Bottlenecks in the development of topical analgesics: molecule, formulation, dose-finding, and phase III design

Topical analgesics can be defined as topical formulations containing analgesics or co-analgesics. Since 2000, interest in such formulations has been on the rise. There are, however, four critical issues in the research and development phases of topical analgesics: 1) The selection of the active pharmaceutical ingredient. Analgesics and co-analgesics differ greatly in their mechanism of action, and it is required to find the most optimal fit between such mechanisms of action and the pathogenesis of the targeted (neuropathic) pain. 2) Issues concerning the optimized formulation. For relevant clinical efficacy, specific characteristics for the selected vehicle (eg, cream base or gel base) are required, depending on the physicochemical characteristics of the active pharmaceutical ingredient(s) to be delivered. 3) Well-designed phase II dose-finding studies are required, and, unfortunately, such trials are missing. In fact, we will demonstrate that underdosing is one of the major hurdles to detect meaningful and statistically relevant clinical effects of topical analgesics. 4) Selection of clinical end points and innovatively designed phase III trials. End point selection can make or break a trial. For instance, to include numbness together with tingling as a composite end point for neuropathic pain seems stretching the therapeutic impact of an analgesic too far. Given the fast onset of action of topical analgesics (usually within 30 minutes), enrichment designs might enhance the chances for success, as the placebo response might decrease. Topical analgesics may become promising inroads for the treatment of neuropathic pain, once sufficient attention is given to these four key aspects.

[1]  D. J. Kopsky,et al.  Topical phenytoin for the treatment of neuropathic pain , 2017, Journal of pain research.

[2]  D. J. Kopsky,et al.  Skin matters! The role of keratinocytes in nociception: a rational argument for the development of topical analgesics , 2016, Journal of pain research.

[3]  D. J. Kopsky,et al.  New topical treatment of vulvodynia based on the pathogenetic role of cross talk between nociceptors, immunocompetent cells, and epithelial cells , 2016, Journal of pain research.

[4]  T. Meert,et al.  NRP-1 Receptor Expression Mismatch in Skin of Subjects with Experimental and Diabetic Small Fiber Neuropathy , 2016, PloS one.

[5]  D. Tu,et al.  Combination of pregabalin with duloxetine for fibromyalgia: a randomized controlled trial , 2016, Pain.

[6]  P. Drummond,et al.  Topical prazosin attenuates sensitivity to tactile stimuli in patients with complex regional pain syndrome , 2016, European journal of pain.

[7]  D. J. Kopsky,et al.  Extending the Therapeutic Scope for the Treatment of Neuropathic Pain with Topical Analgesics , 2016 .

[8]  Danielle M. Santarelli,et al.  A Novel Compound Analgesic Cream (Ketamine, Pentoxifylline, Clonidine, DMSO) for Complex Regional Pain Syndrome Patients , 2016, Pain practice : the official journal of World Institute of Pain.

[9]  K. Hesselink Thinking Out of the Pillbox : The Relevance to Topiceuticals in the Treatment of Neuropathic Pain , 2016 .

[10]  D. J. Kopsky,et al.  Topical analgesic creams and nociception in diabetic neuropathy: towards a rationale fundament , 2016 .

[11]  D. Tu,et al.  Combination of morphine with nortriptyline for neuropathic pain , 2015, Pain.

[12]  D. J. Kopsky,et al.  Analgesic effects of topical ketamine. , 2015, Minerva anestesiologica.

[13]  P. Drummond,et al.  Activation of cutaneous immune responses in complex regional pain syndrome. , 2014, The journal of pain : official journal of the American Pain Society.

[14]  C. Heckler,et al.  A phase III randomized, placebo-controlled study of topical amitriptyline and ketamine for chemotherapy-induced peripheral neuropathy (CIPN): a University of Rochester CCOP study of 462 cancer survivors , 2014, Supportive Care in Cancer.

[15]  D. J. Kopsky,et al.  Neuropathic pain as a result of acromegaly, treated with topical baclofen cream. , 2013, Journal of pain and symptom management.

