the important role of phosphorus and magnesium in calcium metabolism. It’s important to note that these tests are no longer a regular component of many multitest blood panels and must be ordered when hypocalcemia is found.
Evidence summary
Normal values for total or corrected serum calcium are 8.5-10.2 mg/dL and for ionized calcium, 4.4-5.4 mg/dL. Because total serum calcium is approximately 50% free (ionized) and 50% bound, primarily to albumin, the serum level must be “corrected” if hypoalbuminemia exists. Because serum calcium comprises less than 1% of body stores, severe total body deficiency of calcium can exist without hypocalcemia.1,2
Ionized calcium is under tight physiologic control, monitored by calcium-sensing proteins in the parathyroid gland; low ionized calcium augments PTH secretion, which in turn has 3 primary actions:
- decreased calcium excretion by the kidneys
- increased activity of osteoclasts, leading to calcium release from bone
- increased activity of renal 25-OH vitamin D hydroxylase, resulting in elevated serum levels of calcitriol, the active form of vitamin D; elevated calcitriol in turn augments gastrointestinal absorption of calcium.
An adequate supply of 25-OH vitamin D to the kidneys requires adequate gastrointestinal absorption or sun-induced skin production of vitamin D and sufficient liver function to carry out the first of the 2 hydroxylation steps.1,3
Common causes of hypocalcemia
We found no studies that established the frequency of various causes of hypocalcemia in the general population, but reviewers concurred that the most common specific causes, in order of frequency, are (TABLE):2,3
- renal failure
- vitamin D deficiency
- hypomagnesemia
- pancreatitis
- hypoparathyroidism.
It is not surprising that renal failure is a common cause of hypocalcemia, given the high prevalence of chronic kidney disease in adults—11.2% of the total United States population older than 20 years has at least a mildly reduced glomerular filtration rate (stage 2, chronic kidney disease, with glomerular filtration rate <90 cc/min).4 Despite elevated PTH, serum calcium may be slightly reduced (and osteomalacia present) even in mild chronic kidney disease.5,6 Only severe or end-stage chronic kidney disease (glomerular filtration rate <30 cc/min, 5.8% of population) is often associated with actual hypocalcemia.5,6 Likewise, the prevalence of vitamin D deficiency (<15 ng/mL of 25-OH vitamin D) is 35% to 55% in the general population,7,8 and 95% in institutionalized elderly patients.9
Chronic kidney disease (66%) and vitamin D deficiency (24%) were the most common causes of hypocalcemia in a study of 594 elderly general medicine inpatients.10 In a study of 62 hypocalcemic patients in a medical intensive care unit, the cause of the hypocalcemia could be determined in only 28 (45%); most of the cases were caused by hypomagnesemia (28%), renal insufficiency (8%), and pancreatitis (3%).11
TABLE
Causes of hypocalcemia by key test results
| TEST RESULTS | COMMON CAUSES | LESS COMMON CAUSES |
|---|---|---|
| High PTH, high phosphorus | Renal failure |
|
| High PTH, low phosphorus | Vitamin D deficiency (with low bone calcium) caused by:
|
|
| Low PTH, high phosphorus | Hypoparathyroidism and hypomagnesemia |
|
| PTH, parathyroid hormone. | ||
Serious causes of hypocalcemia
The usual cause of critically low serum calcium (<7 mg/dL “corrected” or <3.2 mg/dL ionized) is parathyroidectomy or acute renal failure. Hypocalcemia resulting from partial parathyroidectomy or thyroidectomy (with inadvertent parathyroidectomy) occurs in approximately 5% of these surgeries; 99.5% of cases resolve completely within a year.12
Recommendations
Several reviewers recommend a similar workup and differential diagnosis for hypocalcemia. Unfortunately, none cites quantitative data on the prevalence of hypocalcemia and its causes.2,13
Some authors recommend measuring 25-OH vitamin D in all hypocalcemia patients with elevated PTH without hyperphosphatemia to confirm vitamin D deficiency.1,2 Others emphasize the importance of measuring ionized calcium to detect hypocalcemia, especially in critically ill patients, in whom many acute variables can decrease ionized calcium (alkalosis can increase protein binding, for example).1,3,14
Although several reviewers present an algorithmic approach to determining the cause of hypocalcemia,3 we could find no data on the derivation or validation of the diagnostic effectiveness of these algorithms.
