Interventional Techniques for Cancer Pain Management
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1 Interventional Techniques for Cancer Pain Management Musa M. Aner, MD Director, Cancer Pain Service Arnold - Warfield Pain Center Beth Israel Deaconess Medical Center Boston, MA
2 Disclosure No financial or industry relationships to disclose. Off-label use of drugs will be discussed.
3 Objectives Evaluation of pain in cancer patients Review the indications of interventional pain techniques in cancer patients Discuss different modalities of interventional pain management
4 Incidence of Cancer Pain Up to 70% of patients with advanced cancer report pain: Tumor related (67%) - Direct invasion of the tumor into nerves, bones, soft tissue, ligaments, and fascia Treatment related (23%) - Surgery related - Radiation related bone necrosis, myelopathy and plexopathies - Chemotherapy related mucositis, peripheral neuropathies, and aseptic bone necrosis Unrelated to cancer (10%)
5 Types of Pain Neuropathic pain Described as burning, shooting, electric-like Results from damage or altered function of a nerve Caused by tumor invasion to any areas of the nerves Brachial plexus invasion due to breast cancer Tumor compression of nerves/spinal cord Nociceptive / Visceral pain Described as a dull ache, throbbing or sharp pain Transmitted by nociceptors responsive to high-intensity mechanical, thermal, and chemical stimuli Tumor expansion inside viscera, soft tissue or bone Frequently occurs with metastasis to the bone common progression of breast, prostate and lung cancers
6 Cancer Pain Prevalent and multifactorial Severe and chronic in 67% of patients with advanced disease 46% of dying patients are inadequately treated for their pain, as reported by family members. Close to 80% of cancer patients in pain are well managed by the 3-Step Ladder Model 15-20% of patients with inadequate pain control 2014 Review by Greco at al- Moderate improvement Bruera, E. et al. Opioid rotation in patients with cancer pain. A retrospective comparison of dose ratios between methadone, hydromorphone, and morphine. Cancer 1996,78: Greco et al. Quality of Cancer Pain Management: An Update of a Systematic Review of Undertreatment of Patients with Cancer. Journal of Clinical Oncology 2014, 32:36;
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8 4th Step- Beyond (/Along) WHO Ladder Neuroaxial Techniques - Epidural / Intrathecal Infusion Therapy Neurolytic Techniques - Chemical - Cryoablation - Radiofrequency Neuromodulation Techniques - Spinal Cord and Peripheral Nerve Stimulation Vertebroplasty / Kyphoplasty Lamer, T. Treatment of Cancer-Related Pain: When Orally Administered Medications Fail. Mayo Clinic Proceedings, 1994,69:
9 Indications Intractable pain despite high doses of opioids with adjuvants Persistent pain Mixed Neuropathic/ Nociceptive nature Refractory after opioid rotation (minimum 2 different opioids) Opioid induced hyperalgesia Pain amenable to interventional therapy Anatomical and clinical correlation Uncontrolled side effects due to high dose systemic opioid therapy Fatigue - More prevalent than pain in patients with metastatic cancer Depressed level of consciousness/ Sedation - Dose-limiting problems Constipation/ Nausea Delirium/ Confusion Respiratory depression
10 Contraindications Coagulopathy INR >1.3 Thrombocytopenia < 100K (?) Sepsis Infection at injection/procedure site Tumor invasion at injection/procedure site Skin breakdown at injection/procedure site Patient refusal Poor access to treatment
11 Neuroaxial Techniques Advantages: Targeted therapy- NMDA & opioid reseptors, Ca +2 channels Decreased systemic medication Decreased toxicity Disadvantages: Invasive Risk for complications Specialized treatments Rauck RL et al. Long-term intrathecal opioid therapy with a patient activated, implanted delivery system for the treatment of cancer pain. J Pain 2003; 4:
12 Neuroaxial Techniques Reduced Dose : Pain control with reduced side effects 300 mg oral morphine: 10 mg epidural morphine 300 mg oral morphine: 1 mg intrathecal morphine
13 Intrathecal Drugs Morphine Action site: Substantia gelatinosa Dorsal Horn Dose dependent analgesia- mu receptor The ONLY opioid approved by the FDA for IT use Effective in nociceptive pain Adverse effects Somnolence, weight gain, nightmares, vomiting, itching, constipation, respiratory depression, decreased libido Granuloma formation mg/day
14 Intrathecal Drugs Hydromorphone Semisynthetic hydrogenated ketone of morphine More potent and faster-acting due to greater lipophilic properties Mu receptor (primary), delta and k-opioid receptors Smaller spinal distribution than Morphine- Less SE Granuloma formation Equianalgesic dose: 20% of IT Morphine dose Effective in nociceptive pain Johansen MJ et al. Pain Med 2004,5:14-25.
