Effective treatment of neuropathic pain without unacceptable side effects is challenging. Cancer sufferers increasingly live with long-term treatment-related neuropathic pain, resulting from chemotherapy-induced peripheral neuropathy (CIPN) or surgical scars. This proof-of-concept study aimed to determine whether preclinical evidence for TRPM8 ion channels in sensory neurons as a novel analgesic target could be translated to clinical benefit in patients with neuropathic pain, using the TRPM8 activator menthol.
Patients and methods
Patients with problematic treatment-related neuropathic pain underwent a baseline assessment using validated questionnaires, psychophysical testing, and objective functional measures. The painful area was treated with topical 1 % menthol cream twice daily. Assessments were repeated at 4–6 weeks. The primary outcome was the change in Brief Pain Inventory total scores at 4–6 weeks. Secondary outcomes included changes in function, mood and skin sensation.
Results
Fifty-one patients (female/male, 32/19) were recruited with a median age of 61 (ranging from 20 to 89). The commonest aetiology was CIPN (35/51), followed by scar pain (10/51). Thirty-eight were evaluable on the primary outcome. Eighty-two per cent (31/38) had an improvement in total Brief Pain Inventory scores (median, 47 (interquartile range, 30 to 64) to 34 (6 to 59), P < 0.001). Improvements in mood (P = 0.0004), catastrophising (P = 0.001), walking ability (P = 0.008) and sensation (P < 0.01) were also observed.
Conclusion
This proof-of-concept study indicates that topical menthol has potential as a novel analgesic therapy for cancer treatment-related neuropathic pain. Improvements in patient-rated measures are supported by changes in objective measures of physical function and sensation. Further systematic evaluation of efficacy is required.
Hinweise
Where presented in part elsewhere: Chemotherapy induced neuropathy subgroup presented at ASCO 2011
Introduction
Chronic neuropathic pain, resulting from nerve injury, is a challenging clinical problem which is difficult to treat with current analgesics without unacceptable side effects. It greatly reduces quality of life, even more so than other chronic pain states with a negative impact on mobility, function, mood and general wellbeing [1]. The prevalence of neuropathic pain is likely to be underestimated, but studies from North America and Europe have found between 8 and 17 % of the population may suffer from pain of predominantly neuropathic origin [2‐4]. Neuropathic pain associated with cancer treatment is an increasing challenge. As the incidence of cancer increases and survival improves with better oncological management, there is an increasing number of patients living with the long-term effects of treatment such as chemotherapy-induced peripheral neuropathy (CIPN) or surgical scar pain [5, 6].
CIPN affects up to 96 % of patients who receive potentially neurotoxic chemotherapy (e.g. platinums, taxanes, vinca-alkaloids and bortezomib), resulting in dose reduction or early cessation of treatment for up to 50 % [7‐10]. Symptoms are commonly in a glove and stocking distribution and include spontaneous pain, paraesthesia, allodynia (nonpainful stimuli causing pain), hyperalgesia (increased sensitivity to painful stimuli), hypoaesthesia (numbness) and impaired proprioception, causing difficulty with day-to-day functioning such as fastening buttons, handling coins, walking and driving. In our centre, 50 % of colorectal cancer patients still had symptoms of neuropathy 12 months after completing treatment with curative intent [5].
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Estimates for persistent neuropathic pain after cancer surgery vary, with post-mastectomy and post-thoracotomy pain occurring in 30–60 % of patients [11]. One large study after breast cancer surgery found almost half of patients had persistent pain 2 to 3 years later, with this being moderate to severe in nearly a quarter of patients [12]. In our own centre, approximately 30 % of patients had persistent post-mastectomy pain, with a threefold increase in risk conferred by adjuvant chemotherapy [13]. Recent guidelines suggest the use of objective quantifiable tests such as Quantitative Sensory Testing as clinical biomarkers to strengthen the diagnosis of neuropathic pain, which is made on history and examination [14, 15].
Treatment of neuropathic pain relies on early identification, understanding of the initiating and sustaining pathophysiological mechanisms and use of a range of therapeutic approaches [16]. Evidence is accumulating which suggests that the neurosensory characteristics of the pain may be the most important factor in predicting a treatment response, rather than the underlying aetiology [17, 18]. Current systemic therapy is mainly oral antidepressants or anticonvulsants; however, treatment often requires titration over months and is limited by variable efficacy and unacceptable side effects [19]. Nontoxic therapies, which reduce pain with minimal side effects, are needed.
