Biobank Kohorten
BBMRI.at Partnerbiobanken beherbergen Millionen von Proben und zugehörigen Daten zu verschiedenen Krankheiten und Gesundheitszuständen.
Mehr als 20 Millionen Proben von über 30 Jahren Sammlung werden bei den BBMRI.at Partnerbiobanken gelagert. Jährlich kommen fast eine Million neue Proben dazu.
Diese Proben (Mensch, Tier) repräsentieren alle bekannten Krankheiten in ihrer natürlichen Häufigkeit und umfassen auch gesunde Proben.
Zu den wichtigsten Probentypen gehören in Formalin fixiertes, in Paraffin eingebettetes (FFPE) und frisch eingefrorenes Gewebe, Flüssigproben (Serum, Plasma, Vollblut, Urin, Stuhl, Liquor, Follikel- und Samenflüssigkeit usw.), gefärbte Gewebeschnitte und digitale (ganzer Schnitt) Bilder von H&E- oder immunhistochemisch gefärbten Gewebeschnitten.
Mehr Informationen über die Proben und wie Sie Kontakt zu den Partnerbiobanken von BBMRI.at aufnehmen können.
oder schreiben sie ein Email an [email protected]
(Kontaktperson: Cornelia Stumptner, BBMRI.at)
Einige der vielen besonderen Sammlungen werden hier beschrieben (auf Englisch)
„CoVVac Study: COVID-19 vaccination cohort“
An outstanding sample collection at Biobank Graz (Med Uni Graz)
„Lighthouse collection: COVID-19 Convalescent Cohort“
An exceptional sample collection at Biobank Graz (Med Uni Graz) which is based on a prospective sample cohort for current research on SARS-CoV-2
„Lighthouse collection: Feline Lymphoma Cohort“
An exceptional sample collection at VetBiobank Vienna (University of Veterinary Medicine, Vienna)
„Lighthouse collection: Colorectal Cancer Whole Slide Image – Survival Cohort“
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
„Lighthouse collection: Colorectal Cancer Whole Slide Image – Vascular Invasion Cohort“
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
„Lighthouse collection: Colorectal Cancer Whole Slide Image – Clinical Annotation Cohort“
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
„Paracelsus 10,000 Cohort“
An outstanding population-based collection at BBMRI.at partner PMU / SALK
„LEAD Cohort (Austrian LEAD Study)“
An outstanding collection at BBMRI.at partner MedUni Wien Biobank
„BioPersMed Cohort“
An outstanding interdisciplinary sample collection at Biobank Graz
„PoCOsteo Osteoporosis Cohort“
An outstanding osteoporosis sample collection at Biobank Graz (Med Uni Graz)
„PERFORM Cohort“
An outstanding sample collection at Biobank Graz (Med Uni Graz)
„INTERFAST Cohort“
An outstanding sample collection at Biobank Graz (Med Uni Graz)
The CoVVac Study: COVID-19 vaccination cohort
An outstanding sample collection at Biobank Graz (Med Uni Graz) based on a prospective sample cohort for current research on immune response to COVID-19 vaccines in immunocompromised and healthy individuals.
Study design
This study will characterize and analyze the anit-SARS-CoV-2 humoral and cellular immune response before and after vaccination with a focus on the anti-spike protein response in immunocompromised patients compared to healthy controls. Participants are invited to five visits where samples are collected and one telephone interview:
- 1st visit (60-0 days before vaccination)
- 2nd „visit“ is a telephone interview to get information on vaccine reactions.
