Commentary on D'Agata Mount et al.: Higher dose buprenorphine to improve retention in opioid use disorder treatment, prevent relapse, and optimize integrated care interventions

IF 5.2 1区 医学 Q1 PSYCHIATRY Addiction Pub Date : 2024-09-23 DOI:10.1111/add.16672
Paolo Mannelli
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Consistently, every round of evaluations has shown the use of higher doses to be associated with better outcomes and to be one of the best overdose prevention tools [<span>4</span>].</p><p>One detail of the results stimulates reflection, which is concerning the increased influence of non-physiologic triggers of drug use when the buprenorphine dose is raised to 32 mg. Nothing in the results indicates it is a warning for the higher dose approach. In any case, using a wider range of buprenorphine doses may enhance the possibility to examine quantity and duration of treatment in relation to specific interventions, and further improve outcomes. To avoid a simplistic medication-centered approach, we could envision stepwise multi-phase protocols to address individual problems within a precision medicine framework that includes patients' genetic profile, lifestyle and environment, along with characteristics of disease and the proposed treatment [<span>5</span>]. By now, we can identify triggers and match them with effective interventions. For example, the effects of psychosocial stressors can be partly reduced by adequate buprenorphine dosing [<span>6</span>], but the administration of buprenorphine has limited efficacy on triggers of relapse tied to environmental stressors and social determinants of health, which require the development of sustainable long-term preventive community based interventions [<span>7</span>]. National initiatives such as the National Institute of Health ‘Helping to End Addiction Long-term Initiative (HEAL)’ will provide a path to make evidence-based preventive services accessible to all persons who experience risk for substance use disorder and relapse [<span>8</span>].</p><p>When it comes to the evaluation of triggers of drug use, a single measure of craving would be more powerful than the dichotomous values for each of the triggers in the study. Craving is an important patient-reported symptom, but finding consensus on evaluation methods remains a work in-progress [<span>9</span>]. In this study, craving is listed as one of the physiologic withdrawal symptoms, instead of being considered a final expression of a diverse range of triggers [<span>10</span>]. Following the latter interpretation, all physiologic and non-physiologic factors described in the study would be expressed through ratings of craving and drug seeking. How this can be done while preserving the individuality and traceability of each trigger requires a structured form of craving evaluation, the proof that it is a more informative tool than visual analog scales, and the agreement that craving measures are not limited to acute withdrawal [<span>9</span>].</p><p>One last reflection is about the choice of the ‘best fit’ setting to test a higher dose buprenorphine approach. In the study, mental health stressors are among triggers of relapse in OUD patients treated for medical conditions, namely hepatitis C virus, and the existence of comorbidities in this group of patients is discussed as a potential limit to the generalizability of the results. On the other hand, this limit can be a strength, and treatment of special populations can become a strong support to wider implementation. Following the lost opportunity with HIV care, where high retention rates in retroviral treatment have not translated into overdose prevention [<span>11</span>], we have learned that it can be hard, but not impossible to reach out to people who use drugs. Providing and receiving treatment for a comorbid condition represents one possibility to connect and deliver drug interventions within a harm reduction paradigm. In particular, the integrated treatment of comorbid OUD patients has a natural, underutilized and potentially consequential place in primary care (PC), where retention in treatment is favorable [<span>12</span>]. It is the responsibility of clinical and community research to provide potential PC prescribers with the information that 32 mg, and perhaps higher dose buprenorphine is safe, effective and may facilitate treatment acceptability and ease management [<span>13</span>]. PC providers in turn may find a stronger motivation to prescribe medications for OUD and to educate patients and families. 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Abstract

D'Agata Mount et al. [1] offer convincing proofs of the superiority of 32 mg/day buprenorphine for the low-threshold treatment of opioid use disorder (OUD), despite a non-randomized uncontrolled design. The study is a retrospective longitudinal observation and provides within group and between group comparisons with the 24 mg/day dose, identifying strong differences in a relatively small sample. This is undoubtedly fitting, the benchmark is now 32 mg, it was 24 mg before [2] and 16 mg before that [3]. Consistently, every round of evaluations has shown the use of higher doses to be associated with better outcomes and to be one of the best overdose prevention tools [4].

