WEO 简讯:内窥镜超声引导下腹腔神经丛介入治疗的技巧和窍门。

IF 5 2区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
{"title":"WEO 简讯:内窥镜超声引导下腹腔神经丛介入治疗的技巧和窍门。","authors":"","doi":"10.1111/den.14935","DOIUrl":null,"url":null,"abstract":"<p>WEO Newsletter Editor: Nalini M Guda MD, MASGE, AGAF, FACG, FJGES</p><p><b>Dr. Sridhar Sundaram</b></p><p><b>MD, DM, FISG</b></p><p>Present Designation:</p><p>Professor (Gastroenterology), Department of Digestive Diseases and Clinical Nutrition, Tata Memorial Hospital, Homi Bhabha National Institute, Mumbai</p><p>Consultant- GI Disease Management Group, Tata Memorial Hospital, Mumbai</p><p>Governing Council Member – Indian Society of Gastroenterology</p><p>Member – ESGE Diversity and Equity Working Group</p><p>Managing Editor – Indian Journal of Gastroenterology</p><p>Member – India EUS Club</p><p>Primary areas of interest: Therapeutic Endoscopic Ultrasound, Endoscopic Resection techniques for early GI cancer</p><p>Abdominal pain due to perineural invasion is one of the most debilitating symptoms associated with pancreaticobiliary cancers. In addition, pain remains one of the most complex symptoms associated with chronic pancreatitis needing intervention (<span>1</span>). Pain from upper abdominal viscera is transmitted via the afferent pathway to the celiac plexus leading into the spinal cord at the T12-L2 level. The efferents from the celiac plexus consists mainly of sympathetic fibres of a network of interconnected para-aortic ganglia, including those at the level of the celiac axis, superior mesenteric artery origin and also renal artery. In addition, parasympathetic efferents of the celiac plexus come from the vagus nerve (<span>2</span>). Traditionally celiac plexus block was performed as an intraoperative ablative procedure. Subsequently fluoroscopy guided celiac plexus interventions were performed. Endoscopic Ultrasound guided celiac plexus block (CPB) was first described in 1996 and has now become the standard of care (<span>3</span>).</p><p>Chronic pancreatitis patients with pain not responding to conventional measures like pancreatic enzyme replacement, antioxidants, non-narcotic and narcotic medications may be candidates who may benefit in short term from CPB. However, the caveat remains that block provides temporary relief and may be an adjunct to other modalities. Celiac plexus neurolysis (CPN) is recommended only in the setting of inoperable pancreatic cancer. In cases of operable pancreatic cancer, neurolysis may lead to scarring the operative field, thereby making surgery technically more challenging. Most patients who do not respond to conventional opioids or require significantly higher doses with adverse events are candidates to consider CPN (<span>4</span>).</p><p>CPB is typically for patients with pain not responding to analgesics and can be repeated at 3–6 months intervals. As pain becomes chronic, response to CPB is likely to be lesser, considering formation of neural feedback loops with cerebral pain conditioning. In patients with pancreatic cancer, pain responds better earlier in the course of disease to CPN. As disease progresses and pain persists, the neural pathways become less responsive and efficacy of CPN reduces (<span>5</span>). Kanno et al showed that EUS CPN does not improve Quality of life and pain compared to those medicated with newer analgesics like Oxycodone and fentanyl (<span>6</span>). Hence EUS CPN may be considered an adjunct in patients needing excessive doses of opioids or having significant adverse effects to opioids.</p><p>Background information on antiplatelets and anticoagulants is important. Aspirin may be continued; however other anticoagulants may need to be titrated. In addition, antibiotic prophylaxis pre-procedure is not recommended. Considering the sympatholytic effect of CPB/CPN leading to hypotension and diarrhea, preloading with 0.5 to 1 L of normal saline is helpful (<span>7</span>). CPB/CPN is done under sedation.</p><p>The celiac plexus is located just below the diaphragm above the origin of the celiac trunk from the aorta. The celiac ganglion is visible in 60–70% cases. Once localized, injection can be done using a 19G or 22G EUS-FNA needle into the plexus or ganglion. After puncture, suction is initially applied to make sure it is not in a vessel. For CPB, 10 ml of 0.25% Bupivacaine and Triamcinolone 40–80 mg (10–40 mg/ml) are injected into the celiac axis. For CPN, in addition to 10 ml of 0.25% Bupivacaine, 10–20 ml of absolute alcohol is also injected into the celiac plexus (<span>4</span>). Injection is known to be associated with clouding above the origin of the celiac axis. Unilateral injection means single injection above the origin of the celiac axis while bilateral injection means injection on both sides of the celiac axis. In a previous systematic review, Puli et al showed that the bilateral technique was associated with higher pain relief than the unilateral technique (84% vs 45%) for both CPB and CPN (<span>8</span>). A subsequent randomized trial by LeBlanc et al with 50 patients showed no significant difference between the unilateral and bilateral technique (69% vs 81%) (<span>9</span>).