M/Z: 786.4798
Hit 2 annotations: Tacrolimus_[M+H-H2O]+
; PA(20:3(5Z,8Z,11Z)/22:6(5Z,7Z,10Z,13Z,16Z,19Z)-OH(4))_[M]+
- Confirmed: 这个参考离子已经通过手动审计得到确认和验证。
- Reliable: 这个参考离子可能在特定的解剖组织环境中高度保守。
- Unreliable: 这个参考离子具有较高的排名价值,但缺乏可重复性。
- Unavailable: 由于排名价值低且缺乏可重复性,这个参考离子不应用于注释。
Found 9 Reference Ions Near m/z 786.4798
NovoCell ID | m/z | Mass Window | Metabolite | Ranking | Anatomy Context |
---|---|---|---|---|---|
MSI_000062961 Reliable | 786.4833 | 786.4833 ~ 786.4833 MzDiff: 0.2 ppm |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
0.47 (100%) | Mus musculus [UBERON:0000956] cerebral cortex |
MSI_000046537 Reliable | 786.4798 | 786.4798 ~ 786.4798 MzDiff: none |
PA(20:3(5Z,8Z,11Z)/22:6(5Z,7Z,10Z,13Z,16Z,19Z)-OH(4)) (BioDeep_00000189999) Formula: C45H71O9P (786.4835) |
4.21 (100%) | Mus musculus [UBERON:0002107] liver |
MSI_000002386 Unreliable | 786.4832 | 786.4832 ~ 786.4832 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
2.1 (100%) | Rattus norvegicus [UBERON:0001950] neocortex |
MSI_000003254 Unreliable | 786.4832 | 786.4832 ~ 786.4832 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
0.32 (100%) | Rattus norvegicus [UBERON:0002037] cerebellum |
MSI_000005285 Unavailable | 786.4832 | 786.4832 ~ 786.4832 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
-0.86 (100%) | Rattus norvegicus [UBERON:0002298] brainstem |
MSI_000005867 Unavailable | 786.4832 | 786.4832 ~ 786.4832 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
-0.79 (100%) | Rattus norvegicus [UBERON:0002435] striatum |
MSI_000026447 Unreliable | 786.4799 | 786.4799 ~ 786.4799 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
1.79 (100%) | Mus musculus [UBERON:0002048] lung |
MSI_000026894 Unreliable | 786.487 | 786.487 ~ 786.487 MzDiff: none |
Not Annotated | 1.78 (0%) | Mus musculus [UBERON:0002048] lung |
MSI_000043940 Unreliable | 786.4834 | 786.4834 ~ 786.4834 MzDiff: none |
Tacrolimus (BioDeep_00000000218) Formula: C44H69NO12 (803.482) |
2.59 (100%) | Rattus norvegicus [UBERON:0002264] olfactory bulb |
Found 5 Sample Hits
Metabolite | Species | Sample | |
---|---|---|---|
Tacrolimus Formula: C44H69NO12 (803.482) Adducts: [M+H-H2O]+ (Ppm: 5.8) |
Rattus norvegicus (Brain) |
Spectroswiss - sol_2x_br_2Resolution: 17μm, 488x193
|
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Tacrolimus Formula: C44H69NO12 (803.482) Adducts: [M+H-H2O]+ (Ppm: 1.6) |
Mus musculus (Lung) |
image1Resolution: 40μm, 187x165
Fig. 2 MALDI-MSI data from the same mouse lung tissue analyzed in Fig. 1. A: Optical image of the post-MSI, H&E-stained tissue section. B–D, F–G: Ion images of (B) m/z 796.6855 ([U13C-DPPC+Na]+), (C) m/z 756.5514 ([PC32:0+Na]+), (D) m/z 765.6079 ([D9-PC32:0+Na]+), (F) m/z 754.5359 ([PC32:1+Na]+), and (G) m/z 763.5923 ([D9-PC32:1+Na]+). E, H: Ratio images of (E) [D9-PC32:0+Na]+:[PC32:0+Na]+ and (H) [D9-PC32:1+Na]+:[PC32:1+Na]+. Part-per-million (ppm) mass errors are indicated in parentheses. All images were visualized using total-ion-current normalization and using hotspot removal (high quantile = 99%). DPPC = PC16:0/16:0. U13C-DPPC, universally 13C-labeled dipalmitoyl PC; PC, phosphatidylcholine; MSI, mass spectrometry imaging; H&E, hematoxylin and eosin.