A new potential novel therapeutic approach has arisen as a result of basic science findings from our translational research group which demonstrated that endogenous neural circuitry underlying cooling-induced analgesia may represent a novel target for intervention. Molecular receptors for cooling have been identified in sensory nerves with evidence for their upregulation in neuropathic pain models [20, 21]. Our group identified how activation of one of these, the transient receptor potential melastatin (TRPM)8 ion channel, by topical agents, produced significant analgesia [22]. As a result of this work, we successfully used topical menthol, a TRPM8 agonist, in two cases of treatment-resistant chemotherapy-induced peripheral neuropathy, allowing continuation of life-prolonging treatment [23, 24]. If topical TRPM8 agonists produced profound, mechanistically novel analgesia in chronic neuropathic pain, this would be a significant advance.
Aims
The primary aim of this study is to determine whether 4–6 weeks of topical 1 % menthol in aqueous cream provided effective analgesia for neuropathic pain in a proof-of-concept study (assessed using the Brief Pain Inventory).
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The secondary aims of this study is to determine whether mood and surrogate clinical measures (biomarkers) of neuropathic pain (physical function and quantitative sensory testing) improved after 4–6 weeks of topical 1 % menthol in aqueous cream.
Methods
This was an open-label proof-of-concept study. After obtaining research ethics committee approval and written informed consent, suitable patients were recruited from the Edinburgh Regional Cancer Centre. For inclusion, patients had to meet the following criteria: chronic neuropathic pain (diagnosed by a palliative medicine or pain medicine specialist); stable pain, not expected to change within the following 6 weeks; an average pain severity of ≥/4 on a 0 to 10 scale; aged 18 years or over; and either had tried conventional anti-neuropathic agents or these were contraindicated/declined. Patients were excluded if they had any medical or psychiatric condition that would confound the study objectives. Patients underwent a comprehensive assessment of pain and its impact on function immediately prior to treatment and after 2 and 4–6 weeks of treatment, as recommended by the Initiative on Methods, Measurement and Pain Assessment in Clinical Trials (IMMPACT) [25]. Standard demographic data were collected. The 1 % (−) menthol (levomenthol) in aqueous cream was used topically. Each patient was instructed on how to apply the cream to the affected area and corresponding dermatomal region of spine, twice daily on a regular basis.
Each assessment comprised:
1.
Validated self-report questionnaires to assess the sensory, cognitive and affective components of pain, with higher scores representing more severe symptoms:
a.
The short-form Brief Pain Inventory (BPI): an 11-item assessment using a 0 (no pain/interference) to 10 (worst pain/interference) rating scale of pain intensity and its impact (interference with general activity, mood, walking ability, normal work, relations with others, sleep and enjoyment of life over the last week). The total BPI is the sum of all 11 items (ranging from 0 to 110), the interference subscale is the total of the seven interference items (ranging from 0 to 70) [26].
b.
Hospital Anxiety and Depression scale (HADS): with a range of 0–21 for both anxiety and depression [27].
c.
Pain Catastrophising scale: This measures rumination, magnification and helplessness. Range of 0–65, with values of >30 thought to be of clinical significance [28].
d.
Leeds Assessment of Neuropathic Symptoms and Signs (LANSS): is a validated screening tool for neuropathic pain (range 0-24, score ≥12 is indicative of neuropathic pain) [29].
2.
Surrogate clinical biomarker measures of neuropathic pain:
a.
Objective measures of functional performance:
i.
Walking ability was assessed using a GAITRite® walking mat to measure gait velocity (cm/s) and cadence (steps/min) [30].
ii.
Hand dexterity. Patients were instructed to fill a five-by-five slotted board with grooved pegs in an ordered fashion. The time taken (s) to do this with the dominant and nondominant hands was recorded [31, 32].
b.
Quantitative Sensory Testing (QST) was conducted using our well-established protocol that has been used successfully in frail patients [33]. Skin overlying the affected area and an unaffected control area were assessed (either the equivalent contralateral dermatomal region, or for patients with bilateral peripheral neuropathy, a more proximal unaffected area). Testing was carried out in a quiet environment with the patient relaxed and took 20–40 min. All researchers underwent standardised QST training to use the following protocol:
i.