- 3rd visit (+21-28 days after 2nd vaccination)
- 4th visit (+6 months after 2nd vaccination)
- 5th visit (+3-6 weeks after visit 4 or 3rd vaccination)
- 6th visit (+6 months after visit 4)
Profile of The CoVVac Study:
COVID-19
COVID-19 vaccination, immunocompromised, t-cell immunity, t-cell aging, antibodies
- Serum and saliva (stored at -80 °C)
- PBMC (stored in the gas phase of liquid nitrogen)
Samples will be collected from 189 immunocompromised and 187 healthy controls (6 visits planned)
1371 serum aliquots from 348 participants (May 2021)
- Healthy
- Primary or secondary immunodeficiencies (M05, D38, M34, C90, C91.1, C92, D46)
Serology, immune status, T-cell immunity, nutritive assessment, body fat composition, BMI, date and type of COVID-19 vaccinations, vaccine reactions, medical history, current medication, smoking habits
12/2021
Quality management: ISO 9001:2015 (SOPs)
Principle Investigator: Assoz. Prof. Priv.-Doz. Dr.med.univ. Martin Stradner ([email protected])
- E Schulz et al. CD19+IgD+CD27- Naïve B Cells as Predictors of Humoral Response to COVID 19 mRNA Vaccination in Immunocompromised Patients; Front. Immunol., 07 December 2021, DOI: 10.3389/fimmu.2021.803742 PMID: 34950155
- ORF Report (Wissenschaft) „Wie wirkt CoV-Impfung bei Immunschwäche?“ (15 Dec 2021)
Lighthouse collection: COVID-19 Convalescent Cohort
An exceptional sample collection at Biobank Graz (Med Uni Graz) which is based on a prospective sample cohort for current research on SARS-CoV-2
Summary
Biobank Graz recruited participants (from Austria) who had recovered from COVID-19 and grouped them into two sub cohorts (see profile table). Volunteers were invited to fill in a questionnaire and donate various types of samples at different time points (see study design and table).
This cohort serves for
- the development and validation of new antibody tests and neutralization assays
- the investigation of antibody titres over time
- a better characterization of the course of COVID-19
- the identification of diagnostic or prognostic biomarkers
Study design
Participants are invited five times, i.e. 1st visit (time point 0), 2nd visit (after 1 month), 3rd visit (after 2 months), 4th visit (after 5 months), 5th visit (after 12 months), where the samples are collected. At the 1st visit, donors also fill in a questionnaire concerning symptoms, comorbidities, pre-history and lifestyle.
Profile of the COVID-19 Convalescent Cohort:
COVID-19
COVID-19 recovered patients, SARS-CoV-2, PCR test, antibody test
Serum, EDTA buffy coat, EDTA plasma, lithium heparin plasma, sodium citrate plasma, saliva and nasopharyngeal swabs (stored at -80 °C)
23.739 aliquots from 364 participants as of March 10th
Volunteers who recovered from COVID-19
Sub cohort I (342 participants):
- Persons who were officially tested positive for an infection by PCR test with the SARS-CoV-2 virus, showed symptoms of COVID-19 and recovered.
Sub cohort II (22 participants):
- Persons who lived together or got in contact with a person officially tested positive by PCR test for SARS-CoV-2 and showed symptoms of COVID-19 disease within 14 days, but were not tested themselves, and recovered.
- Persons who showed leading COVID-19 symptoms (fever, dry cough, loss of smell or taste, diarrhoea, fatigue) since December 2019, but were not tested themselves, independent of whether they had contact to a person positive tested for SARS-CoV-2, and recovered.
- Data concerning symptoms, comorbidities, prehistory and lifestyle are collected via questionnaire
- PCR tests and antibody tests are performed
As of now
- Quality management: ISO 9001:2015 (SOPs)
- CEN/TS 16945:2016 (metabolomics in urine, venous blood serum and plasma)
Principle Investigator: Univ.-Prof. Dr. med. univ. Robert Krause ([email protected])
- Kral S, Banfi C, Niedrist T, Sareban N, Guelly C, Kriegl L, Schiffmann S, Zurl C, Herrmann M, Steinmetz I, Schlenke P, Berghold A, Krause R. Long-lasting immune response to a mild course of PCR-confirmed SARS-CoV-2 infection: A cohort study. J Infect. 2021 Nov;83(5):607-635. doi: 10.1016/j.jinf.2021.08.030. PMID: 34433071.
- Niedrist T, Drexler C, Torreiter PP, Matejka J, Strahlhofer-Augsten M, Kral S, Riegler S, Gülly C, Zurl C, Kriegl L, Krause R, Berghold A, Steinmetz I, Schlenke P, Herrmann M. Longitudinal comparison of automated SARS-CoV-2 serology assays in assessing virus neutralization capacity in COVID-19 convalescent sera. Arch Pathol Lab Med. 2022 Jan 27. doi: 10.5858/arpa.2021-0604-SA. PMID: 35085385.