1. Fukugawa M, Kurokawa K. Calcium homeostasis and imbalance. Nephron. 2002;92(suppl 1):41-45.
2. Ruppe M. Hypocalcemia. In: American College of Physicians (ACP) Physician’s Information and Education Resource (PIER) database. Available at: http://pier.acponline.org/index.html. Accessed October 30, 2007.
3. Carlstedt F, Lind L. Hypocalcemic syndromes. Crit Care Clin. 2001;17:139, 53, vii-viii.
4. Centers for Disease Control and Prevention (CDC). Prevalence of chronic kidney disease and associated risk factors—United States, 1999-2004. MMWR Morb Mortal Wkly Rep. 2007;56:161-165.
5. National Kidney Foundation. K/DOQI clinical practice guidelines for bone metabolism and disease in chronic kidney disease. Am J Kidney Dis. 2003;42(4 suppl 3):S1-S201.
6. Rix M, Andreassen H, Eskildsen P, Langdahl B, Olgaard K. Bone mineral density and biochemical markers of bone turnover in patients with predialysis chronic renal failure. Kidney Int. 1999;56:1084-1093.
7. Thomas MK, Lloyd-Jones DM, Thadhani RI, et al. Hypovitaminosis D in medical inpatients. N Engl J Med. 1998;338:777-783.
8. Tangpricha V, Pearce EN, Chen TC, Holick MF. Vitamin D insufficiency among free-living healthy young adults. Am J Med. 2002;112:659-662.
9. Fardellone P, Sebert JL, Garabedian M, et al. Prevalence and biological consequences of vitamin D deficiency in elderly institutionalized subjects. Rev Rhum Engl Ed. 1995;62:576-581.
10. Hodkinson HM. Serum calcium in a geriatric inpatient population. Age Ageing. 1973;2:157-162.
11. Desai TK, Carlson RW, Geheb MA. Prevalence and clinical implications of hypocalcemia in acutely ill patients in a medical intensive care setting. Am J Med. 1988;84:209-214.
12. Pattou F, Combemale F, Fabre S, et al. Hypocalcemia following thyroid surgery: incidence and prediction of outcome. World J Surg. 1998;22:718-724.
13. Guise TA, Mundy GR. Clinical review 69: evaluation of hypocalcemia in children and adults. J Clin Endocrinol Metab. 1995;80:1473-1478.
14. Hastbacka J, Pettila V. Prevalence and predictive value of ionized hypocalcemia among critically ill patients. Acta Anaesthesiol Scand. 2003;47:1264-1269.
1. Fukugawa M, Kurokawa K. Calcium homeostasis and imbalance. Nephron. 2002;92(suppl 1):41-45.
2. Ruppe M. Hypocalcemia. In: American College of Physicians (ACP) Physician’s Information and Education Resource (PIER) database. Available at: http://pier.acponline.org/index.html. Accessed October 30, 2007.
3. Carlstedt F, Lind L. Hypocalcemic syndromes. Crit Care Clin. 2001;17:139, 53, vii-viii.
4. Centers for Disease Control and Prevention (CDC). Prevalence of chronic kidney disease and associated risk factors—United States, 1999-2004. MMWR Morb Mortal Wkly Rep. 2007;56:161-165.
5. National Kidney Foundation. K/DOQI clinical practice guidelines for bone metabolism and disease in chronic kidney disease. Am J Kidney Dis. 2003;42(4 suppl 3):S1-S201.
6. Rix M, Andreassen H, Eskildsen P, Langdahl B, Olgaard K. Bone mineral density and biochemical markers of bone turnover in patients with predialysis chronic renal failure. Kidney Int. 1999;56:1084-1093.
7. Thomas MK, Lloyd-Jones DM, Thadhani RI, et al. Hypovitaminosis D in medical inpatients. N Engl J Med. 1998;338:777-783.
8. Tangpricha V, Pearce EN, Chen TC, Holick MF. Vitamin D insufficiency among free-living healthy young adults. Am J Med. 2002;112:659-662.
9. Fardellone P, Sebert JL, Garabedian M, et al. Prevalence and biological consequences of vitamin D deficiency in elderly institutionalized subjects. Rev Rhum Engl Ed. 1995;62:576-581.
10. Hodkinson HM. Serum calcium in a geriatric inpatient population. Age Ageing. 1973;2:157-162.
11. Desai TK, Carlson RW, Geheb MA. Prevalence and clinical implications of hypocalcemia in acutely ill patients in a medical intensive care setting. Am J Med. 1988;84:209-214.
