Summary of Study ST002065

This data is available at the NIH Common Fund's National Metabolomics Data Repository (NMDR) website, the Metabolomics Workbench, https://www.metabolomicsworkbench.org, where it has been assigned Project ID PR001307. The data can be accessed directly via it's Project DOI: 10.21228/M8S124 This work is supported by NIH grant, U2C- DK119886.

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Study IDST002065
Study TitleMetabolic impact of anticancer drugs Pd2Spermine and Cisplatin on the nonpolar extracts of brain from healthy mice (part 2)
Study TypeNMR-based metabolomics
Study SummaryPlatinum (Pt(II)) drugs, e.g. cisplatin (cDDP), are some of the most used chemotherapeutic agents, yet tumor acquired resistance and high toxicity are still current drawbacks. Palladium (Pd(II))-complexes are alternatives due to similar metal coordination and promising cytotoxic properties. Metabolomics can measure the metabolic response of drug-exposed tissues, unveiling insight into drug mechanisms and new markers of drug efficacy/toxicity. The present 1H NMR metabolomics study aims to characterize the in vivo response of the impact of a Pd(II)-complex with polyamine spermine (Pd2Spm), compared to cDDP, on nonpolar metabolism of brain from healthy mice at 1, 12 and 48 h post-injection times.
Institute
University of Aveiro
DepartmentDepartment of Chemistry and CICECO-Aveiro Institute of Materials
LaboratoryMetabolomics from Ana M. Gil
Last NameCarneiro
First NameTatiana João
AddressCampus Universitário de Santiago, Aveiro, Aveiro, 3810-193, Portugal
Emailtatiana.joao@ua.pt
Phone+351 234 370 200
Submit Date2022-01-10
Num Groups9
Total Subjects45
Num Females45
Raw Data AvailableYes
Analysis Type DetailNMR
Release Date2022-02-02
Release Version1
Tatiana João Carneiro Tatiana João Carneiro
https://dx.doi.org/10.21228/M8S124
ftp://www.metabolomicsworkbench.org/Studies/ application/zip

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Project:

Project ID:PR001307
Project DOI:doi: 10.21228/M8S124
Project Title:Biochemical Impact of Platinum and Palladium-based Anticancer Agents – BioIMPACT
Project Type:NMR-based metabolomics
Project Summary:Platinum (Pt(II)) drugs, e.g. cisplatin (cDDP), are some of the most used chemotherapeutic agents, yet tumor acquired resistance and high toxicity are still current drawbacks. Palladium (Pd(II))-complexes are alternatives due to similar metal coordination and promising cytotoxic properties. Metabolomics can measure the metabolic response of drug-exposed tissues, unveiling insight into drug mechanisms and new markers of drug efficacy/toxicity. The present 1H NMR metabolomics study aims to characterize the in vivo response of the impact of a Pd(II)-complex with polyamine spermine (Pd2Spm), compared to cDDP, on the metabolism of several organs from healthy mice.
Institute:University of Aveiro
Department:Department of Chemistry and CICECO-Aveiro Institute of Materials
Laboratory:Metabolomics from Ana M. Gil
Last Name:Carneiro
First Name:Tatiana J.
Address:Campus Universitário de Santiago, Aveiro, Aveiro, 3810-193, Portugal
Email:tatiana.joao@ua.pt
Phone:+351926369478
Funding Source:This research was developed within the scope of the CICECO—Aveiro Institute of Materials, with references UIDB/50011/2020 and UIDP/50011/2020, financed by national funds through the Por-tuguese Foundation for Science and Technology (FCT/MEC) and when appropriate co-financed by European Regional Development Fund (FEDER) under the PT2020 Partnership Agreement. This work was also funded by the FCT through LAQV/REQUIMTE FCT UIDB/50006/2020 (C.D.), UIDB/00070/2020 (A.L.M.B.d.C and M.P.M.M.), POCI-01-0145-FEDER-0016786, and Cen-tro-01-0145-FEDER-029956 (co-financed by COMPETE 2020, Portugal 2020 and European Com-munity through FEDER). We also acknowledge the Portuguese National NMR Network (PTNMR), supported by FCT funds as the NMR spectrometer used is part of PTNMR and partially supported by Infrastructure Project Nº 022161 (co-financed by FEDER through COMPETE 2020, POCI and PORL, and the FCT through PIDDAC). M.V. thanks the FCT and the PhD Program in Medicines and Pharmaceutical Innovation (i3DU) for his PhD grant PD/BD/135460/2017 and T.J.C. thanks FCT for her PhD grant SFRH/BD/145920/2019; both grants were funded by the European Social Fund of the European Union and national funds FCT/MCTES.

Subject:

Subject ID:SU002147
Subject Type:Mammal
Subject Species:Mus musculus
Taxonomy ID:10090
Genotype Strain:BALB/cByJ
Age Or Age Range:6-weeks
Weight Or Weight Range:20.1 g
Gender:Female
Animal Animal Supplier:Charles River Laboratories (France)
Animal Housing:ICBAS-UP Rodent Animal House Facility (Porto, Portugal)
Animal Light Cycle:12h light/dark cycles (7.00 AM lights on)
Animal Feed:ad libitum
Animal Water:ad libitum
Animal Inclusion Criteria:Healthy animails
Species Group:BALB/cByJ

Factors:

