• Cancer patients
• Immuno-compromised (HIV) and immuno-suppressed (chemotherapy) patients
• Hodgkin's disease
• Kidney transplantation
• After serious injury or infection

• pain and/or itching typically precedes the appearance of rash by several days.
• pain has little or no bearing on the severity of lesions (and visa versa)
• location of the rash
  • thoracic dermatomes 50%
  • trigeminal 3-20% (mainly the ophthalmic division). With advancing age, the incidence of trigeminal HZ increases, and  the incidence of PHN may also be higher with trigeminal eruptions.
  • lumbar/cervical dermatomes 12-20%
  • bilateral eruptions < 1%
  • recurrent HZ 1-8% patients, of these 50% in same location. 
• rash characteristics - red areas of skin --> raised red areas (papules) --> vesicles (blisters) within 24 - 36 hours --> crust formation (this can continue for 1 month)

PHN is simply defined as persisting pain in the area of the rash once the HZ lesions have healed. It presents as:-

• extreme sensitivity of the skin in the area affected by the HZ rash, especially to light touch and brushing by clothing. The sensitivity seems to be worst in the whiter scarred areas of skin which have lost their pigmentation.
• spontaneous pain in the area which may be aching or stabbing in nature.
• secondary musculo-skeletal problems (muscles, joints) caused by excessive guarding of the affected area. This pain can then contribute to the overall clinical picture adding movement induced pain.

• The two most important reasons for treating acute HZ early are :-
  1. To prevent virus multiplication thereby reducing damage to the dorsal horn, dorsal root ganglion, and peripheral sensory receptors in the skin. The early use of anti-viral drugs like acyclovir and famcyclovir help to reduce the severity of acute HZ and the incidence and severity of PHN by limiting viral induced nerve damage.
  2. To prevent excessive degrees of dorsal horn sensitization. Acute HZ pain has both somatic and nerve components. Early pain management with combinations of acetaminophen, NSAIDs, opioids, and amitriptyline help to reduce severe pain and therefore reduce sensitization of the dorsal horn. There is strong evidence that early use of amitriptyline reduces the incidence and severity of PHN.
• Other treatment which have been recommended (but not proven) in acute HZ are:-
  • Early sympathetic nerve blocks.
  • Oral steroids (prednisolone 60-80 mg per day for 10 days then taper off) may help earlier resolution of HZ pain, but may not affect the development of PHN.
  • TENS

• Amitriptyline ** 10 - 50 mg per day
• Anti-convulsants - gabapentin ** is the most popular of these. The use of all the others has been described.
• Topical Capsaicin ** (0.025% or 0.075%) can be useful in some patients.
• Herpetic scar desensitisation ** - some patients find that infiltrating the depigmented areas of skin with LA/steroids on several occasions radically reduces hypersensitivity.
• Lidocaine 5% patch ** - in the USA the topical use of a lidocaine patch can very effectively reduce the degree of skin sensitivity.
• TENS (not proven) - may aggravate sensitivity rather than help it.
• Topical Aspirin (not proven)
• Topical NSAIDs (not proven)
• Combinations of analgesics including acetaminophen, NSAIDs, weak opioids. These however are often found to be ineffective as the pain is mostly neuralgic in nature, and therefore fairly resistant to traditional analgesics.
• Sympathetic Blockade (early)
• Dorsal Root Ganglion Block (early)
• Epidural steroid injections (early) at the correct spinal segment to reduce the degree of nerve damage.
• Physical therapy including spinal manipulation is important for those with secondary musculo-skeletal pain.
• Neuro-ablative procedures - these should be avoided, as few, if any trials have shown them to be helpful for long-term improvement. If considering, consider DREZ and deep brain stimulation (early studies show "some" promise).