12. Pattou F, Combemale F, Fabre S, et al. Hypocalcemia following thyroid surgery: incidence and prediction of outcome. World J Surg. 1998;22:718-724.
13. Guise TA, Mundy GR. Clinical review 69: evaluation of hypocalcemia in children and adults. J Clin Endocrinol Metab. 1995;80:1473-1478.
14. Hastbacka J, Pettila V. Prevalence and predictive value of ionized hypocalcemia among critically ill patients. Acta Anaesthesiol Scand. 2003;47:1264-1269.
Evidence-based answers from the Family Physicians Inquiries Network
What’s the best treatment for sebaceous cysts?
Punch biopsy excision appears to be superior to traditional wide elliptical excision for the treatment of sebaceous cysts when intervention is necessary (strength of recommendation [SOR]: B, based on 1 small randomized study). No rigorous methodological studies have compared punch biopsy excision of sebaceous cysts with the minimal excision technique.
Cyst qualities dictate technique
Gabrielle O’Sullivan, MD
University of Washington, Seattle
There are 3 main techniques for the removal of sebaceous cysts: traditional wide excision, minimal excision, and punch biopsy excision. For large cysts that have never become inflamed or ruptured, I favor the minimal excision technique because it’s likely that I’ll be able to remove the entire capsule with minimal scarring and faster healing times. Also, for cysts on the face, this method produces a better cosmetic result because of the significantly smaller scar.
However, for a cyst that has ruptured internally, has been expressed manually in the past, or recurs following minimal excision, I find traditional wide excision to be best. In these scenarios, it is extremely time-consuming and often impossible to remove the entire capsule using the minimal excision technique.
Evidence summary
Sebaceous cysts—more correctly referred to as epidermal inclusion cysts—are benign lesions of the skin. They rarely require intervention out of medical necessity, but are removed for cosmetic reasons. If the cysts become inflamed, secondary to internal discharge of the cysts’ contents, or grow so large that they interfere with the patient’s functioning, they may need to be removed.1
Traditional wide excision—involving dissection and removal of the cyst completely from the surrounding tissue through an elliptical incision—is considered the gold standard of treatment. This time-consuming endeavor frequently leads to significant scarring in comparison with minimal excision or punch biopsy, but has almost no recurrence when the cyst wall is entirely removed.2
Minimal excision and punch biopsy techniques are purported to produce minimal bleeding, have faster healing times, and produce less scarring.2 Though both techniques offer a shorter procedural time, they appear to have a slightly higher rates of recurrence.
The minimal incision technique involves kneading the lesion following injection of anesthetic and expressing the cyst contents through a 2- to 3-mm incision. Following expulsion of the cyst contents, the loosened capsule is delivered through the small opening. Closure with suture is optional.3
Punch biopsy excision is similar to the minimal excision technique except that the incision is made using a single-use disposable dermal punch following injection of lidocaine. Expulsion of the cyst contents, with cyst wall, via lateral pressure is performed and occasionally followed by closure with one suture.2
The majority of authors agree that inflamed cysts should be allowed to convalesce prior to attempted removal, though one group (Kitamura et al4) suggests primary resection, wound lavage, and primary suture without drainage for infected epidermal cysts. Rarely are these cysts truly infected. The inflammation is secondary to sebaceous cyst wall rupture with leakage of cyst contents, which elicits the inflammatory response.5
A small study points to cosmetic benefits of punch biopsy
To date, no randomized controlled trials have been published that compare the 3 most common techniques for treatment of sebaceous cysts. Only 1 small (n=60) randomized study compared traditional wide excision with punch biopsy.6 They found punch biopsy to be less time-consuming and to offer superior cosmetic results. However, cysts larger than 2 cm took longer with the punch biopsy technique.
Only a single dermatologist performed all of the surgeries, which could introduce bias. There was no mention of blinding of the researcher that subsequently measured the wounds. Of the 31 patients randomized to the punch biopsy technique, there was 1 recurrence in the 16 months of follow-up compared with none in the wide excision arm. This study excluded patients with infected, inflamed, or recurrent cysts.
Recommendations from others
UpToDate does not recommend excision of an inflamed cyst, suggesting that the inflamed cyst wall is more friable and, therefore, more difficult to remove completely.7 This may lead to a higher rate of recurrence.
