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激光捕获显微切割联合超高效液相色谱-串联质谱法对骨组织中抗生素的空间定量分析。

Spatial quantitation of antibiotics in bone tissue compartments by laser-capture microdissection coupled with UHPLC-tandem mass spectrometry.

机构信息

Center for Discovery and Innovation, Hackensack Meridian Health, 111 Ideation Way, Nutley, NJ, 07110, USA.

Department of Medical Sciences, Hackensack Meridian School of Medicine, 123 Metro Blvd, Nutley, NJ, USA.

出版信息

Anal Bioanal Chem. 2022 Sep;414(23):6919-6927. doi: 10.1007/s00216-022-04257-3. Epub 2022 Aug 10.

Abstract

Bones are the site of multiple diseases requiring chemotherapy, including cancer, arthritis, osteoporosis and infections. Yet limited methodologies are available to investigate the spatial distribution and quantitation of small molecule drugs in bone compartments, due to the difficulty of sectioning undecalcified bones and the interference of decalcification methods with spatially resolved drug quantitation. To measure drug concentrations in distinct anatomical bone regions, we have developed a workflow that enables spatial quantitation of thin undecalcified bone sections by laser-capture microdissection coupled to HPLC/tandem mass spectrometry, and spatial mapping on adjacent sections by mass spectrometry imaging. The adhesive film and staining methods were optimized to facilitate histology staining on the same sections used for mass spectrometry image acquisition, revealing drug accumulation in the underlying bone tissue architecture, for the first time. Absolute spatial concentrations of rifampicin, bedaquiline, doxycycline, vancomycin and several of their active metabolites are shown for both small rodent bones and larger rabbit bones that more closely resemble human bone density. Overlaid MALDI mass spectrometry images of drugs and histology staining enabled the generation of semi-quantitative data from regions of interest within anatomical bone compartments. These data correlated with absolute drug concentrations determined by HPLC-MS/MS in laser-capture microdissection samples. Collectively, these techniques enable semi- and fully quantitative drug distribution investigations within bone tissue compartments for the first time. Our workflow can be translated to image and quantify not only drugs but also biomarkers of disease to investigate drug penetration as well as mechanisms underlying bone disorders.

摘要

骨骼是多种需要化疗的疾病的部位,包括癌症、关节炎、骨质疏松症和感染。然而,由于难以对未脱钙的骨骼进行切片,以及脱钙方法会干扰空间分辨药物定量,因此可用的方法有限,无法研究小分子药物在骨骼中的空间分布和定量。为了测量不同解剖骨骼区域的药物浓度,我们开发了一种工作流程,该流程可通过激光捕获微切割与 HPLC/串联质谱联用,对薄的未脱钙骨切片进行空间定量,并通过质谱成像在相邻切片上进行空间映射。优化了粘合膜和染色方法,以促进在用于获取质谱图像的相同切片上进行组织学染色,首次揭示了药物在骨组织结构下的积累。对于更接近人类骨密度的小型啮齿动物骨骼和较大的兔骨骼,均显示了利福平、贝达喹啉、强力霉素、万古霉素及其几种活性代谢物的绝对空间浓度。药物和组织学染色的 MALDI 质谱图像叠加,使我们能够从解剖骨骼腔室的感兴趣区域生成半定量数据。这些数据与激光捕获微切割样本中通过 HPLC-MS/MS 确定的绝对药物浓度相关。总的来说,这些技术首次能够在骨骼组织腔室中进行药物分布的半定量和全定量研究。我们的工作流程不仅可以用于成像和定量药物,还可以用于定量疾病生物标志物,以研究药物渗透以及骨骼疾病的潜在机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/effe/9436889/3884a2b7aef2/216_2022_4257_Fig1_HTML.jpg

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