- Eva M. Matzhold, Günther F. Körmöczi, Chiara Banfi, Marlies Schönbacher, Camilla Drexler, Helmberg, Ivo Steinmetz, Andrea Berghold, Peter Schlenke, Gabriel E. Wagner,
Anja Stoisser, Barbara Kleinhappl, Wolfgang R. Mayr and Thomas Wagner. Lower Levels of ABO Anti-A and Anti-B of IgM, IgG and IgA Isotypes in the Serum but Not the Saliva of COVID-19 Convalescents. J. Clin. Med. 2022, 11(15), 4513, doi: 10.3390/jcm11154513. PMID: 35956128.
Lighthouse collection: Feline Lymphoma Cohort
An exceptional sample collection at VetBiobank Vienna (University of Veterinary Medicine, Vienna)
Summary
Lymphoma is the most common tumor in cats. This neoplasia can develop in every tissue; however, the gastrointestinal tract is in contrast to dogs and people the most frequent localization in the feline species.
The prognosis for cats suffering from intermediate or high-grade lymphoma is still poor and research in this important veterinary area continues to be under-resourced.
The clinical cohort comprises neutered and unneutered male and female patients between 7 months and 15 years. Biospecimens are collected according SOPs. Tissue samples are collected in line with the ISO standards 20166 and 20184 and are therefore suitable for molecular investigations.
Profile of the feline lymphoma cohort:
Lymphoma in cats
Fixed and native samples from tumor and healthy reference tissues (FFPE, glutaraldehyde for electron microscopy, OCT, RNAlater, pure), serum, plasma, urine, feces
Complete set of samples and data with follow up examination for 36 patients available; collection start February 2016 – collection ongoing
untreated, treated
Clinical data (anamnesis, treatment: medication, surgical intervention, laboratory results, imaging data..), sample management data, images from HE stains
Approved by the patient owner
Internal academic research, external academic research, industrial research – cooperation prerred
Tissue samples were collected according to the sample pre-analytics standards: CEN/TS 16826 1-2, CEN/TS 16827 1-3
- Sample Coordinator: VetBiobank, Ingrid Walter ([email protected])
- Principle investigator: Birgitt Wolfesberger ([email protected])
Lighthouse collection: Colorectal Cancer Whole Slide Image – Survival Cohort“
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
Summary
The „Colorectal Cancer Cohort (CRC-Cohort)“ is a huge collection of colorectal cancer resection samples from the Institute of Pathology located at Biobank Graz at Medical University of Graz. It consists of various CRC sub-cohorts from colorectal cancer tissue with associated H&E, histological and immunhistochemical stainings where samples have been analysed and supplemented by digital images of tissue slides in various projects.
A very well sub-cohort is the „Colorectal cancer whole slide image cohort“ (CRC WSI cohort) which consists of 3 parts, i.e.:
1. „CRC whole slide image – survival cohort“
2. „CRC whole slide image – vascular invasion cohort“
3. „CRC whole slide image – clinical annotation cohort“
Profile of (1) "CRC whole slide image - survival cohort": This cohort was/is part of several industrial research collaborations e.g. with Google and Roche Diagnostics
Colorectal cancer / ICD-10: C18.0
Colorectal cancer, survival prediction, artificial Intelligence, etc.