Lookingbill and Marks in Principles of Dermatology8 suggest that, frequently, no therapy is indicated for these lesions. If removal is desired or indicated, every effort should be made to remove the entire cyst lining in order to prevent recurrence of the cyst. They recommend removal of the cyst via the traditional wide excision technique. If the cyst ruptures accidentally during the procedure they suggest removing the remaining contents and wall with a curette.
1. GP Notebook [online database]. Stratford-on-Avon, Warwickshire, UK: Oxbridge Solutions Limited; 2003. Sebaceous Cyst. Available at: www.gpnotebook.co.uk. Accessed on March 7, 2007.
2. Mehrabi D, Leonhardt JM, Brodell RT. Removal of keratinous and pilar cysts with the punch incision technique: analysis of surgical outcomes. Dermatol Surg 2002;28:673-677.
3. Zuber TJ. Minimal excision technique for epidermoid (sebaceous) cysts. Am Fam Physician 2002;65:1409-1412, 14171418, 1420.
4. Kitamura K, Takahashi T, Yamaguchi T, Shimotsuma M, Majima T. Primary resection of infectious epidermal cyst. J Am Coll Surg 1994;179:607.-
5. Diven DG, Dozier SE, Meyer DJ, Smith EB. Bacteriology of inflamed and uninflamed epidermal inclusion cysts. Arch Dermatol 1998;134:49-51.
6. Lee HE, Yang CH, Chen CH, Hong HS, Kuan YZ. Comparison of the surgical outcomes of punch incision and elliptical excision in treating epidermal inclusion cysts: a prospective, randomized study. Dermatol Surg 2006;32:520-525.
7. Goldstein BG, Goldstein AO. Benign neoplasms of the skin. UpToDate [online database]. Updated November 21, 2005. Waltham, Mass: UpToDate.
8. Lookingbill DP, Marks JG. Principles of Dermatology. 3rd ed. Philadelphia, Pa: WB saunders Company; 2000.
Punch biopsy excision appears to be superior to traditional wide elliptical excision for the treatment of sebaceous cysts when intervention is necessary (strength of recommendation [SOR]: B, based on 1 small randomized study). No rigorous methodological studies have compared punch biopsy excision of sebaceous cysts with the minimal excision technique.
Cyst qualities dictate technique
Gabrielle O’Sullivan, MD
University of Washington, Seattle
There are 3 main techniques for the removal of sebaceous cysts: traditional wide excision, minimal excision, and punch biopsy excision. For large cysts that have never become inflamed or ruptured, I favor the minimal excision technique because it’s likely that I’ll be able to remove the entire capsule with minimal scarring and faster healing times. Also, for cysts on the face, this method produces a better cosmetic result because of the significantly smaller scar.
However, for a cyst that has ruptured internally, has been expressed manually in the past, or recurs following minimal excision, I find traditional wide excision to be best. In these scenarios, it is extremely time-consuming and often impossible to remove the entire capsule using the minimal excision technique.
Evidence summary
Sebaceous cysts—more correctly referred to as epidermal inclusion cysts—are benign lesions of the skin. They rarely require intervention out of medical necessity, but are removed for cosmetic reasons. If the cysts become inflamed, secondary to internal discharge of the cysts’ contents, or grow so large that they interfere with the patient’s functioning, they may need to be removed.1
Traditional wide excision—involving dissection and removal of the cyst completely from the surrounding tissue through an elliptical incision—is considered the gold standard of treatment. This time-consuming endeavor frequently leads to significant scarring in comparison with minimal excision or punch biopsy, but has almost no recurrence when the cyst wall is entirely removed.2
Minimal excision and punch biopsy techniques are purported to produce minimal bleeding, have faster healing times, and produce less scarring.2 Though both techniques offer a shorter procedural time, they appear to have a slightly higher rates of recurrence.
