Gli oppioidi sono indicati nel dolore neuropatico? NO
Marco Lacerenza Medicina del Dolore
Fondazione “Opera San Camillo”Casa di Cura S. Pio X, Milano
Palermo, 29-30 novembre 2012, Reale Albergo delle Povere
“Controversie sulla diagnosi e terapia del dolore neuropatico”
Opinioni a confronto
O meglio….ATTENZIONE!
RCT, Linee Guida…………..artefatti della medicina moderna che danno DATI UTILISSIMI MA………….
Possono subire le influenze di forze non utili al nostro finePossono facilitare le generalizzazionipossono facilitare la medicina della INDICAZIONE senza valutazione sedano l’ansia del giovane medico e accorciano le visite dell’espertoProteggono dal pdv medico legaleSmettiamola di parlare di “Dolore Neuropatico”Parliamo di Pazienti SOFFERENTI, con dolore spesso
neuropatico, cronico, complessi, con molte comorbiditàOgnuno diverso dall’altro, con scarsa QoL e problemi
famigliari, lavorativi, economici
Premessa
Sumeri: IX secolo AC: oppio la pianta della gioia
Omero, IV libro Odissea :….“Nel dolce Vino, di cui bevean, farmaco infuse contrario al pianto e all'ira, e che l'obblìo seco inducea d'ogni travaglio e cura”.
“Tra i rimedi che Dio Onnipotente ha
voluto, bontà Sua, dare all’uomo per alleviare
le sue sofferenze, nessuno è universale
ed efficace come l’oppio.”
Thomas Sydenham, 1624-1689GaspareTraversi 1753
Dolore - Sofferenza
OPIOID RECEPTORSROLES IN VIVO
Distinct roles in hedonic homeostasis and
emotional control
Mu
KappaDelta
Reward
Low
High
Mood Low High
Individuals with high reward responsiveness, a personality trait dependent on the endogenous opioid neurotransmission, experience
more exogenous opioid-induced behavioral analgesia.Emerging evidence suggests that MOR polymorphism could contribute to variability in behavioral opioid analgesia by introducing variability of
the MOR responsiveness to exogenous opioids.It is possible that trait RWR and the neuronal response to noxious stimuli
in the endogenous opioid-rich brain reward circuitry could be useful endophenotypes of behavioral opioid analgesia.
Localizzazione dei recettori per gli oppioidi
Corteccia cingolata anteriore, C.prefrontale, strati superficiali della corteccia cerebrale Nuclei della base, talamo, amigdala,
PAG, RMN, reticolare del troncoCorno posteriore midollare: – proiezioni midollari afferenti
primari– Interneuroni midollari
Periferia: nocicettori e afferenti viscerali
Oppioidi: Meccanismi d’azione
DRG
DNIC
Modificata da: A.H.Dickenson, 2000Fuoriuscita di ioni K+
Legame Presinaptico
Recettori oppioidi
Legame postsinaptico
Blocco ingresso ioni Ca++
Fuoriuscita di ioni K+
I recettori per gli oppioidi
I recettori per gli oppioidi: binding
Nerve-injury neuropathy and Diabetic Neuropathy:Functional downregulation and/or desensitization
of μ-opioid receptors in the dorsal horn of the spinal cord (but not a significant decrease in number)
may be related to increased production of PKC .
May be due to: activation of NMDARs in postsynaptic cells, to an autophosphorylation of the TrkB receptor by BDNF.In fact, the development of the hyperalgesia and allodynia in NP states is suppressed by administration of NMDA receptor antagonists, TrkB/Fc chimera protein (sequesters endogenous BDNF) PKC inhibitors.
Perché funzionano poco????
Dolore Neuropatico: Meccanismi che portano alla desensitizzazione di
MORs
Ridotta efficacia nella pratica clinica
Genetic mechanismsSensitiz. of primary afferent N.Central Glutamatergic systemDescending facilitation (in
RVM on-cells and CCK) leading to up-regulation of Spinal dynorphin and enhanced primary afferent neurotransmitter release (CGRP) and pain.
Decreased reuptake of neurotransmitters from the primary afferent fibers
NMDA receptors become activated and when inhibited, prevent the development of toleranceand OIH The glutamate transporter system is inhibited,(increasing the amount of glutamate available to NMDAR) Ca regulated intracellular PKC is likely a link between cellular mechanisms of tolerance and OIH Prolonged morphine administration induces neurotoxicity via NMDA receptor mediated apoptotic cell death in the dorsal horn
Pain that has become more diffuse and less defined in quality and has a wider spatial
distribution than the pre-existing pain.
Smith HS, 2012
Il risveglio americano dall’oppiofobia
“Opioid maintenance therapy can be a safe salutary and more humane alternative…..in those patients with intractable non-malignant
pain and non history of drug abuse”
The dichotomous classification of nociceptive and neuropathic pain is not yet fully recognized in the pain
literature or among physicians dealing with pain.
The reason ………..is unknown.
..comon narcotic analgesics, administered in a double-blind fashion and in doses which effectively control acute and
chronic nociceptive pain, are inefficient for relief of neuropathic (including deafferentation) pain…..