- H&E stained FFPE tissue slides (RT storage)
- Immunohistochemistry (IHC) on FFPE tissue slides (RT storage)
- Whole slide images of H&E and IHC FFPE tissue slides
Over 180.000 images (resolution 0.25µm/pixel, over 800 TByte) from 100 000 slides (H&E and IHC staining of FFPE tissue sections) from over 6 400 cases comprising tissue from colorectal cancer resections (tumour and non-tumour colon tissue, resection margins, fatty tissue, and associated lymph nodes)
Inclusion criteria:
- Patients with colorectal cancer as a primary diagnosis (C18), samples from 1984 to 2013
- Patient age: 18 – 100 years
- Tumour stages: II to III
- Ratio female : male = 45:55
- Pathology diagnosis
- TNM staging
- ICD-10 and ICD-O codes
- Survival data
- Meta data from whole slide images
Depending on year of collection with or without informed consent
Access for collaborative research projects depending on ethics committee approval of Medical University of Graz
ISO 9001:2015 (Biobank Graz)
- Wulczyn E, Steiner DF, Moran M, Plass M, Reihs R, Tan F, Flament-Auvigne I, Brown T, Regitnig P, Chen PC, Hegde N, Sadhwani A, MacDonald R, Ayalew B, Corrado GS, Peng LH, Tse D, Müller H, Xu Z, Liu Y, Stumpe MC, Zatloukal K: Interpretable survival prediction for colorectal cancer using deep learning. Mermel CH. NPJ Digit Med. 2021 Apr 19;4(1):71. DOI: 10.1038/s41746-021-00427-2, PMID: 33875798.
- L’Imperio V, Wulczyn E, Plass M et al.: Pathologist Validation of a Machine Learning-Derived Feature for Colon Cancer Risk Stratification. JAMA Netw Open. 2023;6(3):e2254891. DOI:10.1001/jamanetworkopen.2022.54891, PMID: 36917112
- Media article about research collaboration of Med Uni Graz and Google on revolutionary findings with relevance for diagnostics: algorithms are declaring war on cancer (Kleine Zeitung 2021)
Industry collaboration
Univ.-Prof. Dr. med. univ. Kurt Zatloukal ([email protected])
Lighthouse collection: Colorectal Cancer Whole Slide Image – Vascular Invasion Cohort
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
Summary
The „Colorectal Cancer Cohort (CRC-Cohort)“ is a huge collection of colorectal cancer resection samples from the Institute of Pathology located at Biobank Graz at Medical University of Graz. It consists of various CRC sub-cohorts from colorectal cancer tissue with associated H&E, histological and immunhistochemical stainings where samples have been analysed and supplemented by digital images of tissue slides in various projects.
A very well sub-cohort is the „Colorectal cancer whole slide image cohort“ (CRC WSI cohort) which consists of 3 parts, i.e.:
1. „CRC whole slide image – survival cohort“
2. „CRC whole slide image – vascular invasion cohort“
3. „CRC whole slide image – clinical annotation cohort“
Profile of (2) "CRC whole slide image - vascular invasion cohort": Sub-collection of the CRC collection that was part of the EU H2020 project ADOPT BBMRI-ERIC (grant agreement number: 676550)
Colorectal cancer / ICD-10: C18.0
Colorectal cancer, survival prediction, artificial Intelligence, etc.
- H&E stained FFPE tissue slides (RT storage)
- (Immuno)histochemistry (IHC) on FFPE tissue slides, Elastica van Giesson staining, vascular endothelial marker IHC (CD-31) (RT storage)
- Whole slide images of H&E and IHC FFPE tissue slides
Approx. 800 whole slide images (resolution 0.25µm/pixel) from ~ 800 slides (H&E, histochemical and IHC staining of FFPE tissue sections) from over 260 cases comprising colorectal tumour tissue
Inclusion criteria:
- Patients with colorectal cancer as a primary diagnosis (C18), samples from 1984 to 2013
- Patient age: 18 – 100 years
- Tumour stages: I to IV
- Female, male
- Pathology diagnosis
- TNM staging
- ICD-10 and ICD-O codes
- Clinical data
- Survival data
- Meta data from whole slide images
Depending on year of collection with or without informed consent
Access for collaborative research projects depending on ethics committee approval of Medical University of Graz
ISO 9001:2015 (Biobank Graz)
Univ.-Prof. Dr. med. univ. Kurt Zatloukal ([email protected])
Sub-collection of the CRC collection that was part of the EU H2020 project ADOPT BBMRI-ERIC (grant agreement number 676550)
Lighthouse collection: Colorectal Cancer Whole Slide Image – Clinical Annotation Cohort
An exceptional collection by Diagnostic & Research Institute of Pathology at Biobank Graz (both Med Uni Graz)
Summary
The „Colorectal Cancer Cohort (CRC-Cohort)“ is a huge collection of colorectal cancer resection samples from the Institute of Pathology located at Biobank Graz at Medical University of Graz. It consists of various CRC sub-cohorts from colorectal cancer tissue with associated H&E, histological and immunhistochemical stainings where samples have been analysed and supplemented by digital images of tissue slides in various projects.