15 Intrathecal Drugs Bupivacaine Improvement in quality of pain relief Synergism to opioids Effective at the site of the catheter tip Nociceptive and neuropathic pain Stable with Morphine+Clonidine or Hydromorphone+Clonidine for 90 days at 37 C
16 Intrathecal Drugs Clonidine Selective alpha-2-adrenergic agonist Lipophilic Approved by the FDA for epidural use Dose-dependent anti-hypersensitivity to mechanical stimuli in a rat model of neuropathic pain Stable with Hydromorphone SE: Reduced MAP & HR
17 Intrathecal Drugs Ziconotide (SNX-111) A non-opioid analgesic and a voltage sensitive, N-type Calcium channel blocker Potent synthetic neuroactive peptide isolated from the venom of a marine snail SE: Elevated creatine kinase levels, sedation, somnolence, nausea, headache, neuropsychiatric symptoms, ataxia, gait disturbance, double vision Neuropathic agent Staats et al. Intrathecal ziconotide in the treatment of refractory pain in patients with cancer or AIDS. JAMA 2004;291:63-70.
18 Intrathecal Drugs Line 1 Morphine/ Hydromorphone/ Ziconotide/ Fentanyl Line 2 Morphine/ Hydromorphone/ Fentanyl + Bupivacaine Morphine/Hydromorphone/ Fentanyl + Ziconotide Line 3 Opioid + Clonidine Deer et al. Polyanalgesic Consensus Conference (PACC) 2017: Recommendations for Intrathecal Drug Delivery: Guidance for Improving Safety and Mitigating Risks. Neuromodulation 2017; 20:
19 Implantable Drug Delivery Systems (IDDS) Hockey-puck sized Attached to a catheter Programmable Reservoir 20 or 40 ml Internalized Low maintenance Costly, yet cost effective
20 Efficacy of IDDS Cancer Pain Trial 2002 by Smith TJ et al. Clinical trial of efficacy of Intrathecal Drug Delivery System (IDDS) plus comprehensive medical management (CMM) vs. CMM alone for patients with refractory cancer pain Randomized Prospective International (5 countries) Multi-center (21 centers) Smith TJ et al. Randomized clinical trial of an implantable drug delivery system compared with comprehensive medical management for refractory cancer pain: impact on pain, drug-related toxicity, and survival. J. Clin. Oncol & 2005.
21 At the end of 4 weeks: Efficacy of IDDS CMM+IDDS group reported: Significant decrease in fatigue Elevated level of consciousness Pain reduction (VAS) 39.1% for CMM, 51.5% for IDDS Toxicity 17.1% for CMM, 50.3% for IDDS (p=0.004) At 6 months: (incidental finding) 54% of IDDS patients alive versus 37% of CMM patients
22 Outcomes Improved clinical success Reduced pain scores Relieved most toxicity of pain control drugs Increased survival for duration of 6 month trial Pain control =? Increased survival
23 Neurolysis Intentional injury to a nerve or group of nerves Chemical (alcohol or phenol) Thermal (heat- radiofrequency) Surgical Cryogenic (freezing) Predominantly neuronal axonal damage; cell body is preserved
24 Chemical Neurolysis Pros: Targeted relief Usually single shot Cons: Effective for 3-6 months at most Risk of neuritis, neurologic deficit, damage to non-neural tissue or non-targeted neural structures Incomplete pain relief
25 Neurolytic Blockade and Corresponding Anatomic Structures Stellate Ganglion Head and neck Gasserian Ganglion Face/mouth, trigeminal distribution Thoracic sympathetic chain Upper extremities, thorax, esophagus, lungs Celiac plexus Pancreas, stomach, transverse colon Lumbar sympathetic chain Lower extremities, ureters, kidneys, testes Hypogastric plexus Uterus, ovaries, bladder, prostate, descending and sigmoid colon Ganglion impar Perineum, rectum,anus, vagina, urethra, vulva
26 Agents PHENOL Clear/ colorless/ pungent odor Poorly soluble in water/ viscous Unstable at room temperature Hyperbaric relative to CSF 6-10% Low cost Neurolytic and local anesthetic properties Neuritis (uncommon), toxic in high concentrations Epidural, paravertebral, peripheral nerves, intrathecal, cranial nerves, splanchnic