</p><p>Direct injection into the celiac ganglion was described by Levy et al. and was considered to be safe and effective for pain relief (<span>10</span>). Ascunce et al showed that ability to visualize the celiac ganglion was associated with better response to pain (<span>11</span>). Doi et al. in a randomized controlled trial of 34 patients showed that CGN was associated with higher response rate and higher complete response rate (<span>12</span>). Combination of EUS-CGN with broad plexus neurolysis was associated with higher response rate for pancreatic cancer pain as compared to broad plexus neurolysis (<span>13</span>).</p><p>In a subsequent study, Fujii-Lau et al showed that in 417 patients with pancreatic cancer pain who underwent CPN, survival was lesser in those with CGN than pancreatic cancer controls (193 vs 246 days; HR 1.32) (<span>14</span>). In another randomized trial, Levy et al showed that CPN was associated with higher survival than those who underwent CGN (10.46 months, vs 5.59 months; OR 1.49, p = 0.042), especially those with non-metastatic disease (<span>15</span>). In addition, the concern remains that since all ganglia may not be visible, CGN may have an incomplete effect.</p><p>Another variation is Broad Plexus Neurolysis (BPN) where injection is given above the level of the Superior Mesenteric artery origin leading to more diffuse injection with greater area of neurolysis (<span>16</span>). However, there is lack of large-scale studies backing this practice. It may be an alternative in situations where CPN is ineffective.</p><p>Adverse events are either sedation or procedure related. Transient hypotension due to sympatholytic effect of CPB/CPN is known. Transient diarrhea for 1–2 days is a known complication of CPB/CPN. Transient increase in pain may occur, managed well with narcotic analgesics (<span>17</span>). Rarer complications include bleeding, cardiac complications like arrhythmias, infection with retroperitoneal abscess and also diaphragmatic paralysis.</p><p>Pain relief with CPN is said to be effective in up to 70–80% patients and durable up to 24 months. Patients having metastatic disease and those with direct involvement of celiac plexus by tumor are known to respond poorly. In addition, in case of CPB, previous response to CPB indicates higher likelihood of response to repeat injection (<span>18</span>). In a previous study, heart rate change by &gt;15 beats per min sustained over &gt;30 s was said to be associated with higher response (<span>19</span>). In practice, patients having urge to defecate post-procedure and hypotension intraprocedure suggests likely effective sympatholysis and efficacious CPB/CPN.</p><p>EUS-CPB/CPN remains one of the core interventions performed by endosonologists as an adjunct to medical therapy for managing pain in chronic pancreatitis and pancreatic cancer in a safe and effective manner. While the technique is largely standardized, few variations ensure optimization based on patient and disease related factors. Newer techniques in the form of EUS guided RFA of celiac plexus can be considered in patients who fail conventional EUS CPN.</p><p>Keep in touch! The WEO events calendar</p>","PeriodicalId":159,"journal":{"name":"Digestive Endoscopy","volume":"36 10","pages":"1185-1189"},"PeriodicalIF":5.0000,"publicationDate":"2024-10-10","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://onlinelibrary.wiley.com/doi/epdf/10.1111/den.14935","citationCount":"0","resultStr":"{\"title\":\"WEO Newsletter: Tips and Tricks for Endoscopic Ultrasound guided Celiac Plexus interventions\",\"authors\":\"\",\"doi\":\"10.1111/den.14935\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p>WEO Newsletter Editor: Nalini M Guda MD, MASGE, AGAF, FACG, FJGES</p><p><b>Dr. Sridhar Sundaram</b></p><p><b>MD, DM, FISG</b></p><p>Present Designation:</p><p>Professor (Gastroenterology), Department of Digestive Diseases and Clinical Nutrition, Tata Memorial Hospital, Homi Bhabha National Institute, Mumbai</p><p>Consultant- GI Disease Management Group, Tata Memorial Hospital, Mumbai</p><p>Governing Council Member – Indian Society of Gastroenterology</p><p>Member – ESGE Diversity and Equity Working Group</p><p>Managing Editor – Indian Journal of Gastroenterology</p><p>Member – India EUS Club</p><p>Primary areas of interest: Therapeutic Endoscopic Ultrasound, Endoscopic Resection techniques for early GI cancer</p><p>Abdominal pain due to perineural invasion is one of the most debilitating symptoms associated with pancreaticobiliary cancers. 