A very well sub-cohort is the „Colorectal cancer whole slide image cohort“ (CRC WSI cohort) which consists of 3 parts, i.e.:
1. „CRC whole slide image – survival cohort“
2. „CRC whole slide image – vascular invasion cohort“
3. „CRC whole slide image – clinical annotation cohort“
Profile of (3) "CRC whole slide image - clinical annotation cohort": Sub-collection of the CRC collection that was part of the EU H2020 project ADOPT BBMRI-ERIC (grant agreement number: 676550)
Colorectal cancer / ICD-10: C18.0
Colorectal cancer, survival prediction, artificial Intelligence, etc.
- H&E stained FFPE tissue slides (RT storage)
- Immunohistochemistry (IHC) on FFPE tissue slides (RT storage)
- Whole slide images of H&E and IHC FFPE tissue slides
Approx. 1800 whole slide images (resolution 0.25µm/pixel) from ~800 slides (H&E and IHC staining of FFPE tissue sections) from over 100 cases comprising tissue from colorectal cancer resections (tumour and non-tumour colon tissue, resection margins, fatty tissue, and associated lymph nodes)
Inclusion criteria:
- Patients with colorectal cancer as a primary diagnosis (C18), samples from 1984 to 2013
- Age: 18 – 100 years
- Stages: II and III
- Female, male
- Pathology diagnosis
- TNM staging
- ICD-10 and ICD-O codes
- Clinical data
- Survival data
- Meta data from whole slide images
Depending on year of collection with or without informed consent
Access for collaborative research projects depending on ethics committee approval of Medical University of Graz
ISO 9001:2015 (Biobank Graz)
Univ.-Prof. Dr. med. univ. Kurt Zatloukal ([email protected])
Sub-collection of the CRC collection that was part of the EU H2020 project ADOPT BBMRI-ERIC (grant agreement number 676550)
*Data associated with ADOPT CRC Cohort:
- Sex
- Participation in clinical study (yes/no)
- Age at primary diagnosis
- Time of recurrence (metastasis)
- Family history of cancer
- Other diseases: other cancers, Inflammatory bowel disease, intestinal polyps, other disease requiring therapy (e.g., cardio-vascular, endocrine. musculoskeletal)
- Tumor markers (e.g., CEA) (if available)
- Vital status and survival information: timestamp of last update of vital status, overall survival status
- Surgery: time difference between initial diagnosis and surgery, surgery radicality, type of surgery
- Pharmacotherapy (REQUIRED if occurred): start of pharmacotherapy (relative date referring to the primary diagnosis), scheme of pharmacotherapy
- Targeted therapy (REQUIRED if occurred): start of targeted therapy (relative date referring to the primary diagnosis), end of targeted therapy (relative date referring to the primary diagnosis)
- Radiation therapy (REQUIRED if occurred): start of radiotherapy (relative date referring to the primary diagnosis), end of radiotherapy (relative date referring to the primary diagnosis)
- Response to therapy: specific response; the response is linked to the patient and specified by a timestamp. This is to avoid need to specify to which therapy the response is, since there might be combination of different therapies
- Molecular markers (if available): Microsatellite instability, Mismatch repair gene expression – IHC array for different genes (common for 3; if applicable), risk situation (only HNPCC), RAS mutation status (if applicable), BRAF, PIC3CA. HER2 mutation status (optional)
- Histopathology: pTNM, UICC staging, WHO grading, histological classification (according to WHO), localization of the tumor, high resolution digital images (resolution < 0.25 Microns/pixel) of the tumor, resection margin and lymph nodes
- Diagnostic exam: result of colonoscopy, array of diagnostic methods (results of liver imaging, lung imaging, MRI, CT; if occurred)
Paracelsus 10,000 Cohort
An outstanding population-based collection at BBMRI.at partner PMU / SALK
Summary
Paracelsus 10,000 Cohort is a population-based collection from 5,000 male and 5,000 female probands from Salzburg (Austria). It comprises numerous different types of samples and data from diverse analyses and different follow up visits.