Short-term studies: equivocal evidence regarding the efficacy of opioids in neuropathic pain. Intermediate-term studies demonstrated significant efficacy of opioids over placebo for neuropathic pain. The difference in outcomes does not support the use of short-term opioid administration as a predictive tool to decide whether to initiate intermediate-term opioid therapy. …the participants in the included studies may not reflect those commonly seen in practice. Therefore, issues such as abuse of medication, or conversely, non-compliance due to participants’ unwillingness to tolerate side effects may not be accurately reflected in our results.
Opioids for neuropathic pain (Review), 2009Eisenberg E, McNicol ED, Carr DB
Studi epidemiologici documentano nel LBP dolore misto nel 20-35% dei casi
1/3 della popolazione ha LBP, quindi il 6% ha una componente neuropatica
Il costo dei pazienti con LBP e componente neuropatica è il 70% > rispetto a LBP nocicettivo
The meta-analysis of Martell et al. 2007 identifies also a number of relevant issues:
patients were more likely to be prescribed opioids if they reported greater distress and suffering. The prevalence of substance abuse disorders was in the range of 40% to 50% in these patients and up to 24% showed aberrant medication-taking behaviour
Long-term trials of opioid efficacy for chronic back pain are lacking, and there is other evidence that indicates that the long-term efficacy of opioids for chronic pain may be limited
Opioids and opioid combinations were exceeding NSAIDs in proportion of patients and number of prescriptions.Short-acting opioids are frequently used as rescue medication…. high prescribing..(36.5%). Although the frequency of use of long-acting opioids was low (3.8%), the median (7.0) number of prescriptions were higher than for any other medication.
Opioids continue to be recommended and used, despite evidence of a negative association with outcomes in CLBP, including function and productivity and an increased likelihood of substance use disorders.
In such “pathological pain states”, nociception is not the sole target, but also suffering, dysfunction, mood states, psychosocial factors and dependence on the health system. Then opioid use is less likely to improve analgesia and even less to yield psychological or functional improvement.
Several investigations have identified drug abuse in 18%to 41% of patients receiving opioids for chronic pain.36-40 The prevalence of lifetime substance use disorders range from 36% to 56%, with an estimate of 43% current substance use disorders and 5% to 24% of the patients with aberrant medication taking behaviours.
Storia di abuso di sostanzeDisturbi mentaliStoria di dolori multipliGenere maschileGiovani adultiPrescrizioni di > 90gg
Fattori di Rischio per l’Abuso e la Dipendenza
ATTENZIONE
Programma multidisciplinareValutazione dolore, QoL, funzionamentoSupporto psicologico-occupazionaleEducativo-motivazionaleFisioterapico
ContrattoSpiegazioni esaustive dei rischiA breve e lungo termine
Unintentional overdose death related to an opioid analgesic
9 persons are admitted for
substance abuse treatment
35 visit ER
161 report drug abuse or dependence
461 report nonmedical uses of opioid analgesics
It has been shown that from 1997 through 2007, there was a seven fold increase in the number of prescriptions for opioids. The pharmaceutical industry aggressively marketed long-acting opioids for chronic pain relying on 2 erroneous facts:That medical management with opioids is the recommended solution for undertreated chronic painThat the use of long-acting formulations decreases incidences of prescription opioid abuse. The principles of opioid management in acute pain and cancer pain were transferred to the chronic pain arena.JAMA 2000, 283: 1710-1714: ”Increased opioid use is not associated with deleterious health consequences”.
Approximately two-thirds of the panel responsible for writing guidelines for the use of opioids for chronic pain for the American Academy of Pain Medicine (AAPM) and American Pain Society (APS) had conflicts of interest with the opioid pharmaceutical industry.
The investigation announced by the Senate in reference to conflicts of interest in preparation of opioid guidelines and promotion of opioid usage,
have resulted in abandonment of the American Pain Foundation on May 10, 2012, which was a pivotal
organization in promoting opioid use.
Dipendenza fisicaSviluppo di tolleranzaIperalgesia indotta da oppioidiAbuso e Dipendenza Deficit cognitiviIpogonadismo (Disfunzioni sessuali, osteoporosi, depressione, fatica)
Alterazioni del sistema immunitario (attraverso il sistema ipotalamo-ipofisi-surrene)
riduce la produzione di anticorpiriduce l’attività delle cellule Natural Killerriduce l’espressione di citochineriduce l’attività fagocitaria
Rischi del trattamento con oppioidi nel lungo termine:
Opioid use for the management of pain in fibromyalgia is strongly discouraged and is not recommended by any current guideline.
1) women could be at higher risk for the negative medical and psychological effects of opioids because they have more persistent pain than men, and may be prescribed opioids more often and at higher doses than men
2) multiple psychophysiological factors may contribute to certain risks and consequences of chronic opioid therapy
3) risks in pregnancy and breast-feeding 4) as in men, risks that are unique to women may increase
concomitantly with greater exposure to opioids (in terms of frequency and dosage)
5) as in men, risks for women appear to vary at different ages.
GRAZIE PER LA VOSTRA ATTENZIONE
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