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Endoscopic Ultrasound guided celiac plexus block (CPB) was first described in 1996 and has now become the standard of care (<span>3</span>).</p><p>Chronic pancreatitis patients with pain not responding to conventional measures like pancreatic enzyme replacement, antioxidants, non-narcotic and narcotic medications may be candidates who may benefit in short term from CPB. However, the caveat remains that block provides temporary relief and may be an adjunct to other modalities. Celiac plexus neurolysis (CPN) is recommended only in the setting of inoperable pancreatic cancer. In cases of operable pancreatic cancer, neurolysis may lead to scarring the operative field, thereby making surgery technically more challenging. Most patients who do not respond to conventional opioids or require significantly higher doses with adverse events are candidates to consider CPN (<span>4</span>).</p><p>CPB is typically for patients with pain not responding to analgesics and can be repeated at 3–6 months intervals. As pain becomes chronic, response to CPB is likely to be lesser, considering formation of neural feedback loops with cerebral pain conditioning. In patients with pancreatic cancer, pain responds better earlier in the course of disease to CPN. As disease progresses and pain persists, the neural pathways become less responsive and efficacy of CPN reduces (<span>5</span>). Kanno et al showed that EUS CPN does not improve Quality of life and pain compared to those medicated with newer analgesics like Oxycodone and fentanyl (<span>6</span>). Hence EUS CPN may be considered an adjunct in patients needing excessive doses of opioids or having significant adverse effects to opioids.</p><p>Background information on antiplatelets and anticoagulants is important. Aspirin may be continued; however other anticoagulants may need to be titrated. In addition, antibiotic prophylaxis pre-procedure is not recommended. Considering the sympatholytic effect of CPB/CPN leading to hypotension and diarrhea, preloading with 0.5 to 1 L of normal saline is helpful (<span>7</span>). CPB/CPN is done under sedation.</p><p>The celiac plexus is located just below the diaphragm above the origin of the celiac trunk from the aorta. The celiac ganglion is visible in 60–70% cases. Once localized, injection can be done using a 19G or 22G EUS-FNA needle into the plexus or ganglion. After puncture, suction is initially applied to make sure it is not in a vessel. For CPB, 10 ml of 0.25% Bupivacaine and Triamcinolone 40–80 mg (10–40 mg/ml) are injected into the celiac axis. For CPN, in addition to 10 ml of 0.25% Bupivacaine, 10–20 ml of absolute alcohol is also injected into the celiac plexus (<span>4</span>). Injection is known to be associated with clouding above the origin of the celiac axis. Unilateral injection means single injection above the origin of the celiac axis while bilateral injection means injection on both sides of the celiac axis. In a previous systematic review, Puli et al showed that the bilateral technique was associated with higher pain relief than the unilateral technique (84% vs 45%) for both CPB and CPN (<span>8</span>). A subsequent randomized trial by LeBlanc et al with 50 patients showed no significant difference between the unilateral and bilateral technique (69% vs 81%) (<span>9</span>).</p><p>Direct injection into the celiac ganglion was described by Levy et al. and was considered to be safe and effective for pain relief (<span>10</span>). Ascunce et al showed that ability to visualize the celiac ganglion was associated with better response to pain (<span>11</span>). Doi et al. in a randomized controlled trial of 34 patients showed that CGN was associated with higher response rate and higher complete response rate (<span>12</span>). Combination of EUS-CGN with broad plexus neurolysis was associated with higher response rate for pancreatic cancer pain as compared to broad plexus neurolysis (<span>13</span>).</p><p>In a subsequent study, Fujii-Lau et al showed that in 417 patients with pancreatic cancer pain who underwent CPN, survival was lesser in those with CGN than pancreatic cancer controls (193 vs 246 days; HR 1.32) (<span>14</span>). In another randomized trial, Levy et al showed that CPN was associated with higher survival than those who underwent CGN (10.46 months, vs 5.59 months; OR 1.49, p = 0.042), especially those with non-metastatic disease (<span>15</span>). In addition, the concern remains that since all ganglia may not be visible, CGN may have an incomplete effect.</p><p>Another variation is Broad Plexus Neurolysis (BPN) where injection is given above the level of the Superior Mesenteric artery origin leading to more diffuse injection with greater area of neurolysis (<span>16</span>). 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引用次数: 0