27 Agents ALCOHOL Clear/ colorless Stable at room temperature Hypobaric relative to CSF % Neurolytic- Inflammation and arterial vasospasm Expensive Neuritis (common), toxic in normal concentrations Intrathecal, celiac ganglion, lumbar sympathetic chain, cranial nerves, paravertebral, epidural
28 Chest Wall Pain and Neurolysis Pain Med Apr;16(4): A retrospective review and treatment paradigm of interventional therapies for patients suffering from intractable thoracic chest wall pain in the oncologic population. Gulati A, Shah R, Puttanniah V, Hung JC, Malhotra V. Discussion: Intercostal nerve diagnostic blockade with local anesthetic and steroid may lead to prolonged pain relief in this population. Furthermore, depending on tumor location, we have developed a paradigm for the treatment of thoracic chest wall pain in the oncologic population.
29 Chest Wall Pain and Neurolysis
30 Chest Wall Pain and Neurolysis J Pain Res Nov 19;7: Paraplegia after intercostal neurolysis with phenol. Gollapalli L, Muppuri R. 66-year-old female with metastatic adenoid cystic carcinoma of the left submandibular gland and developed paraplegia following intercostal neurolysis with phenol. After a successful diagnostic T6 to T12 intercostal nerve block, the patient was scheduled for an intercostal neurolytic block. We injected 2 ml of 10% aqueous phenol at each level on the left from the T6 to T12 ribs. One hour after the procedure, the patient developed bilateral lower extremity weakness with difficulty moving.
31 Celiac Plexus Block and Neurolysis First described by Kappis in 1919 One of the most useful and effective neurolytic blocks Pancreatic, primary intra-abdominal and hepatic metastatic tumors Network of neuronal ganglia under the diaphragmatic crus in the retroperitoneal space, anterolateral to the aorta Greater, lesser and least splanchnic nerves (sympathetic rami from T5-T12) and superior mesenteric ganglion
32 Celiac Plexus Block and Neurolysis Anatomy Sympathetic fibers from the splanchnic nerves, vagal parasympathetic fibers and visceral afferent fibers Function Nociceptive transmission innervating the pancreas, liver, gallbladder, stomach, spleen, kidneys, intestines and adrenals
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34 Celiac Plexus Block and Neurolysis Percutaneous Techniques (need fluoroscopic or CT guidance) Transcrural Approach Two needle Retrocrural Approach Two needle splanchnic Transaortic Approach Single needle through the aorta Anterior Approach Single needle w/ CT or US guidance Endoscopic US Guided Technique
35 Celiac Plexus Block and Neurolysis Complications: Hypotension - transient Diarrhea - transient Hematuria from renal injury Pain at the site of injection Pneumothorax Impotence Paraplegia (1%) - Ischemia of anterior spinal cord due to vasospasm or mechanical injury to the Artery of Adamkiewicz
36 Celiac Plexus Block and Neurolysis Efficacy: RCT of 24 patients show decreased use of analgesics in the group that received NCPB A meta-analysis of NCPB for pancreatic and other intraabdominal cancer pain demonstrates 90% of the patients reported partial to complete relief at 3 months, while 70-90% patients had partial to complete relief at the time of death Moore JC, Adler DG. Celiac Plexus Neurolysis for Pain Relief in Pancreatic Cancer. The Journal of Supportive Oncology 2009, 7:3,
37 Celiac Plexus Block and Neurolysis Clin J Pain Sep;29(9): Comparative study between 2 protocols for management of severe pain in patients with unresectable pancreatic cancer: one-year follow-up. Amr YM, Makharita MY. Conclusion: Controlling severe pain with medication and then performing the celiac block seems to be more effective in controlling pain, reducing opioid consumption, and improving the quality of life of patients with pancreatic cancer compared with performing the celiac block at the beginning followed by pharmacotherapy for pain relief.
