R.M. Poole’s research while affiliated with University of Rochester and other places

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Publications (5)


Lesser H, Sharma U, LaMoreaux L, Poole RM. Pregabalin relieves symptoms of painful diabetic neuropathy: a randomized controlled trial. Neurology 63: 2104-2110
  • Article

December 2004

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242 Reads

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577 Citations

Neurology

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R M Poole

Pregabalin, an alpha2-delta ligand with analgesic, anxiolytic, and anticonvulsant activity, has been evaluated for treatment of neuropathic pain. The authors assessed the efficacy and tolerability of pregabalin (75, 300, 600 mg/day) vs placebo in patients with diabetic peripheral neuropathy (DPN). Patients with a 1- to 5-year history of DPN and average weekly pain score of > or =4 on an 11-point numeric pain-rating scale were enrolled in a 5-week, double-blind, multicenter, placebo-controlled study. Patients (n = 338) were randomized to receive one of three doses of pregabalin or placebo TID. Pregabalin 600 mg/day was titrated over 6 days; lower doses were initiated on day 1. Patients in the 300- and 600-mg/day pregabalin groups showed improvements in endpoint mean pain score (primary efficacy measure) vs placebo (p = 0.0001). Improvements were also seen in weekly pain score, sleep interference score, patient global impression of change, clinical global impression of change, SF-McGill Pain Questionnaire, and multiple domains of the SF-36 Health Survey. Improvements in pain and sleep were seen as early as week 1 and were sustained throughout the 5 weeks. Responders (patients with > or =50% reduction in pain compared to baseline) were 46% (300 mg/day), 48% (600 mg/day), and 18% (placebo). Pregabalin was well tolerated with a low discontinuation rate. The most common adverse events were dizziness and somnolence. In patients with diabetic peripheral neuropathy, pregabalin demonstrated early and sustained improvement in pain and a beneficial effect on sleep, which were confirmed by positive patient global impression. Pregabalin was well tolerated at all doses.


Pregabalin for the treatment of postherpetic neuralgia: A randomized, placebo-controlled trial

April 2003

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499 Reads

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766 Citations

Neurology

R H Dworkin

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J. P. Jr. Young

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R M Poole

To evaluate the efficacy and safety of pregabalin in the treatment of postherpetic neuralgia (PHN). The authors conducted a multicenter, parallel-group, double-blind, placebo-controlled, 8-week, randomized clinical trial in PHN, defined as pain for 3 or more months following herpes zoster rash healing. Patients (n = 173) were randomized to treatment with pregabalin or placebo. Patients randomized to pregabalin received either 600 mg/day (creatinine clearance > 60 mL/min) or 300 mg/day (creatinine clearance 30 to 60 mL/min). The primary efficacy measure was the mean of the last seven daily pain ratings. Secondary endpoints included additional pain ratings, sleep interference, quality of life, mood, and patient and clinician ratings of global improvement. Pregabalin-treated patients had greater decreases in pain than patients treated with placebo (endpoint mean scores 3.60 vs 5.29, p = 0.0001). Pain was significantly reduced in the pregabalin-treated patients after the first full day of treatment and throughout the study, and significant improvement on the McGill Pain Questionnaire total, sensory, and affective pain scores was also found. The proportions of patients with >or=30% and >or=50% decreases in mean pain scores were greater in the pregabalin than in the placebo group (63% vs 25% and 50% vs 20%, p = 0.001). Sleep also improved in patients treated with pregabalin compared to placebo (p = 0.0001). Both patients and clinicians were more likely to report global improvement with pregabalin than placebo (p = 0.001). Given the maximal dosage studied, pregabalin had acceptable tolerability compared to placebo despite a greater incidence of side effects, which were generally mild to moderate in intensity. Treatment of PHN with pregabalin is safe, efficacious in relieving pain and sleep interference, and associated with greater global improvement than treatment with placebo.



Farrar JT, Young JP Jr, LaMoreaux L, Werth JL, Poole RM. Clinical importance of changes in chronic pain intensity measured on an 11-point numerical pain rating scale. Pain. 94: 149-158

