糖尿病皮肤特性改变对芬太尼透皮滴药期的影响：单中心回顾性研究及糖尿病动物模型研究

IF 1.2 Q4 PHARMACOLOGY & PHARMACY Journal of Pharmaceutical Health Care and Sciences Pub Date : 2024-12-18 DOI:10.1186/s40780-024-00402-5

Satoshi Mizuno, Makiko Takabayashi, Hiroko Makihara, Kazuhiro Ogai, Kei Tsukui, Yuriko Ito, Takahiro Kawakami, Yusuke Hara, Arimi Fujita, Yoshihiro Tokudome, Tomoko Akase, Yukio Kato, Tsutomu Shimada, Yoshimichi Sai

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引用次数: 0

摘要

背景：芬太尼透皮剂量滴定预防疼痛未缓解，不仅要考虑剂量调整，而且要考虑滴定周期，而滴定周期受达到稳定状态所需时间的影响。许多癌症性疼痛患者都有可能影响皮肤特性和透皮吸收的合并症。我们假设糖尿病（DM）引起的皮肤变化会影响透皮芬太尼的滴定期。我们通过回顾性研究和糖尿病动物模型研究来验证这一假设。方法：采用回顾性研究，以经皮芬太尼起始患者的“剂量变化”和“救援阿片类药物数量”来定义滴定期。采用多元logistic回归分析滴定期与合并症（包括糖尿病）的关系。在糖尿病动物模型研究中，分析DM模型Goto-Kakizaki （GK）大鼠角质层（SC）细胞间脂质，并检测静脉或经皮给药芬太尼的药代动力学。结果：在回顾性研究中，滴药周期为5 ~ 39天（n = 387），服用更长时间（6天以上）的患者与未明确DM患者的AOR（95%可信区间）显著相关，为0.438（0.217-0.884）。在糖尿病动物模型研究中，与Wistar大鼠相比，GK大鼠SC中的神经酰胺（CERs）含量降低了约30%。GK大鼠经皮给药芬太尼的吸收率常数（ka）增加了约1.4倍，但透皮生物利用度(F)和全身清除率（CLtot）没有差异。结论：我们的研究结果表明，经皮给药芬太尼在合并糖尿病的癌症患者中更快达到稳定状态。对这些患者进行早期疼痛评估和剂量调整是可能的。

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Effect of changes in skin properties due to diabetes mellitus on the titration period of transdermal fentanyl: single-center retrospective study and diabetic animal model study.

Background: In the dose titration of transdermal fentanyl to prevent unrelieved pain, it is important to consider not only dose adjustment, but also the titration period, which is influenced by the time required to reach the steady state. Many patients with cancer pain experience comorbidities that might affect the skin properties and influence transdermal absorption. We hypothesized that skin changes due to diabetes mellitus (DM) would affect the titration period of transdermal fentanyl. We conducted a retrospective study and diabetic animal model study to test this hypothesis.

Methods: In the retrospective study, the titration period was defined in terms of "dose change" and "number of rescue opioids" in patients initiated on transdermal fentanyl. Multiple logistic regression analysis was performed to analyze the relation between the titration period and comorbidities, including DM. In the diabetic animal model study, intercellular lipids of stratum corneum (SC) were analyzed in Goto-Kakizaki (GK) rats, a model of DM, and the pharmacokinetics of intravenously or transdermally administered fentanyl was examined.

Results: In the retrospective study, the titration period ranged from 5 to 39 days (n = 387), and the patients taking a longer period (6 days or more) was significantly related to in patients with unspecified DM: AOR (95% confidence interval), 0.438 (0.217-0.884). In the diabetic animal model study, the ceramides (CERs) content in the SC was decreased by approximately 30% in GK rats compared to Wistar rats. The absorption rate constant (k_a) of fentanyl administered transdermally was increased approximately 1.4-fold in GK rats, though there was no difference in transdermal bioavailability (F) or systemic clearance (CL_tot).

Conclusion: Our results suggest that the steady state of transdermally administered fentanyl is reached sooner in cancer patients with DM as a comorbidity. Earlier pain assessment and dose adjustment may be possible in these patients.

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