确定氮芥暴露后25(OH)D挽救治疗的时机。
Defining the timing of 25(OH)D rescue following nitrogen mustard exposure.
作者信息
Das Lopa M, Binko Amy M, Traylor Zachary P, Duesler Lori, Lu Kurt Q
机构信息
a Department of Dermatology , Case Western Reserve University School of Medicine , Cleveland , OH , USA.
c Department of Biology , Case Western Reserve University , Cleveland , OH , USA.
出版信息
Cutan Ocul Toxicol. 2018 Jun;37(2):127-132. doi: 10.1080/15569527.2017.1355315. Epub 2017 Aug 8.
OBJECTIVE
Mass exposure to alkylating agents such as nitrogen mustard (NM), whether accidental or intentional as during warfare, are known to cause systemic toxicity and severe blistering from cutaneous exposure. Thus, establishing the timing and appropriate dose of any potential drug designed to reverse or impede these toxicities is critical for wound repair and survival. Our previous data demonstrates that a single intraperitoneal injection of low-dose 25-hydroxyvitamin D3 (25(OH)D) given as early as 1 h following NM exposure is sufficient to rescue mice from pancytopenia and death. However, the duration of time following exposure where intervention is still effective as a countermeasure is unknown. In this study, we sought to assess the maximal time permissible following NM exposure where 25(OH)D still affords protection against NM-induced cutaneous injury. Additionally, we determined if a higher dose of 25(OH)D would be more efficacious at time interval where low dose 25(OH)D is no longer effective.
METHODS
Low (5 ng) and high (50 ng) doses of 25(OH)D were administered intraperitoneally to mice following exposure to topical NM to assess wound resolution and survival. Mice were imaged and weighed daily to measure wound healing and to monitor systemic toxicity.
RESULTS
We demonstrated that 5 ng 25(OH)D administered as early as 1 h and as late as 24 h post-NM exposure is able to achieve 100% recovery in mice. In contrast, intervention at and beyond 48 h of NM exposure failed to achieve full recovery and resulted in ≥60% death between days 6 and 12, demonstrating the critical nature of timely intervention with 25(OH)D at each respective dose. In order to circumvent the observed failure at >48 h exposure, we provided two consecutive doses of 5 ng or 50 ng of 25(OH)D at 48 h and 72 h post-NM exposure. Repeat dosing with 25(OH)D at 48 h and beyond led to marked improvement of lesion size with 75% recovery from mortality.
CONCLUSIONS
The opportunity to use 25(OH)D as a medical countermeasure for NM-induced toxicity has a finite of window for intervention. However, modifications such as repeat dosing can be an effective strategy to extend the intervention potential of 25(OH)D.
目的
大量接触烷基化剂如氮芥(NM),无论是意外接触还是如战争期间的故意接触,均已知会导致全身毒性以及皮肤接触引起的严重水疱。因此,确定任何旨在逆转或减轻这些毒性的潜在药物的给药时间和合适剂量对于伤口修复和存活至关重要。我们之前的数据表明,在接触NM后1小时尽早单次腹腔注射低剂量的25-羟基维生素D3(25(OH)D)足以使小鼠免于全血细胞减少和死亡。然而,接触后干预作为一种对策仍有效的持续时间尚不清楚。在本研究中,我们试图评估NM接触后25(OH)D仍能提供针对NM诱导的皮肤损伤保护作用的最长允许时间。此外,我们确定在低剂量25(OH)D不再有效的时间间隔给予更高剂量的25(OH)D是否会更有效。
方法
在局部接触NM后,给小鼠腹腔注射低剂量(5 ng)和高剂量(50 ng)的25(OH)D,以评估伤口愈合情况和存活率。每天对小鼠进行成像和称重,以测量伤口愈合情况并监测全身毒性。
结果
我们证明,在接触NM后1小时尽早且最晚在24小时给予5 ng 25(OH)D能够使小鼠100%恢复。相比之下,在接触NM后48小时及以后进行干预未能实现完全恢复,并导致在第6天至第12天之间≥60%的小鼠死亡,这表明在每个相应剂量下及时用25(OH)D进行干预的重要性。为了规避在接触>48小时时观察到的失败情况,我们在接触NM后48小时和72小时连续给予两剂5 ng或50 ng的25(OH)D。在48小时及以后重复给予剂量的25(OH)D导致损伤大小显著改善,死亡率恢复75%。
结论
将25(OH)D用作NM诱导毒性的医学对策的干预机会有一个有限的窗口。然而,如重复给药等调整可以是扩展25(OH)D干预潜力的有效策略。
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