Spatial detection of fetal marker genes expressed at low level in adult human heart tissue.
Michaela AspFredrik SalménPatrik L StåhlSanja VickovicUlrika FelldinMarie LöflingJosé Fernandez NavarroJonas MaaskolaMaria J ErikssonBengt PerssonMatthias CorbascioHans PerssonCecilia LindeJoakim LundebergPublished in: Scientific reports (2017)
Heart failure is a major health problem linked to poor quality of life and high mortality rates. Hence, novel biomarkers, such as fetal marker genes with low expression levels, could potentially differentiate disease states in order to improve therapy. In many studies on heart failure, cardiac biopsies have been analyzed as uniform pieces of tissue with bulk techniques, but this homogenization approach can mask medically relevant phenotypes occurring only in isolated parts of the tissue. This study examines such spatial variations within and between regions of cardiac biopsies. In contrast to standard RNA sequencing, this approach provides a spatially resolved transcriptome- and tissue-wide perspective of the adult human heart, and enables detection of fetal marker genes expressed by minor subpopulations of cells within the tissue. Analysis of patients with heart failure, with preserved ejection fraction, demonstrated spatially divergent expression of fetal genes in cardiac biopsies.
Keyphrases
- heart failure
- genome wide
- left ventricular
- poor prognosis
- endothelial cells
- atrial fibrillation
- healthcare
- public health
- single cell
- gene expression
- mental health
- type diabetes
- magnetic resonance
- bioinformatics analysis
- magnetic resonance imaging
- cardiovascular disease
- dna methylation
- oxidative stress
- coronary artery disease
- obstructive sleep apnea
- computed tomography
- risk assessment
- cell proliferation
- cardiac resynchronization therapy
- social media
- contrast enhanced
- pi k akt
- positive airway pressure