Data from: Layer-specific proteomic analysis of human hearts in patients with sudden cardiac death
Data files
Feb 18, 2026 version files 13.22 GB
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CH1_I.mznld
244.90 MB
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CH1_M.mznld
241.75 MB
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CH1_O.mznld
245.36 MB
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CH2_I.mznld
250.50 MB
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CH2_M.mznld
246.38 MB
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CH2_O.mznld
244.91 MB
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CH3_I.mznld
245.61 MB
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CH3_M.mznld
242.84 MB
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CH3_O.mznld
246.99 MB
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CH4_I.mznld
245.80 MB
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CH4_M.mznld
248.30 MB
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CH4_O.mznld
245.94 MB
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CH5_I.mznld
251.33 MB
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CH5_M.mznld
246.16 MB
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CH5_O.mznld
246.80 MB
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Ctl1_I.mznld
235.82 MB
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Ctl1_M.mznld
232.82 MB
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Ctl1_O.mznld
240.34 MB
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Ctl2_I.mznld
241.33 MB
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Ctl2_M.mznld
246.24 MB
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Ctl2_O.mznld
239.07 MB
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Ctl3_I.mznld
238.04 MB
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Ctl3_M.mznld
236.85 MB
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Ctl3_O.mznld
244.51 MB
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Ctl4_I.mznld
237.64 MB
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Ctl4_M.mznld
238.01 MB
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Ctl4_O.mznld
236.74 MB
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Ctl5_I.mznld
231.05 MB
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Ctl5_M.mznld
233.85 MB
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Ctl5_O.mznld
230.46 MB
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InnerGroup_protein_quantification.csv
800.31 KB
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MiddleGroup_protein_quantification.csv
757.06 KB
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OuterGroup_protein_quantification.csv
779.66 KB
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README.md
9.76 KB
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SCD1_I.mznld
259.56 MB
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SCD1_M.mznld
249.37 MB
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SCD1_O.mznld
246.60 MB
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SCD2_I.mznld
250.49 MB
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SCD2_M.mznld
248.43 MB
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SCD2_O.mznld
250.75 MB
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SCD3_I.mznld
251.61 MB
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SCD3_M.mznld
250.40 MB
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SCD3_O.mznld
260.42 MB
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SCD4_I.mznld
252.28 MB
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SCD4_M.mznld
246.88 MB
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SCD4_O.mznld
250.77 MB
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SCD5_I.mznld
247.24 MB
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SCD5_M.mznld
246.43 MB
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SCD5_O.mznld
244.39 MB
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SCD6_I.mznld
245.21 MB
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SCD6_M.mznld
242.62 MB
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SCD6_O.mznld
241.04 MB
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SCD7_I.mznld
241.77 MB
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SCD7_M.mznld
258.04 MB
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SCD7_O.mznld
248.02 MB
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SCD8_I.mznld
243.65 MB
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SCD8_M.mznld
243.01 MB
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SCD8_O.mznld
242.76 MB
Abstract
Recent studies have shown that decreased longitudinal strain in speckle-tracking echography can predict sudden cardiac death (SCD) in patients with cardiac hypertrophy (CH). Histologically, the heart wall consists of the inner longitudinal, middle circular, and outer longitudinal layers. Thus, layer-specific proteomic changes may contribute to SCD risk. The three layers in human cardiac tissues were obtained during autopsies of SCD, compensated CH, and control cases (18 cases aged > 40 years, 54 samples in total). SCD cases consisted of patients with ischemic or hypertensive heart failure, whereas CH and control cases were accidental deaths. After histological analysis, cardiomyocytes were collected separately from the three layers of the left ventricular wall using laser microdissection. The extracted proteins were analyzed using liquid chromatography–tandem mass spectrometry, followed by label-free quantification. Histologically, cardiomyocytes were enlarged in all layers of SCD and CH cases without significant progression of myocardial fibrosis. The proteomic profiles of SCD and CH cases were distinguishable from those of control cases, especially in the inner layer. The levels of mitochondrial and calcium-handling proteins were significantly decreased in SCD hearts. Arrhythmogenic changes, including decreased PKP2 and RYR2 levels, developed in a stepwise manner from control through CH to SCD, most prominently in the inner layer. Immunohistochemical analysis showed reduced levels of PKP2 in intercalated disks and RYR2 in sarcomeres. Because proteomic alterations precede the progression of myocardial fibrosis, their detection may enhance the accuracy of postmortem diagnosis of SCD in middle-aged and older asymptomatic individuals with CH.
