Tubular cell polyploidy protects from lethal acute kidney injury but promotes consequent chronic kidney disease.
Letizia De ChiaraCarolina ConteRoberto SemeraroPaula Diaz-BulnesMaria Lucia AngelottiBenedetta MazzinghiAlice MolliGiulia AntonelliSamuela LandiniMaria Elena MelicaAnna Julie PeiredLaura MaggiMarta DonatiGilda La ReginaMarco AllinoviFiammetta RavagliaDaniele GuastiDaniele BaniLuigi CirilloFrancesca BecherucciFrancesco GuzziAlberto MagiFrancesco AnnunziatoLaura LasagniHans-Joachim AndersElena LazzeriPaola RomagnaniPublished in: Nature communications (2022)
Acute kidney injury (AKI) is frequent, often fatal and, for lack of specific therapies, can leave survivors with chronic kidney disease (CKD). We characterize the distribution of tubular cells (TC) undergoing polyploidy along AKI by DNA content analysis and single cell RNA-sequencing. Furthermore, we study the functional roles of polyploidization using transgenic models and drug interventions. We identify YAP1-driven TC polyploidization outside the site of injury as a rapid way to sustain residual kidney function early during AKI. This survival mechanism comes at the cost of senescence of polyploid TC promoting interstitial fibrosis and CKD in AKI survivors. However, targeting TC polyploidization after the early AKI phase can prevent AKI-CKD transition without influencing AKI lethality. Senolytic treatment prevents CKD by blocking repeated TC polyploidization cycles. These results revise the current pathophysiological concept of how the kidney responds to acute injury and identify a novel druggable target to improve prognosis in AKI survivors.
Keyphrases
- acute kidney injury
- chronic kidney disease
- cardiac surgery
- end stage renal disease
- single cell
- young adults
- rna seq
- induced apoptosis
- liver failure
- cell proliferation
- cancer therapy
- single molecule
- cell death
- dna damage
- drug induced
- electronic health record
- quantum dots
- bone marrow
- adverse drug
- loop mediated isothermal amplification