摘要

WEO 通讯编辑:Nalini M Guda MD, MASGE, AGAF, FACG, FJGESDr.Sridhar Sundaram MD、DM、FISG 现任职务:孟买霍米-巴巴国立研究所塔塔纪念医院消化疾病和临床营养科教授(消化内科)孟买塔塔纪念医院消化内科疾病管理组组长印度消化内科学会理事会成员 ESGE 多样性和公平工作组成员印度消化内科杂志管理编辑印度 EUS 俱乐部成员主要兴趣领域:治疗性内镜超声、内镜下切除技术、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断、内镜下超声诊断:治疗性内镜超声、早期消化道癌症的内镜下切除技术会阴部受侵导致的腹痛是胰胆管癌症最令人衰弱的症状之一。此外,疼痛仍是需要干预的慢性胰腺炎最复杂的相关症状之一(1)。上腹部内脏的疼痛通过传入途径传到腹腔神经丛,在 T12-L2 水平进入脊髓。腹腔神经丛的传出神经主要由交感神经纤维组成,交感神经纤维由腹主动脉旁神经节网络相互连接而成,包括腹腔轴、肠系膜上动脉起源和肾动脉水平的交感神经纤维。此外,腹腔神经丛的副交感神经传出也来自迷走神经 (2)。传统的腹腔神经丛阻断是作为术中消融手术进行的。后来,人们开始在透视引导下进行腹腔神经丛介入治疗。内镜超声引导下腹腔神经丛阻断术(CPB)于 1996 年首次被描述,目前已成为治疗标准(3)。慢性胰腺炎患者的疼痛对胰酶替代物、抗氧化剂、非麻醉性和麻醉性药物等常规措施无效,可能会成为 CPB 的短期受益者。但需要注意的是,阻滞只能暂时缓解疼痛,只能作为其他方法的辅助手段。只有在胰腺癌无法手术的情况下,才推荐使用腹腔神经丛神经溶解术(CPN)。在可手术的胰腺癌病例中,神经溶解术可能会导致手术区域结疤,从而使手术在技术上更具挑战性。大多数对传统阿片类药物无反应或需要明显加大剂量并出现不良反应的患者都可以考虑使用 CPN(4)。CPB 通常用于对镇痛药无反应的疼痛患者,可每隔 3-6 个月重复使用一次。随着疼痛转为慢性,考虑到大脑疼痛调节神经反馈环路的形成,对 CPB 的反应可能会减弱。在胰腺癌患者中,疼痛在病程早期对 CPN 的反应较好。随着病情的发展和疼痛的持续,神经通路的反应会减弱,CPN 的疗效也会降低(5)。Kanno 等人的研究表明,与使用羟考酮和芬太尼等新型镇痛药的患者相比,EUS CPN 无法改善患者的生活质量和疼痛状况(6)。因此,对于需要过量阿片类药物或对阿片类药物有明显不良反应的患者,可将 EUS CPN 作为一种辅助治疗手段。阿司匹林可以继续使用,但其他抗凝药物可能需要调整剂量。此外,不建议在术前使用抗生素预防。考虑到 CPB/CPN 的交感神经溶解作用会导致低血压和腹泻,预充 0.5 至 1 升生理盐水会有所帮助 (7)。腹腔神经丛位于腹腔干起源于主动脉的膈肌下方。腹腔神经节在 60-70% 的病例中可见。