Purpose of this cohort is to serve the following study aims:
- Collection of valid epidemiological data on the state of health of the Salzburg population
- Clarification of the interaction of genetic disposition and lifestyle factors in the development of degenerative diseases
- Development of well-directed prevention processes for the population of Salzburg
- Strengthening of the research location Salzburg and Austria
Profile of the Paracelsus 10,000 Cohort:
Plasma (EDTA, citrate and heparin), serum, EDTA blood for DNA isolation, buffy Coat, urine, stool samples
Representative sample of 10 000 participants (5.000 male, 5.000 female) by 03/2020
- 40-49 years: 2700 participants
- 50-59 years: 4300 participants
- 60-69 years: 3000 participants
From the city of Salzburg and surrounding townships
Male-female ratio 1:1
1. Basic investigations of all participants:
- Questionnaires on diet, exercise, socio-economic anamnesis, depression, cognitive performance, quality of life, stress and environmental factors
- Anthropometry: height, weight, abdominal girth
- Resting blood pressure, heart rate, resting 12-channel ECG
- Laboratory parameters: Lipid profile, Apo-B, Apo-AI, Lp(a), FBS, HbA1c, Electrolytes, CR, Urea, LFT, Fe-Status, hsCRP, fibrinogen, BC, TSH, PSA (men), Fasting-Insulin
- Urine: chemistry, albumin/creatinine ratio
- Ultrasound of the carotides
2. Additional investigations for the intensively phenotyped subgroup (50 to 59 years):
- Laboratory parameters: fasting proinsulin, free fatty acids, adiponectin, vitamin D
- Determination of insulin sensitivity and beta cell function by frequently sampled OGTT (with simultaneous determination of insulin, C-peptide and blood glucose at the time points 0 min., 30 min., 60 min., 90 min. and 120 min.)
- Pulmonary function test
- Pulse wave analysis
- Multi-frequency body composition B.I.A.
- Measurement of intima-media thickness and plaque score of carotid arteries
- Measurement of the coronary artery calcium score
- 24h blood pressure measurement
- 7-day nutrition protocol
- 7-day movement monitoring using movement sensors
- Ankle-brachial index
- Hand grip
- 6 meter walking test
3. Additional investigations for two participants per day (50 to 59 years):
- Coronary Ca-score
- Body fat distribution and bone density (measured with DEXA-scan)
- Ergospirometry
- Ultrasound of the liver
- Prof. Dr. Bernhard Paulweber ([email protected])
- Dr. Ludmilla Kedenko PhD ([email protected])
Vanessa Natalie Frey, Patrick Langthaler, Emanuel Raphaelis et al. Paracelsus 10,000: A Prospective Cohort Study Based On The Population of Salzburg, Austria. Rationale, Objectives And Study Design, 17 August 2021, PREPRINT (Version 1). doi: 10.21203/rs.3.rs-740574/v1.
LEAD Cohort (Austrian LEAD Study)
An outstanding collection at BBMRI.at partner MedUni Wien Biobank
Summary
The Biobank of the Medical University of Vienna harbours the sample cohort of the „Austrian LEAD-Study“ collected at the Ludwig Bolzmann Institute. It is a population based cohort and one of the largest long-term studies in Austria on the topic of lung health.
The Lung, hEart, sociAl, boDy (LEAD) Study is a longitudinal, observational, epidemiological cohort study aiming to investigate respiratory health through life. The survey includes a representative sample of the Austrian general population between 6 and 80 years of age and focuses on three areas:
- Normal and pathologic lung growth and development (natural history of lung function).
- Genetic, environmental and socioeconomic risk factors for abnormal lung function.
- Extrapulmonary manifestations of abnormal lung function and related comorbidities (cardiovascular disease, metabolic disorders, depression and anxiety).
BioPersMed Cohort
An outstanding interdisciplinary sample collection at Biobank Graz
Summary
„BioPersMed“ stands for „Biomarkers for Personalised Medicine in Common Metabolic Disorders.