One detail of the results stimulates reflection, which is concerning the increased influence of non-physiologic triggers of drug use when the buprenorphine dose is raised to 32 mg. Nothing in the results indicates it is a warning for the higher dose approach. In any case, using a wider range of buprenorphine doses may enhance the possibility to examine quantity and duration of treatment in relation to specific interventions, and further improve outcomes. To avoid a simplistic medication-centered approach, we could envision stepwise multi-phase protocols to address individual problems within a precision medicine framework that includes patients' genetic profile, lifestyle and environment, along with characteristics of disease and the proposed treatment [5]. By now, we can identify triggers and match them with effective interventions. For example, the effects of psychosocial stressors can be partly reduced by adequate buprenorphine dosing [6], but the administration of buprenorphine has limited efficacy on triggers of relapse tied to environmental stressors and social determinants of health, which require the development of sustainable long-term preventive community based interventions [7]. National initiatives such as the National Institute of Health ‘Helping to End Addiction Long-term Initiative (HEAL)’ will provide a path to make evidence-based preventive services accessible to all persons who experience risk for substance use disorder and relapse [8].

When it comes to the evaluation of triggers of drug use, a single measure of craving would be more powerful than the dichotomous values for each of the triggers in the study. Craving is an important patient-reported symptom, but finding consensus on evaluation methods remains a work in-progress [9]. In this study, craving is listed as one of the physiologic withdrawal symptoms, instead of being considered a final expression of a diverse range of triggers [10]. Following the latter interpretation, all physiologic and non-physiologic factors described in the study would be expressed through ratings of craving and drug seeking. How this can be done while preserving the individuality and traceability of each trigger requires a structured form of craving evaluation, the proof that it is a more informative tool than visual analog scales, and the agreement that craving measures are not limited to acute withdrawal [9].

One last reflection is about the choice of the ‘best fit’ setting to test a higher dose buprenorphine approach. In the study, mental health stressors are among triggers of relapse in OUD patients treated for medical conditions, namely hepatitis C virus, and the existence of comorbidities in this group of patients is discussed as a potential limit to the generalizability of the results. On the other hand, this limit can be a strength, and treatment of special populations can become a strong support to wider implementation. Following the lost opportunity with HIV care, where high retention rates in retroviral treatment have not translated into overdose prevention [11], we have learned that it can be hard, but not impossible to reach out to people who use drugs. Providing and receiving treatment for a comorbid condition represents one possibility to connect and deliver drug interventions within a harm reduction paradigm. In particular, the integrated treatment of comorbid OUD patients has a natural, underutilized and potentially consequential place in primary care (PC), where retention in treatment is favorable [12]. It is the responsibility of clinical and community research to provide potential PC prescribers with the information that 32 mg, and perhaps higher dose buprenorphine is safe, effective and may facilitate treatment acceptability and ease management [13]. PC providers in turn may find a stronger motivation to prescribe medications for OUD and to educate patients and families. In fact, although a minority of PC providers feel comfortable handling buprenorphine [14], as many as 61% Americans do not even know that PC physicians can prescribe buprenorphine, although 82% of potential patients would feel comfortable to receive the treatment by their family doctor [15].

Paolo Mannelli: Conceptualization; writing—original draft.

The author declares funds for research, fees for consulting, and educational services from Indivior PLC, Alkermes, Guidepoint global.