The affected area was mapped using a calibrated brush (Senselab 0.5 mN Somedic, Sweden) moving from normal to affected areas. Areas of abnormal sensation were marked out on the skin. The patient was asked to describe how this sensation compared with the control area (hyperaesthesia, hypoaesthesia or unchanged) and, if painful, it was rated on a 0 to 10 numerical rating scale (NRS). The area of abnormal sensation was measured using tracing paper (recorded in cm2 for patients with scar pain) or distance (cm) measured from the middle finger tip or great toe for peripheral neuropathies. For the latter, the percentage of the limb affected was calculated as a proportion of the distance from the finger tip/great toe to the olecranon/inferior patella border.
ii.
Thermal sensory mapping was conducted in a similar way using warm (40 °C) and cool (25 °C) rollers (Rolltemp, Somedic, Sweden).
iii.
Mechanical Detection Threshold (MDT) and Mechanical Pain Threshold (MPT) were assessed with 17 von Frey monofilaments of varying thickness, calibrated according to the force required to make them bend (0.026 to 110 g, Somedic, Sweden). Using the Method of Levels the monofilaments were applied to the skin in ascending order and the MDT noted when felt consistently (detecting three out of five applications). MPT was the force when the stimulus became unpleasant and rated using a NRS from 0 to 10.
iv.
Mechanical pain sensitivity (hyperalgesia) was tested using noxious pin prick stimulus (NeurotipsTM Owen Mumford) and rated using an NRS from 0 to 10.
v.
Temporal summation was assessed using five rapidly repeated pin prick stimuli and a NRS rating. The wind up ratio was calculated as the NRS score (repeated stimuli)/NRS score (single stimulus) [34].
Statistical analysis
Data were displayed as mean (standard deviation (SD)), median (interquartile range) or proportions as appropriate. Continuous variables at baseline and 4–6 weeks were compared using the Wilcoxon signed rank test or paired t test as appropriate. The primary variable of interest was the change in pain as assessed by the total BPI. Responders were defined as a ≥30 % reduction in total BPI, which is considered to be a clinically meaningful improvement [35]. Responders and nonresponders were compared, to define any patient characteristics associated with a treatment response, using the Mann–Whitney U test or two-sample t test as appropriate. This was an exploratory analysis and a P value of <0.05 was considered statistically significant with no correction for multiple testing.
Results
Fifty-one patients entered the study. The median age was 61 (ranging from 20 to 89), and the majority were female (32/51, 63 %). Most had been treated for cancer (41/51, 80 %) and the majority of these were recurrence free (33/41, 80 %). The commonest neuropathic pain aetiology was CIPN (31/51, 61 %), followed by scar pain (10/51, 20 %, most frequently post-mastectomy) and miscellaneous reasons (10/51, 20 %) (Table 1). Thirty (59 %) patients had tried a range of standard analgesics and anti-neuropathic agents. During the study period 7 (14 %), patients were on a variety of standard analgesics, with no relevant medication change during the study period. Forty-four (86 %) patients were on no analgesics during the study period.
Table 1
Patients’ characteristics at baseline
Neuropathic pain aetiology
Total n = 51 (n (%))
CIPN
31 (61)
Chemotherapy
Oxaliplatin
21 (41)
Paclitaxel
2 (4)
Taxotere
1(2)
Bortezomib
2 (4)
Cisplatin
4(8)
Carboplatin
1(2)
Median months since last dose (IQ range)
11 (8 to 24)
Neuropathic scar pain
10 (20)
Neuropathic pain due to other causes
10 (20)
Median months of pain: all causes (IQ range)
19 (9 to 34)
Previous/current cancer diagnosis
41 (80)
Type of cancer
Colorectal
22 (43)
Multiple myeloma
2 (4)
Lung
3 (6)
Ovary
2 (4)
Breast
12 (23)
Cancer status
No recurrence
33 (65)
Local disease
6 (12)
Metastatic disease
2 (4)
IQ interquartile, CIPN chemotherapy-induced peripheral neuropathy
Forty of fifty-one patients completed 4–6 weeks of treatment. Ten patients discontinued the topical menthol treatment early for the following reasons: disliked the cream (n = 2), found cream application difficult (n = 2), developed brain metastases (n = 1), felt no benefit (n = 1), pain worsened (n = 2), (resolved to baseline levels within 2 weeks of stopping menthol) or withdrew from the trial without giving a reason (n = 2). One patient only attended at 10 weeks after baseline, so did not complete the 4–6-week assessment. Thirty-eight patients had complete evaluable outcome data. All completing patients used very similar quantities of menthol cream over the study period (1000×g, i.e. 10 g menthol).