38 Celiac Plexus Block and Neurolysis Cochrane Database Syst Rev Mar 16;(3):CD Celiac plexus block for pancreatic cancer pain in adults. Arcidiacono PG, Calori G, Carrara S, McNicol ED, Testoni PA. Conclusion: Although statistical evidence is minimal for the superiority of pain relief over analgesic therapy, the fact that CPB causes fewer adverse effects than opioids is important for patients. Further studies and RCTs are recommended to demonstrate the potential efficacy of a less invasive technique under EUS guidance.
39 Celiac Plexus Block and Neurolysis Pain Med Aug;14(8): Celiac plexus neurolysis for abdominal cancer pain: a systematic review. Nagels W, Pease N, Bekkering G, Cools F, Dobbels P. Conclusion: Following this review, evidence suggests that CPN should be considered in patients with upper abdominal cancer where the pain is not adequately controlled with systemic analgesics or when significant opioid-induced side effects are present. The percutaneous approach remains the standard technique as robust evidence for EUS CPN is lacking.
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42 Splanchnic Nerve RFL Bilateral Thoracic Splanchnic Nerve Radiofrequency Thermocoagulation for the Management of End-Stage Pancreatic Abdominal Cancer Pain Papadopoulos et al. Pain Physician 2013; 16: Retrospective study of 35 patients at the end of life followed for 6 months Sustained pain relief from 8.9/10 to 3-4/10 Improved QOL and decreased opioid consumption
43 Anatomy Superior Hypogastric Block and Neurolysis The sympathetic trunk from T10-L2 and the parasympathetic fibers from S2-S4 create neuronal network at the anterior projection of the sacral promontorium at L5-S1 level Located retroperitoneally in the subserous fascia of the common iliac bifurcation Function Sensory information from the bladder, rectum, prostate, testes, vagina, uterus, ovaries and descending and sigmoid colon
44 Superior Hypogastric Block and Neurolysis Percutaneous techniques: Initially described by Plancarte in 1990 for the treatment of pelvic cancer pain Requires fluoroscopic or CT guidance Posterior Approach: Two needle technique Transdiscal Approach: Through L5-S1 disc space Anterior Approach: Single needle technique
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47 Superior Hypogastric Block and Neurolysis Complications: Hypotension Pain at injection tract Bladder puncture Retroperitoneal hematoma L5- S1 nerve root injury Discitis (1-4%)
48 Efficacy: Superior Hypogastric Block and A trial of 227 patients Neurolysis 72% reported effective pain relief with reduction of opioid consumption At 6 months, 69% had continued pain relief Plancarte, R. Et al. Neurolytic superior hypogastric plexus block for chronic pelvic pain associated with cancer. Reg. Anesth. 1997, 22: Only one RCT comparing opioid therapy with neurolytic SHP found decreased pain intensity, opioid consumption and increased quality of life de Oliveira, R. et al. The effects of early or late neurolytic sympathetic plexus block on the management of abdominal or pelvic cancer pain. Pain 2004, 110:
49 Ganglion Impar Block and Neurolysis First described by Plancarte in 1990 for the treatment of intractable perineal pain Primary indications are perineal pain due to anal or rectal cancer Anatomy: Located anterior to the lower portion of the first coccygeal body Termination of the paravertebral sympathetic chains
50 Function: Ganglion Impar Block and Neurolysis Contains visceral afferent fibers that innervate the perineum, distal part of the rectum, anus, distal urethra, distal third of the vagina and vulva Techniques: Anococcygeal Approach Trans-Sacrococcygeal Approach Intercoccygeal Approach Coccygeal Transverse Approach
51 Ganglion Impar Block and Neurolysis Complications: Rectal perforation Sacral nerve root injury Epidural injection Bowel or bladder dysfunction Efficacy: Two prospective studies with good efficacy One study using RF lesioning with 50% decrease in pain scores
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53 Conclusion The need and responsibility to treat pain Communication between disciplines to establish treatment goals and life expectancy Risk / Benefit ratio Patient preference Vigilance Multimodal therapy
54 To cure sometimes, to relieve often, to comfort always
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