This prospectively collected cohort comprises a huge number of samples and data being collected and used since 2010 (still ongoing). Aim is to detect and define specific characteristics and personalized biomarkers of patients at risk for cardiovascular and metabolic diseases and to follow them for future developments.
The „BioPersMed Cohort“ includes the research areas endocrinology & metabolism and cardiology. Diabetes, fatty liver disease, osteoporosis or cardiovascular diseases are only some of the topics in the focus of this cohort.
The samples meet the requirements of the sample quality standards „CEN/TC 140 Molecular in vitro diagnostic examinations – Specifications for preexamination processes (CEN/TS) for metabolomics in urine, venous blood serum and plasma“ (CEN/TS 16945:2016) that were published by the European Committee for Standardization (CEN).
Profile of the BioPersMed Cohort:
Diabetes, fatty liver disease, osteoporosis, cardiovascular diseases
Biomarker, endocrinology, metabolism, cardiology
Plasma (EDTA, Lithium Heparin, Sodium Citrate), serum, buffy coat; urine, 24h urine of healthy and diseased patients
- 1,024 probands (in 4 follow-up visits): healthy and diseased
- >220,000 aliquots (as per March 2018)
collection ongoing
- Healthy and diseased
- Age: adults 35+ years
- Gender: 50/50 female/male
Clinical records/diagnosis, smoking and lifestyle anamnesis, follow-up laboratory results, follow-up clinical data
Cooperation only
- Sample quality: CEN/TS 16945:2016 – Molecular in vitro diagnostic examinations. Specifications for pre-examination processes for metabolomics in urine, venous blood serum and plasma
- Quality management: ISO 9001:2015 (SOPs)
- Scientific director: Barbara Obermayer-Pietsch ([email protected])
- Partners: Thomas Pieber, Karine Sargsyan, Albrecht Schmidt ([email protected])
PoCOsteo Osteoporosis Cohort
An outstanding osteoporosis sample collection at Biobank Graz (Med Uni Graz)
Summary
„PoCOsteo“ stands for Point-of-care in-office device for identifying individuals at high risk of Osteoporosis and osteoporotic fracture.
It is being collected (starting May 2018) in the context of the HORIZON 2020 project PoCOsteo (Proposal number 767325) which aims at developing point-of-care in-vitro devices to measure and/or quantify proteomic and genomic factors in human whole blood.
The clinical cohort includes male and female patients fifty years and above and ranges from healthy (per definition) to those who experienced multiple fragility fractures due to secondary osteoporosis.
It comprises untreated patients as well as those treated for osteoporosis, with or without concomitant diseases such as hypertension, diabetes etc.
The samples meet the requirements of the sample quality standards „CEN/TC 140 Molecular in vitro diagnostic examinations – Specifications for preexamination processes (CEN/TS) for metabolomics in urine, venous blood serum and plasma“ (CEN/TS 16945:2016) that were published by the European Committee for Standardization (CEN).
Profile of the PoCOsteo Cohort:
Endocrinology, osteoporosis, osteoporotic fractures
Biomarker development & detection
Serum, EDTA-plasma and buffy coat (stored at -80°C)
1,000 probands
Collection start in May 2018 – collection ongoing
- Healthy and diseased, treated and untreated for osteoporosis with or without concomitant diseases (e.g. hypertension, diabetes, …)
- Age: adults > 50 years
- Gender: female and male
From the following time-points:
- study inclusion
- after 12 months
- possibly after 24 months
Bone mineral density (BMD) of the hip and the lumbar spine as well as vertebral fracture assessment (VFA) by Dual X-ray absorptiometry (DXA), grip strength (hydraulic hand dynamometer), and a routine blood test including renal and hepatic parameters together with a lipid profile
Cooperation preferred
- Sample quality: CEN/TS 16945:2016 – Molecular in vitro diagnostic examinations. Specifications for pre-examination processes for metabolomics in urine, venous blood serum and plasma
- Quality management: ISO 9001:2015 (SOPs)
Principle Investigator: Hans Dimai, Medical University of Graz, Department of Internal Medicine, Division of Endocrinology and Metabolism ([email protected], [email protected])
PERFORM Cohort
An outstanding sample collection at Biobank Graz (Med Uni Graz)
Summary
„PERFORM“ stands for Personalised Risk assessment in Febrile illness to Optimise Real-life Management across the European Union. It represents a pediatric cohort of samples from children and is collected in the context of the PERFORM EU Horizon 2020 project.