Change in pain scores and other patient-rated outcomes
Eighty-two per cent (31/38) of evaluable patients had an improvement in their pain scores. The median total BPI improved from 47 (interquartile range, 30 to 64) to 34 (6 to 59), P < 0.001. There were also significant improvements in ‘worst pain’ and the pain interference subscales (Table 2). The mean total BPI decrease was 11 (SD 16). Fifty per cent (19/38) were responders, with 11 % (4/38) having complete pain relief. All the statistically significant improvements in pain were also clinically significant [21]. Along with the improvement in pain scores, there were also statistically significant improvements in HADS total score, HADS anxiety score and catastrophising (Table 2). The LANSS scores, as expected, did not demonstrate any significant treatment effect. Patients who were taking other regular pain medication remained on the same dose throughout the 6 weeks.
Table 2
Comparison of measures at baseline and after 4–6 weeks of menthol
Measure (possible score)
Number
Baseline median (IQ range)
4–6 weeks median (IQ range)
Mean/median of individual changesb (95 % CI)
P value
Brief Pain Inventorya
Total BPI (0 to 110)
38
47 (30 to 64)
34 (6 to 59)
−11 (−16.1 to −5.5)
<0.001
Worst pain item (0 to 10)
39
6 (4 to 7)
3 (1 to 7)
−1.3 (−2.1 to −0.6)
0.001
Total interference (0 to 70)
38
32 (17 to 43)
24 (3 to 37)
−6.3 (−10.2 to −2.5)
0.002
HADSa
Depression (0 to 21)
38
4 (2 to 7)
4 (1 to 6)
0b (−1.6 to 0.1)
0.168c
Anxiety (0 to 21)
38
7.5 (4 to 9)
5 (2 to 8)
−1.7 (−2.6 to −0.8)
0.001
Total (0 to 42)
38
12 (6 to 16)
9 (5 to 13)
−2.5 (−4.1 to −0.8)
0.004
PCSa (0 to 65)
37
13 (9 to 19)
10 (2 to 17)
−4.5 (−7.0 to 2.0)
0.001
LANSSa (0 to 24)
40
14 (11 to 19)
13 (8 to 19)
−1.1 (−2.6 to 0.4)
0.160
Peg boarda
Dominant hand (s)
15
98 (79 to 147)
85 (77 to 103)
−10.8 (−34 to 12.5)
0.337
Nondominant hand (s)
15
95 (92 to 147)
92 (76 to 102)
−13.5 (−34.7 to 7.7)
0.195
GAITRite
Velocity (metres/s)
21
79 (68 to 106)
93 (79 to 113)
12.1 (3.6 to 20.6)
0.008
Cadence (steps/min)
21
100 (89 to 110)
105 (96 to 113)
6.0 (0.8 to 11.2)
0.027
BPI Brief Pain Inventory, HADS Hospital Anxiety and Depression scale, LANSS Leeds Assessment of Neuropathic Symptoms and Signs, PCS Pain Catastrophising scale 95 % CI 95 % confidence interval, IQ range interquartile range
aHigher scores indicate more severe symptoms
bMedian change (when distribution of variables relating to the change between baseline and 4–6 weeks was not normally distributed)
cException—compared using paired t test when Wilcoxon signed rank test used
Change in quantitative sensory testing (QST), objectively measured walking ability and hand dexterity
As well as an improvement in subjectively rated pain, there was also an improvement in objectively measured physical function and some QST parameters. Both walking velocity and cadence improved over the treatment period, although there was no significant improvement in hand dexterity (Table 2). QST showed a decrease in the mechanical detection threshold (became less numb), and for the CIPN patients, the percentage of the distal limb skin which had abnormal sensation in response to brush, cool and warm stimuli decreased and moved distally (Table 3; Fig. 1).