December 2001

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7,338 Reads

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4,523 Citations

Pain

Pain intensity is frequently measured on an 11-point pain intensity numerical rating scale (PI-NRS), where 0=no pain and 10=worst possible pain. However, it is difficult to interpret the clinical importance of changes from baseline on this scale (such as a 1- or 2-point change). To date, there are no data driven estimates for clinically important differences in pain intensity scales used for chronic pain studies. We have estimated a clinically important difference on this scale by relating it to global assessments of change in multiple studies of chronic pain. Data on 2724 subjects from 10 recently completed placebo-controlled clinical trials of pregabalin in diabetic neuropathy, postherpetic neuralgia, chronic low back pain, fibromyalgia, and osteoarthritis were used. The studies had similar designs and measurement instruments, including the PI-NRS, collected in a daily diary, and the standard seven-point patient global impression of change (PGIC), collected at the endpoint. The changes in the PI-NRS from baseline to the endpoint were compared to the PGIC for each subject. Categories of "much improved" and "very much improved" were used as determinants of a clinically important difference and the relationship to the PI-NRS was explored using graphs, box plots, and sensitivity/specificity analyses. A consistent relationship between the change in PI-NRS and the PGIC was demonstrated regardless of study, disease type, age, sex, study result, or treatment group. On average, a reduction of approximately two points or a reduction of approximately 30% in the PI-NRS represented a clinically important difference. The relationship between percent change and the PGIC was also consistent regardless of baseline pain, while higher baseline scores required larger raw changes to represent a clinically important difference. The application of these results to future studies may provide a standard definition of clinically important improvement in clinical trials of chronic pain therapies. Use of a standard outcome across chronic pain studies would greatly enhance the comparability, validity, and clinical applicability of these studies.


Citations (5)


... Pregabalin is a selective, high-affinity ligand for a novel central nervous system binding site, the a 2 d subunit of voltage-dependent calcium channels (Gee et al., 1996). The ability of pregabalin to decrease neuronal excitability by selectively attenuating presynaptic calcium influx through these channels Fink et al., 2002) may underlie its efficacy in patients with partial seizures (French et al., 2003;Miller et al., 2003), chronic pain disorders (Iacobellis et al., 2000;Glessner et al., 2001;Crofford et al., 2002;Dworkin et al., 2003), and generalized anxiety disorder Pande et al., 2003). A population pharmacokinetic analysis (Bockbrader et al., 2010) was performed to characterize pregabalin pharmacokinetics in healthy volunteers (Corrigan et al., 2001), patients with various chronic pain disorders, and patients with epilepsy who participated in a series of phase 3 add-on trials. ...

Reference:

Pregabalin effect on steady-state pharmacokinetics of carbamazepine, lamotrigine, phenobarbital, phenytoin, topiramate, valproate, and tiagabine
Pregabalin improves pain associated with fibromyalgia syndrome in a multicenter, randomized, placebo-controlled monotherapy trial
  • Citing Article
  • January 2002

Arthritis & Rheumatology

... After obtaining informed consent from the participants, data was collected using the Standard Nordic Musculoskeletal Questionnaire (SNMQ) 19 , the Beck Depression Inventory (BDI) 20 , and the Numeric Pain Rating Scale (NPRS) 21 (Figure 1). Body mass index (BMI) of all the subjects was also calculated in line with the World Health Organisation (WHO) recommendations specific to South Asia. ...

Clinical importance of changes in chronic pain intensity measured on an 11-point numerical pain rating scale
  • Citing Article
  • January 2001

Pain

... The face scale of the JACQLQ Domain III comprised a 5-scale anchor to categorize the participants into 5 severity categories [29]. A previous study used a 2-point change as a meaningful difference on an 11-point scale [29,46,47]. Based on this method, an 11-point stress level scale was used as the 5-scale anchor, and participants were assigned to one of the five severity groups [47]. ...

Farrar JT, Young JP Jr, LaMoreaux L, Werth JL, Poole RM. Clinical importance of changes in chronic pain intensity measured on an 11-point numerical pain rating scale. Pain. 94: 149-158
  • Citing Article
  • December 2001

Pain

... These findings are promising, given that the use of gabapentinoids is often associated with concerns regarding side effects [66,67]. These side effects are dose-dependent and can lead to the discontinuation of the drug due to intolerability [56]. ...

Pregabalin for the treatment of postherpetic neuralgia: A randomized, placebo-controlled trial
  • Citing Article
  • April 2003

Neurology

... A total of 321 studies were screened in the title and abstract phases, and 297 were full-text screened. A final 16 studies were reviewed, and their reported PROs were systematically summarized ( Figure 1) [15][16][17][18][19][20][21][22][23][24][25][26][27][28][29][30]. The summary of the study characteristics is reported in Table 1. ...

Lesser H, Sharma U, LaMoreaux L, Poole RM. Pregabalin relieves symptoms of painful diabetic neuropathy: a randomized controlled trial. Neurology 63: 2104-2110
  • Citing Article
  • December 2004

Neurology