定位后,可使用 19G 或 22G EUS-FNA 针注入腹腔神经丛或腹腔神经节。穿刺后,首先进行抽吸,以确保不在血管内。对于 CPB,向腹腔轴注射 10 毫升 0.25% 布比卡因和曲安奈德 40-80 毫克(10-40 毫克/毫升)。对于 CPN,除 10 毫升 0.25% 布比卡因外,还要向腹腔神经丛注射 10-20 毫升无水酒精 (4)。众所周知,注射与腹腔轴起源上方的混浊有关。单侧注射是指腹腔轴起源上方的单次注射,而双侧注射是指腹腔轴两侧的注射。Puli 等人在之前的系统回顾中显示,在 CPB 和 CPN 中,双侧技术的疼痛缓解率(84% 对 45%)高于单侧技术(8)。Levy 等人随后对 50 名患者进行了随机试验,结果显示单侧和双侧技术无明显差异(69% 对 81%)(9)。Ascunce 等人的研究表明,能看到腹腔神经节与更好的疼痛反应有关(11)。Doi 等人 在一项对 34 名患者进行的随机对照试验中,结果显示 CGN 与较高的应答率和较高的完全应答率相关(12)。在随后的一项研究中,Fuji-Lau 等人发现,在 417 名接受 CPN 治疗的胰腺癌疼痛患者中,CGN 患者的生存期低于胰腺癌对照组(193 天 vs 246 天;HR 1.32)(14)。在另一项随机试验中,Levy 等人的研究表明,与接受 CGN 的患者相比,接受 CPN 的患者生存率更高(10.46 个月 vs 5.59 个月;OR 1.49,p = 0.042),尤其是那些非转移性疾病患者(15)。另一种方法是宽神经丛神经溶解术(BPN),即在肠系膜上动脉起源水平以上注射,从而使注射更加弥散,神经溶解面积更大(16)。然而,缺乏支持这种做法的大规模研究。在 CPN 无效的情况下,这可能是一种替代方法。众所周知,CPB/CPN 的交感溶解作用会导致一过性低血压。持续 1-2 天的一过性腹泻是 CPB/CPN 的已知并发症。可能会出现短暂的疼痛加剧,使用麻醉镇痛药后可得到很好的控制(17)。较罕见的并发症包括出血、心律失常等心脏并发症、腹膜后脓肿感染以及膈肌麻痹。转移性疾病患者和腹腔神经丛直接受肿瘤累及的患者对 CPN 的反应较差。此外,在 CPB 的情况下,之前对 CPB 有反应的患者更有可能对重复注射产生反应(18)。在之前的一项研究中,据说心率在 30 秒内持续每分钟变化 15 次与较高的反应相关(19)。在实践中,术后有排便冲动和术中出现低血压的患者表明交感神经溶解可能有效,CPB/CPN 也可能有效。EUS-CPB/CPN 仍是内镜医师执行的核心干预措施之一,作为药物治疗的辅助手段,可安全有效地控制慢性胰腺炎和胰腺癌患者的疼痛。虽然该技术在很大程度上已经标准化,但很少有变化,以确保根据患者和疾病相关因素进行优化。对于传统 EUS CPN 治疗失败的患者,可以考虑采用 EUS 引导的腹腔神经丛 RFA 等新技术!WEO 活动日历
本文章由计算机程序翻译,如有差异,请以英文原文为准。