Dataset DOI: 10.5061/dryad.q573n5tx2
Description of the data and file structure
Proteome profiles were individually determined by using a Q Exactive mass spectrometer (Thermo Fisher Scientific) equipped with an UltiMate 3000 LC system (Thermo Fisher Scientific). All patients were divided into three groups: SCD, CH, and Control. All samples were dissected from three myocardial layers: inner longitudinal layer (I), middle circular layer (M), and outer longitudinal layer (O) using laser microdissection (LMD 6500; Leica Microsystems, Wetzlar, Germany)
Note: The mznld files contain raw MS data, while the three CSV files contain processed quantitative protein data extracted from those mznld files. Each CSV file contains protein-level quantification results for one myocardial layer.
Description of the data and file structure
File name includes sample group and layer information.
For example: SCD1_I.mznld: "SCD1" corresponds tothe sample group, and id "I"corresponds to the layer (Inner longitudinal layer, Middle circular layer, er and Outer longitudinal layer)
The .mznld files are raw data export files generated by Progenesis QI for Proteomics. Each heart was dissected into three myocardial layers before proteomic analysis.
They contain:
- MS1 full scan spectra (300–1500 m/z)
- MS/MS (HCD) spectra of the top 20 most abundant precursor ions
- Peptide peak lists
- Quantitative intensity information
- Alignment and normalization data
- Protein inference information
Files and variables
File: SCD1_I.mznld
Description: SCD, inner layer
File: SCD2_I.mznld
Description: SCD, inner layer
File: CH1_I.mznld
Description: CH, inner layer
File: SCD3_I.mznld
Description: SCD, inner layer
File: SCD4_I.mznld
Description: SCD, inner layer
File: CH2_I.mznld
Description: CH, inner layer
File: SCD5_I.mznld
Description: SCD, inner layer
File: CH3_I.mznld
Description: CH, inner layer
File: SCD6_I.mznld
Description: SCD, inner layer
File: CH4_I.mznld
Description: CH, inner layer
File: SCD7_I.mznld
Description: SCD, inner layer
File: SCD8_I.mznld
Description: SCD, inner layer
File: CH5_I.mznld
Description: CH, inner layer
File: SCD1_M.mznld
Description: SCD, middle layer
File: SCD2_M.mznld
Description: SCD, middle layer
File: CH1_M.mznld
Description: CH, middle layer
File: SCD3_M.mznld
Description: SCD, middle layer
File: SCD4_M.mznld
Description: SCD, middle layer
File: CH2_M.mznld
Description: CH, middle layer
File: SCD5_M.mznld
Description: SCD, middle layer
File: CH3_M.mznld
Description: CH, middle layer
File: SCD6_M.mznld
Description: SCD, middle layer
File: CH4_M.mznld
Description: CH, middle layer
File: SCD8_M.mznld
Description: SCD, middle layer
File: SCD7_M.mznld
Description: SCD, middle layer
File: CH5_M.mznld
Description: CH, middle layer
File: SCD1_O.mznld
Description: SCD, outer layer
File: SCD2_O.mznld
Description: SCD, outer layer
File: CH1_O.mznld
Description: CH, outer layer
File: SCD3_O.mznld
Description: SCD, outer layer
File: SCD4_O.mznld
Description: SCD, outer layer
File: CH2_O.mznld
Description: CH, outer layer
File: SCD5_O.mznld
Description: SCD, outer layer
File: CH3_O.mznld
Description: CH, outer layer
File: CH4_O.mznld
Description: CH, outer layer
File: SCD6_O.mznld
Description: SCD, outer layer
File: SCD7_O.mznld
Description: SCD, outer layer
File: SCD8_O.mznld
Description: SCD, outer layer
File: CH5_O.mznld
Description: CH, outer layer
File: Ctl1_I.mznld
Description: Control, inner layer
File: Ctl2_I.mznld
Description: Control, inner layer
File: Ctl3_I.mznld
Description: Control, inner layer
File: Ctl4_I.mznld
Description: Control, inner layer
File: Ctl5_I.mznld
Description: Control, inner layer
File: Ctl1_M.mznld
Description: Control, middle layer
File: Ctl2_M.mznld
Description: Control, middle layer
File: Ctl3_M.mznld
Description: Control, middle layer
File: Ctl4_M.mznld
Description: Control, middle layer
File: Ctl5_M.mznld
Description: Control, middle layer
File: Ctl1_O.mznld
Description: Control, outer layer
File: Ctl2_O.mznld
Description: Control, outer layer
File: Ctl3_O.mznld
Description: Control, outer layer
File: Ctl4_O.mznld
Description: Control, outer layer
File: Ctl5_O.mznld
Description: Control, outer layer
File: InnerGroup_protein_quantification.csv
Description:
Protein quantification in the inner layer group.