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对 D'Agata Mount 等人的评论:加大丁丙诺啡剂量以改善阿片类药物使用障碍的治疗效果、预防复发并优化综合护理干预。
D'Agata Mount 等人的研究[1]提供了令人信服的证据,证明 32 毫克/天丁丙诺啡用于阿片类药物使用障碍(OUD)的低阈值治疗具有优越性,尽管该研究采用的是非随机非对照设计。该研究是一项回顾性纵向观察,提供了组内和组间与 24 毫克/天剂量的比较,在相对较小的样本中发现了强烈的差异。这无疑是合适的,现在的基准是 32 毫克,之前是 24 毫克[2],再之前是 16 毫克[3]。一致的是,每一轮评估都表明,使用更大的剂量会带来更好的疗效,并且是预防用药过量的最佳工具之一[4]。结果中的一个细节引起了人们的反思,那就是当丁丙诺啡剂量提高到 32 毫克时,非生理性用药诱因的影响会增加。结果中没有任何迹象表明这是对高剂量方法的警告。无论如何,使用更大范围的丁丙诺啡剂量可能会提高研究与特定干预措施相关的治疗数量和持续时间的可能性,并进一步改善结果。为了避免简单化的以药物为中心的方法,我们可以设想在精准医学框架内采用分步多阶段方案来解决个体问题,该框架包括患者的遗传特征、生活方式和环境,以及疾病的特点和建议的治疗方法[5]。现在,我们已经可以确定诱发因素,并将其与有效的干预措施相匹配。例如,适当的丁丙诺啡剂量可以部分减轻社会心理压力的影响[6],但丁丙诺啡的使用对与环境压力和健康的社会决定因素相关的复发诱因的疗效有限,这就需要制定可持续的长期预防性社区干预措施[7]。国家健康研究所的 "帮助戒除毒瘾长期倡议(HEAL)"等国家倡议将提供一条途径,让所有面临药物使用障碍和复吸风险的人都能获得循证预防服务[8]。渴望是一种重要的患者报告症状,但就评估方法达成共识仍是一项正在进行的工作[9]。在本研究中,渴求被列为生理戒断症状之一,而不是被视为各种诱因的最终表现[10]。根据后一种解释,研究中描述的所有生理和非生理因素都将通过对渴求和毒品寻求的评分来表达。如何做到这一点,同时保留每个触发因素的个体性和可追溯性,需要一种结构化的渴求评价形式,证明它是比视觉模拟量表更有参考价值的工具,并同意渴求测量不仅限于急性戒断[9]。最后一个思考是关于选择 "最合适 "的环境来测试高剂量丁丙诺啡的方法。在这项研究中,心理健康压力因素是因疾病(即丙型肝炎病毒)而接受治疗的 OUD 患者复发的诱因之一。另一方面,这种限制也可以成为一种优势,对特殊人群的治疗可以成为更广泛实施的有力支持。在艾滋病护理方面,高逆转录病毒治疗保留率并没有转化为过量用药预防[11],在失去机会之后,我们认识到,向吸毒者伸出援手可能很难,但并非不可能。提供和接受并发症治疗是在减少危害范例内连接和提供毒品干预的一种可能性。特别是,对合并有 OUD 的患者进行综合治疗在初级保健(PC)中具有天然的、未得到充分利用的和潜在的重要地位,因为在初级保健中保持治疗是有利的[12]。临床和社区研究有责任向潜在的初级保健处方者提供信息,说明 32 毫克或更高剂量的丁丙诺啡是安全、有效的,并可促进治疗的可接受性和简化管理[13]。反过来,PC 提供者可能会发现他们有更强的动力来开具治疗 OUD 的药物并教育患者和家属。事实上,尽管少数个体化医疗服务提供者对丁丙诺啡的使用感到得心应手[14],但多达61%的美国人甚至不知道个体化医疗医生可以开丁丙诺啡处方,尽管82%的潜在患者愿意接受家庭医生的治疗[15]。
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来源期刊
Addiction
Addiction 医学-精神病学
CiteScore
10.80
自引率
6.70%
发文量
319
审稿时长
3 months
期刊介绍: Addiction publishes peer-reviewed research reports on pharmacological and behavioural addictions, bringing together research conducted within many different disciplines. Its goal is to serve international and interdisciplinary scientific and clinical communication, to strengthen links between science and policy, and to stimulate and enhance the quality of debate. We seek submissions that are not only technically competent but are also original and contain information or ideas of fresh interest to our international readership. We seek to serve low- and middle-income (LAMI) countries as well as more economically developed countries. Addiction’s scope spans human experimental, epidemiological, social science, historical, clinical and policy research relating to addiction, primarily but not exclusively in the areas of psychoactive substance use and/or gambling. In addition to original research, the journal features editorials, commentaries, reviews, letters, and book reviews.
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