Subject type: Mammal; Subject species: Mus musculus (Factor headings shown in green)

mb_sample_id local_sample_id Treatment_group
SA194225healthy_B_EL_B4_2_1_2Cisplatin_12h
SA194226healthy_B_EL_B4_3_1_2Cisplatin_12h
SA194227healthy_B_EL_B4_5_1_2Cisplatin_12h
SA194228healthy_B_EL_B4_1_1_2Cisplatin_12h
SA194229healthy_B_EL_B4_4_1_2Cisplatin_12h
SA194230healthy_B_EL_B2_2_1_2Cisplatin_1h
SA194231healthy_B_EL_B2_4_1_2Cisplatin_1h
SA194232healthy_B_EL_B2_3_1_2Cisplatin_1h
SA194233healthy_B_EL_B2_1_1_2Cisplatin_1h
SA194234healthy_B_EL_B2_5b_1_2Cisplatin_1h
SA194235healthy_B_EL_B6_1b_1_2Cisplatin_48h
SA194236healthy_B_EL_B6_5b_1_2Cisplatin_48h
SA194237healthy_B_EL_B6_4b_1_2Cisplatin_48h
SA194238healthy_B_EL_B6_3b_1_2Cisplatin_48h
SA194239healthy_B_EL_B6_2b_1_2Cisplatin_48h
SA194240healthy_B_EL_A4_4_1_2Control_12h
SA194241healthy_B_EL_A4_3b_1_2Control_12h
SA194242healthy_B_EL_A4_5_1_2Control_12h
SA194243healthy_B_EL_A4_2_1_2Control_12h
SA194244healthy_B_EL_A4_1b_1_2Control_12h
SA194245healthy_B_EL_A2_5_1_2Control_1h
SA194246healthy_B_EL_A2_2b_1_2Control_1h
SA194247healthy_B_EL_A2_3b_1_2Control_1h
SA194248healthy_B_EL_A2_4b_1_2Control_1h
SA194249healthy_B_EL_A2_1b_1_2Control_1h
SA194250healthy_B_EL_A6_3_1_2Control_48h
SA194251healthy_B_EL_A6_4_1_2Control_48h
SA194252healthy_B_EL_A6_2_1_2Control_48h
SA194253healthy_B_EL_A6_1_1_2Control_48h
SA194254healthy_B_EL_C4_1b_1_2Pd2Spermine_12h
SA194255healthy_B_EL_C4_3b_1_2Pd2Spermine_12h
SA194256healthy_B_EL_C4_5_1_2Pd2Spermine_12h
SA194257healthy_B_EL_C4_2_1_2Pd2Spermine_12h
SA194258healthy_B_EL_C4_4b_1_2Pd2Spermine_12h
SA194259healthy_B_EL_C2_2_1_2Pd2Spermine_1h
SA194260healthy_B_EL_C2_5_1_2Pd2Spermine_1h
SA194261healthy_B_EL_C2_1b_1_2Pd2Spermine_1h
SA194262healthy_B_EL_C2_3b_1_2Pd2Spermine_1h
SA194263healthy_B_EL_C2_4_1_2Pd2Spermine_1h
SA194264healthy_B_EL_C6_5_1_2Pd2Spermine_48h
SA194265healthy_B_EL_C6_4c_1_2Pd2Spermine_48h
SA194266healthy_B_EL_C6_2b_1_2Pd2Spermine_48h
SA194267healthy_B_EL_C6_1b_1_2Pd2Spermine_48h
SA194268healthy_B_EL_C6_3c_1_2Pd2Spermine_48h
Showing results 1 to 44 of 44

Collection:

Collection ID:CO002140
Collection Summary:After the respective post-injection time, the mice were sacrificed with pentobarbital injection and the brain was excised, snap-frozen and stored at -80 ºC.
Sample Type:Brain
Storage Conditions:-80℃

Treatment:

Treatment ID:TR002159
Treatment Summary:Fifteen animals per group were injected with single doses of cisplatin (3.5 mg/kg b.w.), Pd2Spermine (3.0 mg/kg b.w.) and phosphate-buffered saline solution as controls (200 uL). Five animals of each group were sacrificed at 1, 12 and 48 h post-injection times.
Treatment Route:Intraperitoneal injection
Treatment Dosevolume:200 uL
Treatment Vehicle:PBS (phosphate-buffered saline solution)

Sample Preparation:

Sampleprep ID:SP002153
Sampleprep Summary:The frontal cortex of each mice brain was mechanically grounded in liquid nitrogen and samples were extracted using the biphasic methanol/ chloroform/ water (2:2:1) method. Lipophilic phases were recovered and dried. Previously to NMR acquisition, lipophilic extracts were suspended in 650 µL of CDCl3, containing 0.03% tetramethylsilane (TMS). Samples were then homogenized and transferred into 5mm NMR tubes.
Processing Storage Conditions:-80℃
Extraction Method:Biphasic method (methanol/ chloroform/ water)
Extract Storage:-80℃

Analysis:

Analysis ID:AN003364
Laboratory Name:Metabolomics Ana M. Gil
Analysis Type:NMR
Acquisition Date:February 2021
Software Version:Topspin 3.2
Results File:matrix_bioimpact_healthy_EL_brain.txt
Units:ppm

NMR:

NMR ID:NM000229
Analysis ID:AN003364
Instrument Name:Avance III TM HD 500MHz
Instrument Type:FT-NMR
NMR Experiment Type:1D-1H
Field Frequency Lock:Deuterated chloroform
Spectrometer Frequency:500MHz
NMR Probe:TXI
NMR Solvent:CDCl3
NMR Tube Size:5mm
Shimming Method:Topshim
Pulse Sequence:"zg" (Bruker library)
Receiver Gain:203
Temperature:298K
Number Of Scans:512
Acquisition Time:2.34s
Relaxation Delay:2s
Spectral Width:7002.801
Zero Filling:64k
Baseline Correction Method:Manual
Chemical Shift Ref Std:TMS (tetramethylsilane)
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