The minimal incision technique involves kneading the lesion following injection of anesthetic and expressing the cyst contents through a 2- to 3-mm incision. Following expulsion of the cyst contents, the loosened capsule is delivered through the small opening. Closure with suture is optional.3
Punch biopsy excision is similar to the minimal excision technique except that the incision is made using a single-use disposable dermal punch following injection of lidocaine. Expulsion of the cyst contents, with cyst wall, via lateral pressure is performed and occasionally followed by closure with one suture.2
The majority of authors agree that inflamed cysts should be allowed to convalesce prior to attempted removal, though one group (Kitamura et al4) suggests primary resection, wound lavage, and primary suture without drainage for infected epidermal cysts. Rarely are these cysts truly infected. The inflammation is secondary to sebaceous cyst wall rupture with leakage of cyst contents, which elicits the inflammatory response.5
A small study points to cosmetic benefits of punch biopsy
To date, no randomized controlled trials have been published that compare the 3 most common techniques for treatment of sebaceous cysts. Only 1 small (n=60) randomized study compared traditional wide excision with punch biopsy.6 They found punch biopsy to be less time-consuming and to offer superior cosmetic results. However, cysts larger than 2 cm took longer with the punch biopsy technique.
Only a single dermatologist performed all of the surgeries, which could introduce bias. There was no mention of blinding of the researcher that subsequently measured the wounds. Of the 31 patients randomized to the punch biopsy technique, there was 1 recurrence in the 16 months of follow-up compared with none in the wide excision arm. This study excluded patients with infected, inflamed, or recurrent cysts.
Recommendations from others
UpToDate does not recommend excision of an inflamed cyst, suggesting that the inflamed cyst wall is more friable and, therefore, more difficult to remove completely.7 This may lead to a higher rate of recurrence.
Lookingbill and Marks in Principles of Dermatology8 suggest that, frequently, no therapy is indicated for these lesions. If removal is desired or indicated, every effort should be made to remove the entire cyst lining in order to prevent recurrence of the cyst. They recommend removal of the cyst via the traditional wide excision technique. If the cyst ruptures accidentally during the procedure they suggest removing the remaining contents and wall with a curette.
Punch biopsy excision appears to be superior to traditional wide elliptical excision for the treatment of sebaceous cysts when intervention is necessary (strength of recommendation [SOR]: B, based on 1 small randomized study). No rigorous methodological studies have compared punch biopsy excision of sebaceous cysts with the minimal excision technique.
Cyst qualities dictate technique
Gabrielle O’Sullivan, MD
University of Washington, Seattle
There are 3 main techniques for the removal of sebaceous cysts: traditional wide excision, minimal excision, and punch biopsy excision. For large cysts that have never become inflamed or ruptured, I favor the minimal excision technique because it’s likely that I’ll be able to remove the entire capsule with minimal scarring and faster healing times. Also, for cysts on the face, this method produces a better cosmetic result because of the significantly smaller scar.
However, for a cyst that has ruptured internally, has been expressed manually in the past, or recurs following minimal excision, I find traditional wide excision to be best. In these scenarios, it is extremely time-consuming and often impossible to remove the entire capsule using the minimal excision technique.
Evidence summary
Sebaceous cysts—more correctly referred to as epidermal inclusion cysts—are benign lesions of the skin. They rarely require intervention out of medical necessity, but are removed for cosmetic reasons. If the cysts become inflamed, secondary to internal discharge of the cysts’ contents, or grow so large that they interfere with the patient’s functioning, they may need to be removed.1
Traditional wide excision—involving dissection and removal of the cyst completely from the surrounding tissue through an elliptical incision—is considered the gold standard of treatment. This time-consuming endeavor frequently leads to significant scarring in comparison with minimal excision or punch biopsy, but has almost no recurrence when the cyst wall is entirely removed.2
Minimal excision and punch biopsy techniques are purported to produce minimal bleeding, have faster healing times, and produce less scarring.2 Though both techniques offer a shorter procedural time, they appear to have a slightly higher rates of recurrence.
The minimal incision technique involves kneading the lesion following injection of anesthetic and expressing the cyst contents through a 2- to 3-mm incision. Following expulsion of the cyst contents, the loosened capsule is delivered through the small opening. Closure with suture is optional.3
Punch biopsy excision is similar to the minimal excision technique except that the incision is made using a single-use disposable dermal punch following injection of lidocaine. Expulsion of the cyst contents, with cyst wall, via lateral pressure is performed and occasionally followed by closure with one suture.2
The majority of authors agree that inflamed cysts should be allowed to convalesce prior to attempted removal, though one group (Kitamura et al4) suggests primary resection, wound lavage, and primary suture without drainage for infected epidermal cysts. Rarely are these cysts truly infected. The inflammation is secondary to sebaceous cyst wall rupture with leakage of cyst contents, which elicits the inflammatory response.5
A small study points to cosmetic benefits of punch biopsy
To date, no randomized controlled trials have been published that compare the 3 most common techniques for treatment of sebaceous cysts. Only 1 small (n=60) randomized study compared traditional wide excision with punch biopsy.6 They found punch biopsy to be less time-consuming and to offer superior cosmetic results. However, cysts larger than 2 cm took longer with the punch biopsy technique.