Variable List:
- Accession: UniProt/Swiss-Prot database identifier.
- Peptide counts: The number of peptide sequences assigned to the corresponding protein.
- Unique peptides: The number of unique peptide sequences among the peptides counted for the corresponding protein.
- Confidence score: The protein confidence score is calculated as the sum of the identification scores of the assigned peptides.
- Anova (p): The p-value obtained from a one-way analysis of variance (ANOVA).
- q Value: Corrected p-value.
- Max fold change: The fold change between the condition with the highest mean abundance and the condition with the lowest mean abundance.
- Power: Statistical power for ANOVA.
- Highest mean condition: The condition showing the highest mean protein abundance.
- Lowest mean condition: The condition showing the lowest mean protein abundance.
- Description: The protein name corresponding to the accession number.
- Normalized abundance: The summed abundance of peptide-derived peaks used for protein quantification after normalization in the inner group.
- Raw abundance: The total abundance of peptide-derived peaks used for protein quantification before normalization in the inner group.
- Spectral counts: The total number of peptide spectral counts prior to normalization in the inner group.
File: MiddleGroup_protein_quantification.csv
Description:
Protein quantification in the middle layer group.
Variable List:
- Accession: UniProt/Swiss-Prot database identifier.
- Peptide counts: The number of peptide sequences assigned to the corresponding protein.
- Unique peptides: The number of unique peptide sequences among the peptides counted for the corresponding protein.
- Confidence score: The protein confidence score is calculated as the sum of the identification scores of the assigned peptides.
- Anova (p): The p-value obtained from a one-way analysis of variance (ANOVA).
- q Value: Corrected p-value.
- Max fold change: The fold change between the condition with the highest mean abundance and the condition with the lowest mean abundance.
- Power: Statistical power for ANOVA.
- Highest mean condition: The condition showing the highest mean protein abundance.
- Lowest mean condition: The condition showing the lowest mean protein abundance.
- Description: The protein name corresponding to the accession number.
- Normalized abundance: The summed abundance of peptide-derived peaks used for protein quantification after normalization in the middle group.
- Raw abundance: The total abundance of peptide-derived peaks used for protein quantification before normalization in the middle group.
- Spectral counts: The total number of peptide spectral counts prior to normalization in the middle group.
File: OuterGroup_protein_quantification.csv
Description:
Protein quantification in the outer layer group.
Variable List:
- Accession: UniProt/Swiss-Prot database identifier.
- Peptide counts: The number of peptide sequences assigned to the corresponding protein.
- Unique peptides: The number of unique peptide sequences among the peptides counted for the corresponding protein.
- Confidence score: The protein confidence score is calculated as the sum of the identification scores of the assigned peptides.
- Anova (p): The p-value obtained from a one-way analysis of variance (ANOVA).
- q Value: Corrected p-value.
- Max fold change: The fold change between the condition with the highest mean abundance and the condition with the lowest mean abundance.
- Power: Statistical power for ANOVA.
- Highest mean condition: The condition showing the highest mean protein abundance.
- Lowest mean condition: The condition showing the lowest mean protein abundance.
- Description: The protein name corresponding to the accession number.
- Normalized abundance: The summed abundance of peptide-derived peaks used for protein quantification after normalization in the outer group.
- Raw abundance: The total abundance of peptide-derived peaks used for protein quantification before normalization in the outer group.
- Spectral counts: The total number of peptide spectral counts prior to normalization in the outer group.
Code/software
The mass spectrometer was operated using Xcalibur software. Full-scan MS spectra were measured from 300 to 1,500 m/z, and each of the 20 most abundant ions was subsequently subjected to HCD product ion scans. For protein and peptide identification, peak lists and exported mznld files were generated using Progenesis QI for proteomics.
We have also extracted the MS information from the mznld files and placed it in tabular data documents using Progenesis QI for proteomics. The data in Excel format is available in three CSV files.
Human subjects data
Written informed consent for the academic use of the tissue was obtained from the relatives of all decedents included in the study, and the study was approved by the institutional ethics committee (approval number: 21R177). This study was conducted in accordance with the ethical standards of the 1964 Declaration of Helsinki and its subsequent amendments.