Table 3
Quantitative sensory testing (QST) and proportion of distal limbs with abnormal sensation to brush, cool and warm stimuli at baseline and 4–6 weeks
Measure (possible score)
Number
Baseline median (IQ range)
4–6 weeks median (IQ range)
Median of individual changesa (95 % CI)
P value
QST
Mechanical detection threshold forcec (0.026 to 110 g)
40
1.1 (0.3 to 2.9)
0.3 (0.1 to 1.1)
−0.2a (−7.9 to 1.7)
0.016b
Mechanical detection threshold NRS (0 to 10)
40
0 (0.0 to 0.0)
0 (0.0 to 0.0)
0.0a (−0.3 to 0.0)
0.131b
Mechanical pain threshold forced (0.026 to 110 g)
40
34 (11 to 110)
110 (17 to 110)
0.0a (−7.4 to 31.9)
0.198b
Mechanical pain threshold NRS (0 to 10)
39
2 (0 to 4)
1 (0 to 3)
−0.4 (−1.3 to 0.6)
0.445
Windup ratio
40
1 (0.0 to 2.0)
1 (0.0 to1.3)
0.0a (−2.0 to 0.2)
0.098b
Extent of abnormal receptive field
Brush stimulus
% of forearm below elbow
20
55 (2 to 73)
24 (0 to 57)
−16 (−32 to 1)
0.062
% of lower leg below knee
19
65 (16 to 82)
39 (16 to 64)
−13 (−26 to 0)
0.056
Cool (25 °C) stimulus
% of forearm below elbow
19
70 (34 to 88)
37 (9 to 79)
−19 (−37 to −2)
0.036
% of lower leg below knee
19
67 (48 to 97)
43 (21 to 79)
−24 (−36 to 12)
0.001
Warm (40 °C) stimulus
% of forearm below elbow
18
72 (50 to 88)
24 (8 to 79)
−28a (−39 to −11)
0.004b
% of lower leg below knee
19
89 (78 to 93)
56 (20 to 77)
−25 (−41 to −10)
0.003
NRS Numerical Rating Scale (higher scores indicate worse pain), 95 % CI 95 % confidence interval, IQ range interquartile range
aMedian change (when distribution of variables relating to the change between baseline and 4–6 weeks was not normally distributed)
bException—compared using paired t test when Wilcoxon signed rank test used
cHigher values indicate the skin is more numb
dLower values indicate increased sensitivity to painful stimuli
×
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Comparison of responders and non responders at 4–6 weeks
Responders had a significantly greater degree of improvement than nonresponders in catastrophising and dominant hand dexterity but not on other variables (Table 4).
Table 4
Comparison of the mean difference (change) between baseline and 6 weeks for responders and nonresponders (statistically significant P values are set in bold)
4–6 weeks measure
Nonresponder (n = 19)
Responder (n = 19)
P valuea
Mean difference (SD) or median (IQ range)
Mean difference (SD) or median (IQ range)
n
n
Clinical assessments
HADS
Total
18
−2.1 (4.1)
19
−3.0 (5.7)
0.589
Depression
18
−0.4 (2.2)
19
−1.1 (3.1)
0.459
Anxiety
18
−1.6 (2.4)
19
−1.8 (3.2)
0.807
PCS
17
−1.2 (7.5)
19
−8.1 (5.8)
0.004
LANSS (total)
19
−0.2 (4.3)
19
−2.4 (4.5)
0.129
Peg board (s)
Dominant hand
5
19 (41)
10
−25.7 (35.4)
0.048
Nondominant hand
5
6.8 (39.5)
10
−23.6 (35.2)
0.153
GAITRite
Velocity (m/s)
8
8.3 (22.9)
12
13.8 (16.8)
0.536
Cadence (steps/min)
8
2.3 (11.9)
12
7.8 (11.4)
0.310
QST
Mechanical detection threshold (g)
19
−0.24 (−3.4 to 0.26)
19
−0.26 (−0.78 to 0)
0.563a
Mechanical detection threshold NRS
19
0.0 (0.0 to 0.0)
19
0.0 (0.0 to 0.0)
0.418a
Mechanical pain threshold (g)
19
0.0 (−5 to 17)
19
0.0 (−16 to 86)
0.863a
Mechanical pain threshold NRS
19
−0.2 (3.5)
18
0.5 (2.0)
0.742
Windup ratio
19
0.0 (−2.0 to 0.63)
19
0.0 (−2.0 to 0.5)
0.729a
HADS Hospital Anxiety and Depression scale, LANSS Leeds Assessment of Neuropathic Symptoms and Signs, PCS Pain Catastrophising Scale, NRS Numerial Rating Scale, 95 % CI 95 % confidence interval, IQ range interquartile range
aException—all compared using two-sample t test where Mann–Whitney U test used
Discussion
Main finding
This is, to our knowledge, the first clinical study to report an analgesic benefit from the application of topical menthol to treat CIPN and Post-mastectomy Pain Syndrome (PMPS). Eighty-two per cent of evaluable patients had an improvement in their total pain scores after 4–6 weeks of treatment. Fifty per cent had a clinically relevant reduction in pain scores of at least 30 %.