Fig 1-3, Fig S1-S3, S5 |
|
Tacrolimus Formula: C44H69NO12 (803.482) Adducts: [M+H-H2O]+ (Ppm: 1.6) |
Mus musculus (Lung) |
image4Resolution: 40μm, 162x156
Fig 6c
Fig. 6 MALDI-MSI of U13C-PC16:0/16:0 acyl chain remodeling. A: Averaged MALDI mass spectrum from lung tissue collected from mice euthanized 12 h after administration of D9-choline and U13C-DPPC–containing Poractant alfa surfactant. The ion at m/z 828.6321 is assigned as the [M+Na]+ ion of 13C24-PC16:0_20:4 formed by acyl remodeling of U13C-PC16:0/16:0. The “NL” value refers to the intensity of the base peak in the full range MS1 spectrum. B: MS/MS spectrum of precursor ions at m/z 828.5 ± 0.5 with fragment ions originating from [13C24-PC16:0_20:4+Na]+ annotated. Part-per-million (ppm) mass errors are provided in parentheses. C, D: MALDI-MSI data of [U13C-DPPC+Na]+ (blue), [PC36:4+Na]+ (green) and [13C24-PC16:0_20:4+Na]+ (red) in lung tissue collected from mice (C) 12 h and (D) 18 h after label administration. All images were visualized using total-ion-current normalization and hotspot removal (high quantile = 99%). MS/MS, tandem mass spectrometry; MSI, mass spectrometry imaging; PC, phosphatidylcholine; U13C-DPPC, universally 13C-labeled dipalmitoyl PC. |
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Tacrolimus Formula: C44H69NO12 (803.482) Adducts: [M+H-H2O]+ (Ppm: 6.2) |
Mus musculus (Lung) |
image5Resolution: 40μm, 163x183
Supplementary Figure S8. MALDI-MSI data of mouse lung tissue administered with D9-choline and
U 13C-DPPC–containing Poractant alfa surfactant (labels administered 18 h prior to sacrifice). Ion
images of (a) m/z 796.6856 ([U13C-DPPC+Na]+), (b) m/z 756.5154 [PC32:0+Na]+ and (c) m/z 765.6079
([D9-PC32:0+Na]+). (d) Overlay image of [U13C-DPPC+Na]+ (red) and [D9-PC32:0+Na]+ (green).
Parts per million (ppm) mass errors are indicated in parentheses. All images were visualised using totalion-current normalisation and using hotspot removal (high quantile = 99%). DPPC = PC16:0/16:0. |
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PA(20:3(5Z,8Z,11Z)/22:6(5Z,7Z,10Z,13Z,16Z,19Z)-OH(4)) Formula: C45H71O9P (786.4835) Adducts: [M]+ (Ppm: 4.1) |
Mus musculus (Liver) |
Salmonella_final_pos_recalResolution: 17μm, 691x430
A more complete and holistic view on host–microbe interactions is needed to understand the physiological and cellular barriers that affect the efficacy of drug treatments and allow the discovery and development of new therapeutics. Here, we developed a multimodal imaging approach combining histopathology with mass spectrometry imaging (MSI) and same section imaging mass cytometry (IMC) to study the effects of Salmonella Typhimurium infection in the liver of a mouse model using the S. Typhimurium strains SL3261 and SL1344. This approach enables correlation of tissue morphology and specific cell phenotypes with molecular images of tissue metabolism. IMC revealed a marked increase in immune cell markers and localization in immune aggregates in infected tissues. A correlative computational method (network analysis) was deployed to find metabolic features associated with infection and revealed metabolic clusters of acetyl carnitines, as well as phosphatidylcholine and phosphatidylethanolamine plasmalogen species, which could be associated with pro-inflammatory immune cell types. By developing an IMC marker for the detection of Salmonella LPS, we were further able to identify and characterize those cell types which contained S. Typhimurium.
[dataset] Nicole Strittmatter. Holistic Characterization of a Salmonella Typhimurium Infection Model Using Integrated Molecular Imaging, metabolights_dataset, V1; 2022. https://www.ebi.ac.uk/metabolights/MTBLS2671. |
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