[16]  D. J. Kopsky,et al.  Treatment of chronic regional pain syndrome type 1 with palmitoylethanolamide and topical ketamine cream: modulation of nonneuronal cells , 2013, Journal of pain research.

[17]  S. Mariz,et al.  The development and registration of topical pharmaceuticals. , 2012, International journal of pharmaceutics.

[18]  V. Vardaxis,et al.  Topical ketamine cream in the treatment of painful diabetic neuropathy: a randomized, placebo-controlled, double-blind initial study. , 2012, Journal of the American Podiatric Medical Association.

[19]  D. J. Kopsky,et al.  High Doses of Topical Amitriptyline in Neuropathic Pain: Two Cases and Literature Review , 2012, Pain practice : the official journal of World Institute of Pain.

[20]  C. Loprinzi,et al.  A double-blind, placebo-controlled trial of a topical treatment for chemotherapy-induced peripheral neuropathy: NCCTG trial N06CA , 2011, Supportive Care in Cancer.

[21]  Richard E. White,et al.  Research design considerations for confirmatory chronic pain clinical trials: IMMPACT recommendations , 2010, PAIN®.

[22]  N. Latov,et al.  Differential gene expression in chronic inflammatory demyelinating polyneuropathy (CIDP) skin biopsies , 2010, Journal of the Neurological Sciences.

[23]  L. Knudsen,et al.  Reduction of allodynia in patients with complex regional pain syndrome: A double-blind placebo-controlled trial of topical ketamine , 2009, PAIN.

[24]  D. Tu,et al.  Nortriptyline and gabapentin, alone and in combination for neuropathic pain: a double-blind, randomised controlled crossover trial , 2009, The Lancet.

[25]  C. Mariani,et al.  Overview on Pathophysiology and Newer Approaches to Treatment of Peripheral Neuropathies , 2007, CNS Drugs.

[26]  D. Selvarajah,et al.  Morphine, gabapentin, or their combination for neuropathic pain. , 2005, The New England journal of medicine.

[27]  A. J. Clark,et al.  A Pilot Study Examining Topical Amitriptyline, Ketamine, and a Combination of Both in the Treatment of Neuropathic Pain , 2003, The Clinical journal of pain.

[28]  D. Gilden,et al.  Topical ketamine treatment of postherpetic neuralgia , 2003, Neurology.

[29]  Jesse A. Berlin,et al.  Defining the clinically important difference in pain outcome measures , 2000, PAIN.

[30]  M. Esser,et al.  Peripheral antinociceptive actions of desipramine and fluoxetine in an inflammatory and neuropathic pain test in the rat , 1999, Pain.

[31]  M. Esser,et al.  Acute amitriptyline in a rat model of neuropathic pain: differential symptom and route effects , 1999, Pain.

[32]  M. Rowbotham,et al.  Topical lidocaine patch relieves postherpetic neuralgia more effectively than a vehicle topical patch: results of an enriched enrollment study , 1999, Pain.

[33]  M. Esser,et al.  Peripheral antinociceptive action of amitriptyline in the rat formalin test: involvement of adenosine , 1999, Pain.

[34]  M. Scott,et al.  Use of Transdermal Amitriptyline Gel in a Patient with Chronic Pain and Depression , 1999, Pharmacotherapy.

[35]  G. Gebhart,et al.  Effects of tricyclic antidepressants on mechanosensitive pelvic nerve afferent fibers innervating the rat colon , 1998, Pain.

[36]  P. Luisi,et al.  Lecithin organogel as matrix for transdermal transport of drugs. , 1992, Journal of pharmaceutical sciences.

[37]  A. Eschalier,et al.  Evidence for a central but not a peripheral analgesic effect of clomipramine in rats , 1991, Pain.

[38]  J. Besson,et al.  Reduction of arthritis and pain behaviour following chronic administration of amitriptyline or imipramine in rats with adjuvant-induced arthritis , 1985, Pain.

[39]  K. Soltani,et al.  Inhibition of histamine-induced pruritus by topical tricyclic antidepressants. , 1981, Journal of the American Academy of Dermatology.