WEO Newsletter: Tips and Tricks for Endoscopic Ultrasound guided Celiac Plexus interventions

WEO Newsletter: Tips and Tricks for Endoscopic Ultrasound guided Celiac Plexus interventions

WEO Newsletter Editor: Nalini M Guda MD, MASGE, AGAF, FACG, FJGES

Dr. Sridhar Sundaram

MD, DM, FISG

Present Designation:

Professor (Gastroenterology), Department of Digestive Diseases and Clinical Nutrition, Tata Memorial Hospital, Homi Bhabha National Institute, Mumbai

Consultant- GI Disease Management Group, Tata Memorial Hospital, Mumbai

Governing Council Member – Indian Society of Gastroenterology

Member – ESGE Diversity and Equity Working Group

Managing Editor – Indian Journal of Gastroenterology

Member – India EUS Club

Primary areas of interest: Therapeutic Endoscopic Ultrasound, Endoscopic Resection techniques for early GI cancer

Abdominal pain due to perineural invasion is one of the most debilitating symptoms associated with pancreaticobiliary cancers. In addition, pain remains one of the most complex symptoms associated with chronic pancreatitis needing intervention (1). Pain from upper abdominal viscera is transmitted via the afferent pathway to the celiac plexus leading into the spinal cord at the T12-L2 level. The efferents from the celiac plexus consists mainly of sympathetic fibres of a network of interconnected para-aortic ganglia, including those at the level of the celiac axis, superior mesenteric artery origin and also renal artery. In addition, parasympathetic efferents of the celiac plexus come from the vagus nerve (2). Traditionally celiac plexus block was performed as an intraoperative ablative procedure. Subsequently fluoroscopy guided celiac plexus interventions were performed. Endoscopic Ultrasound guided celiac plexus block (CPB) was first described in 1996 and has now become the standard of care (3).

Chronic pancreatitis patients with pain not responding to conventional measures like pancreatic enzyme replacement, antioxidants, non-narcotic and narcotic medications may be candidates who may benefit in short term from CPB. However, the caveat remains that block provides temporary relief and may be an adjunct to other modalities. Celiac plexus neurolysis (CPN) is recommended only in the setting of inoperable pancreatic cancer. In cases of operable pancreatic cancer, neurolysis may lead to scarring the operative field, thereby making surgery technically more challenging. Most patients who do not respond to conventional opioids or require significantly higher doses with adverse events are candidates to consider CPN (4).

CPB is typically for patients with pain not responding to analgesics and can be repeated at 3–6 months intervals. As pain becomes chronic, response to CPB is likely to be lesser, considering formation of neural feedback loops with cerebral pain conditioning. In patients with pancreatic cancer, pain responds better earlier in the course of disease to CPN. As disease progresses and pain persists, the neural pathways become less responsive and efficacy of CPN reduces (5). Kanno et al showed that EUS CPN does not improve Quality of life and pain compared to those medicated with newer analgesics like Oxycodone and fentanyl (6). Hence EUS CPN may be considered an adjunct in patients needing excessive doses of opioids or having significant adverse effects to opioids.

Background information on antiplatelets and anticoagulants is important. Aspirin may be continued; however other anticoagulants may need to be titrated. In addition, antibiotic prophylaxis pre-procedure is not recommended. Considering the sympatholytic effect of CPB/CPN leading to hypotension and diarrhea, preloading with 0.5 to 1 L of normal saline is helpful (7). CPB/CPN is done under sedation.