Importantly, there were also improvements in objectively measured physical function. The significant increase in walking velocity and cadence are important read-outs of increased function. Such objective improvements in function increase the likelihood that we are seeing a genuine response to treatment. In addition, QST showed a shrinkage of the skin area with abnormal sensation to several different stimuli (warm, cool and mechanical). The associated changes in mechanical detection threshold and response to warm and cold between baseline and study endpoint again reinforce the evidence for an objective improvement in pain as the key outcome of this study.
Comparison with other studies
Cooling of injured areas by for example, cold compresses/icepacks or application of menthol for pain relief has a long history in medicine. The analgesic effect of menthol was reported in 1870 by Wright et al. [36], and its beneficial properties were known to the Ancient Greeks. More recent case reports demonstrated potential increased efficacy for neuropathic pain. While the mechanism of these traditional treatments has long been obscure, our recent demonstration that TRPM8 activation acts through central inhibition of nociceptive input provides a scientific rationale for a new generation of analgesics targeting TRPM8 [22]. In fact, several members of the TRP super family have emerged as important targets for new drugs, especially analgesics, due to their expression in sensory neurons and their critical role in nociception, particularly in chronic pain states [37, 38].
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The effective use of menthol depends on the understanding that at higher doses of menthol, there may be off-target effects as it is known to interact with other potentially nociceptive TRP channels and voltage-sensitive channels [39, 40]. Very high concentrations of topically applied menthol (40 %) are overtly noxious and have been used to produce clinical pain models [41], but there are likely to be numerous nonspecific actions at this level.
In this study of topical menthol as an anti-neuropathic agent, the effect was rapid with no dose titration required, which, combined with no apparent side effects, is a clear potential advantage over other neuropathic agents [19].
This work adds significantly to the increasing body of evidence for the efficacy and safety of menthol and peppermint oil as an analgesic in diverse pain states such as muscle strain, migraine, irritable bowel syndrome, post-herpetic neuralgia and CIPN [23, 24, 41‐44] and true responders. Despite this, not only did patient show a significant improvement in pain relief, but this was supported by objective clinical biomarker methodology and adherence to the IMMPACT recommendations [25].
1.
Patients were recruited from one specialist cancer centre and findings may not apply to similar patients treated elsewhere
2.
It is possible that some patients may have had a spontaneous improvement in pain and function. However, this is unlikely to have happened in the 6-week study timescale in this patient group, who all had stable, established chronic pain of at least 6 months duration.
The underlying neuropathic pain aetiology varied, however there is accumulating evidence that aetiology is not the driving factor in a treatment response, rather it is the neurobiological changes in any individual, as characterised by QST, which will determine response [45]. These characteristics were examined in detail in this study, using QST. The resolving numbness along with normalisation of response to brush, cold and warm, all moving in synchrony with resolving pain compared with baseline, were important neurosensory biomarkers of response. In this patient sample, it was not possible to identify neurosensory predictors of response: this should be explored in future studies.
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It is important when investigating new treatments to examine in detail the characteristics of those who respond versus those who do not respond. Analgesic studies are often dismissed as negative, when in fact there is an important group of responders hidden in the final result. It is accepted that not all patients will respond to a treatment, no matter how promising that treatment. It is crucial however that relevant biomarker data are used to further identify and understand the characteristics of a response. This approach makes identification of responders more scientifically robust and acceptable. In a randomised controlled trial of menthol, both study assessments and a responder analysis will be facilitated by continuing the biomarker work established in this proof of concept study.
Implications for practice
Chronic established neuropathic pain is particularly difficult to treat and represents a largely unmet therapeutic need. Although progress has been made in curing and prolonging life in patients with cancer, there are a number of long-term treatment-related problems (such as CIPN and PMPS) which can limit further palliative chemotherapeutic options or impact significantly on the patient's quality of life despite being cured of cancer.
The discovery of the TRP channels has provided an opportunity for the development of analgesics, which are potentially more specific for certain pain syndromes and have a better side-effect profile than other interventions. TRP channels are being investigated as novel targets for drug discovery; they have a major advantage over more widely distributed voltage-sensitive ion channels, in their potential for achieving analgesia without overwhelming side effects in neuropathic pain [38]. This translational work with topical menthol, a TRPM8 agonist, shows significant promise, and points to the need for further validation through a phase 2 double-blind efficacy study.
If this preliminary work translates into positive further phase 2/3 studies, then it could have a significant impact on quality of life of both many patients being treated for cancer and survivors of cancer.
Acknowledgments
CJW was supported in this work by NHS Lothian through the Health Services Research Unit, Edinburgh.
Conflict of interest
None
Open Access This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and the source are credited.
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