The collection aims to improve the diagnostics in febrile children and adolescents and to develop a comprehensive management plan for febrile patients in Europe. It helps to improve the diagnostics in febrile children and adolescents.
The „PERFORM cohort“ comprises PAXgene stabilized and EDTA blood samples (whole blood, plasma, pellet), cerebrospinal fluid, throat swab, urine and stool. It includes children below the age of 18 (both genders) with i) fever >38ºC, or a history of fever (within 3 days), or ii) suspected of infection.
Profile of PERFORM Cohort:
Febrile illness
ETDA blood (plasma, pellet and whole blood), blood in PAXgene tubes, cerebrospinal fluid, throat swab, urine, and stool stored at -80°C
Samples from 500 patients
Children <18 years
- with fever >38ºC, or a history of fever (within 3 days), in whom the attending clinician determines the need for blood sampling or whom parents give consent for bloods taken for research purposes
- suspected of infection (included: full spectrum of disease severity, and with co-morbidities)
Specific study IC
Cooperation only
Quality management: ISO 9001:2015 (SOPs)
ORF Report „Lebensbedrohlich krank: Neuer Schnelltest“
Principle Investigator: Univ. Prof. Dr. Werner Zenz, Pediatric and Adolescent University Hospital, Department of General Pediatrics Medical University of Graz ([email protected], [email protected])
INTERFAST Cohort
An outstanding sample collection at Biobank Graz (Med Uni Graz)
Summary
„INTERFAST“ stands for Intermittent Fasting (i.e. a dietary regimen of alternating fasting and „feeding“ cycles, e.g. practised by alternate day fasting). The INTERFAST collection represents cohort of blood and urine samples from healthy donors who have undergone different types of intermittent fasting and is collected in the context of the INTERFAST project (www.interfast.at).
The cohort supports studies that aim to investigate the effects of repeating fasting periods on human physiology, aging process and molecular cellular processes in humans.
This includes both studying
- long term effects of fasting (as donors are included in the cohort, who already practice alternate day fasting (ADF) for a defined time period) as well as
- short term effects of this nutritional intervention (i.e. intermittent fasting)
The INTERFAST cohort comprises serum, plasma and urine samples.
Profile of the INTERFAST Cohort:
Intermittent fasting, alternate day fasting (ADF), effects on autophagy, human physiology, aging process and molecular-cellular processes
Serum, plasma and urine samples stored at -80°C
90 donors:
- 30 subjects cohort – 2 study visits
- 60 subjects RCT – 4 study visits
Cohort (Alternate day fasting for at least 6 months before the start of the trial – 30 subjects) as well as randomized control-trial (60 subjects – randomized to either intervention group (alternate day fasting) or control group with no intervention 1:1).
- Adults 35 – 65 years; ratio female:male = 57:43
Further inclusion criteria: - Body mass index in the range of 22.0 – 30.0 kg/m2
- Fasting blood glucose <110mg/dL (without medication)
- LDL-cholesterol <180 mg/dL (without medication)
- Blood pressure <140/90 mmHg (without medication)
- Stable weight (change <± 10%) for 3 months immediately
Exclusion criteria: see INTERFAST cohort details
- Demographics
- Medical history
- Concomitant medication
- Vital signs
- Physical examination
- Blood sampling with oral glucose tolerance test (oGTT)
- Electrocardiogram (ECG)
Cooperation preferred
Quality management: ISO 9001:2015 (SOPs)
Principle Investigator: Assoz. Prof. Dr. Harald Sourij ([email protected])
„Intermittent Fasting (Alternate Day Fasting) in Healthy, Non-obese Adults: Protocol for a Cohort Trial with an Embedded Randomized Controlled Pilot Trial“ (Advances in Therapy, August 2018, Volume 35, Issue 8) PMID: 30046988.