The celiac plexus is located just below the diaphragm above the origin of the celiac trunk from the aorta. The celiac ganglion is visible in 60–70% cases. Once localized, injection can be done using a 19G or 22G EUS-FNA needle into the plexus or ganglion. After puncture, suction is initially applied to make sure it is not in a vessel. For CPB, 10 ml of 0.25% Bupivacaine and Triamcinolone 40–80 mg (10–40 mg/ml) are injected into the celiac axis. For CPN, in addition to 10 ml of 0.25% Bupivacaine, 10–20 ml of absolute alcohol is also injected into the celiac plexus (4). Injection is known to be associated with clouding above the origin of the celiac axis. Unilateral injection means single injection above the origin of the celiac axis while bilateral injection means injection on both sides of the celiac axis. In a previous systematic review, Puli et al showed that the bilateral technique was associated with higher pain relief than the unilateral technique (84% vs 45%) for both CPB and CPN (8). A subsequent randomized trial by LeBlanc et al with 50 patients showed no significant difference between the unilateral and bilateral technique (69% vs 81%) (9).

Direct injection into the celiac ganglion was described by Levy et al. and was considered to be safe and effective for pain relief (10). Ascunce et al showed that ability to visualize the celiac ganglion was associated with better response to pain (11). Doi et al. in a randomized controlled trial of 34 patients showed that CGN was associated with higher response rate and higher complete response rate (12). Combination of EUS-CGN with broad plexus neurolysis was associated with higher response rate for pancreatic cancer pain as compared to broad plexus neurolysis (13).

In a subsequent study, Fujii-Lau et al showed that in 417 patients with pancreatic cancer pain who underwent CPN, survival was lesser in those with CGN than pancreatic cancer controls (193 vs 246 days; HR 1.32) (14). In another randomized trial, Levy et al showed that CPN was associated with higher survival than those who underwent CGN (10.46 months, vs 5.59 months; OR 1.49, p = 0.042), especially those with non-metastatic disease (15). In addition, the concern remains that since all ganglia may not be visible, CGN may have an incomplete effect.

Another variation is Broad Plexus Neurolysis (BPN) where injection is given above the level of the Superior Mesenteric artery origin leading to more diffuse injection with greater area of neurolysis (16). However, there is lack of large-scale studies backing this practice. It may be an alternative in situations where CPN is ineffective.

Adverse events are either sedation or procedure related. Transient hypotension due to sympatholytic effect of CPB/CPN is known. Transient diarrhea for 1–2 days is a known complication of CPB/CPN. Transient increase in pain may occur, managed well with narcotic analgesics (17). Rarer complications include bleeding, cardiac complications like arrhythmias, infection with retroperitoneal abscess and also diaphragmatic paralysis.

Pain relief with CPN is said to be effective in up to 70–80% patients and durable up to 24 months. Patients having metastatic disease and those with direct involvement of celiac plexus by tumor are known to respond poorly. In addition, in case of CPB, previous response to CPB indicates higher likelihood of response to repeat injection (18). In a previous study, heart rate change by >15 beats per min sustained over >30 s was said to be associated with higher response (19). In practice, patients having urge to defecate post-procedure and hypotension intraprocedure suggests likely effective sympatholysis and efficacious CPB/CPN.

EUS-CPB/CPN remains one of the core interventions performed by endosonologists as an adjunct to medical therapy for managing pain in chronic pancreatitis and pancreatic cancer in a safe and effective manner. While the technique is largely standardized, few variations ensure optimization based on patient and disease related factors. Newer techniques in the form of EUS guided RFA of celiac plexus can be considered in patients who fail conventional EUS CPN.

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来源期刊
Digestive Endoscopy
Digestive Endoscopy 医学-外科
CiteScore
10.10
自引率
15.10%
发文量
291
审稿时长
6-12 weeks
期刊介绍: Digestive Endoscopy (DEN) is the official journal of the Japan Gastroenterological Endoscopy Society, the Asian Pacific Society for Digestive Endoscopy and the World Endoscopy Organization. Digestive Endoscopy serves as a medium for presenting original articles that offer significant contributions to knowledge in the broad field of endoscopy. The Journal also includes Reviews, Original Articles, How I Do It, Case Reports (only of exceptional interest and novelty are accepted), Letters, Techniques and Images, abstracts and news items that may be of interest to endoscopists.
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