2011
DOI: 10.1177/2042018810391900
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Clinical approach to the treatment of painful diabetic neuropathy

Abstract: Painful neuropathy is a common and often progressive complication of diabetes. Patients frequently report symptoms of tingling, burning, lancinating pain, hyperesthesia and allodynia. The natural history of the disease may vary from intermittent mild symptoms to severe chronic daily pain; the latter is often associated with diminished quality of life. There are a variety of pharmaceutical agents from different medicinal categories available for the symptomatic treatment of painful diabetic neuropathy, however … Show more

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Cited by 34 publications
(26 citation statements)
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“…Treatments that are currently prescribed to lessen neuropathic pain have undesirable secondary effects and situational variable efficacy [12] . Therefore, researchers are searching for better diabetic neuropathy drug options.…”
Section: Introductionmentioning
confidence: 99%
“…Treatments that are currently prescribed to lessen neuropathic pain have undesirable secondary effects and situational variable efficacy [12] . Therefore, researchers are searching for better diabetic neuropathy drug options.…”
Section: Introductionmentioning
confidence: 99%
“…Advanced peripheral diabetic neuropathy classically manifests as chronic progressive thick (Aβ) and thin (Aδ) fiber neuropathy affecting myelinated axons and later affecting also the unmyelinated C-fibers [2,3]. The natural history of the disease varies from intermittent mild symptoms to manifest neuropathic pain, the latter being present in up to one fourth of the patients diminishing their quality of life [4][5][6]. The typical appearance is length dependent sensorimotor neuropathy caused by chronic progressive symmetric deafferentation and Schwann cell degeneration affecting axons of the distal lower extremities [2,7].…”
Section: Introductionmentioning
confidence: 99%
“…In this regard, the mean dose of pregabalin, which ranged from 155.3 to 165.3 mg across the cohorts, is lower than the therapeutic dose of 300 mg and thus may have contributed to the low rates of adherence, especially relative to duloxetine for which the mean dose, 54.8 mg, approximates the therapeutic dose of 60 mg. Furthermore, the mean doses of gabapentin (698.8 mg) and amitriptyline (32.5 mg) were also substantially lower than the average effective doses, although high doses of the latter drug are also associated with anticholinergic adverse effects. While reports of the relationship between dose and adherence have also been published for duloxetine in pDPN, it is worth identifying factors other than dose level that can be leveraged for improving patient adherence to therapy.…”
Section: Discussionmentioning
confidence: 96%