Only a single dermatologist performed all of the surgeries, which could introduce bias. There was no mention of blinding of the researcher that subsequently measured the wounds. Of the 31 patients randomized to the punch biopsy technique, there was 1 recurrence in the 16 months of follow-up compared with none in the wide excision arm. This study excluded patients with infected, inflamed, or recurrent cysts.
Recommendations from others
UpToDate does not recommend excision of an inflamed cyst, suggesting that the inflamed cyst wall is more friable and, therefore, more difficult to remove completely.7 This may lead to a higher rate of recurrence.
Lookingbill and Marks in Principles of Dermatology8 suggest that, frequently, no therapy is indicated for these lesions. If removal is desired or indicated, every effort should be made to remove the entire cyst lining in order to prevent recurrence of the cyst. They recommend removal of the cyst via the traditional wide excision technique. If the cyst ruptures accidentally during the procedure they suggest removing the remaining contents and wall with a curette.
1. GP Notebook [online database]. Stratford-on-Avon, Warwickshire, UK: Oxbridge Solutions Limited; 2003. Sebaceous Cyst. Available at: www.gpnotebook.co.uk. Accessed on March 7, 2007.
2. Mehrabi D, Leonhardt JM, Brodell RT. Removal of keratinous and pilar cysts with the punch incision technique: analysis of surgical outcomes. Dermatol Surg 2002;28:673-677.
3. Zuber TJ. Minimal excision technique for epidermoid (sebaceous) cysts. Am Fam Physician 2002;65:1409-1412, 14171418, 1420.
4. Kitamura K, Takahashi T, Yamaguchi T, Shimotsuma M, Majima T. Primary resection of infectious epidermal cyst. J Am Coll Surg 1994;179:607.-
5. Diven DG, Dozier SE, Meyer DJ, Smith EB. Bacteriology of inflamed and uninflamed epidermal inclusion cysts. Arch Dermatol 1998;134:49-51.
6. Lee HE, Yang CH, Chen CH, Hong HS, Kuan YZ. Comparison of the surgical outcomes of punch incision and elliptical excision in treating epidermal inclusion cysts: a prospective, randomized study. Dermatol Surg 2006;32:520-525.
7. Goldstein BG, Goldstein AO. Benign neoplasms of the skin. UpToDate [online database]. Updated November 21, 2005. Waltham, Mass: UpToDate.
8. Lookingbill DP, Marks JG. Principles of Dermatology. 3rd ed. Philadelphia, Pa: WB saunders Company; 2000.
1. GP Notebook [online database]. Stratford-on-Avon, Warwickshire, UK: Oxbridge Solutions Limited; 2003. Sebaceous Cyst. Available at: www.gpnotebook.co.uk. Accessed on March 7, 2007.
2. Mehrabi D, Leonhardt JM, Brodell RT. Removal of keratinous and pilar cysts with the punch incision technique: analysis of surgical outcomes. Dermatol Surg 2002;28:673-677.
3. Zuber TJ. Minimal excision technique for epidermoid (sebaceous) cysts. Am Fam Physician 2002;65:1409-1412, 14171418, 1420.
4. Kitamura K, Takahashi T, Yamaguchi T, Shimotsuma M, Majima T. Primary resection of infectious epidermal cyst. J Am Coll Surg 1994;179:607.-
5. Diven DG, Dozier SE, Meyer DJ, Smith EB. Bacteriology of inflamed and uninflamed epidermal inclusion cysts. Arch Dermatol 1998;134:49-51.
6. Lee HE, Yang CH, Chen CH, Hong HS, Kuan YZ. Comparison of the surgical outcomes of punch incision and elliptical excision in treating epidermal inclusion cysts: a prospective, randomized study. Dermatol Surg 2006;32:520-525.
7. Goldstein BG, Goldstein AO. Benign neoplasms of the skin. UpToDate [online database]. Updated November 21, 2005. Waltham, Mass: UpToDate.
8. Lookingbill DP, Marks JG. Principles of Dermatology. 3rd ed. Philadelphia, Pa: WB saunders Company; 2000.
Evidence-based answers from the Family Physicians Inquiries Network