Universitat de Barcelona. Departament de Genètica, Microbiologia i Estadística
[eng] Inherited Retinal Dystrophies (IRDs) are a clinically and genetically highly heterogeneous group of genetic pathologies characterized by progressive attrition of photoreceptor cells and other retinal neurons, which eventually leads to vision loss. The retina, the most affected tissue in IRDs, is the specialized region of the central nervous system capable of transducing light into neural signals. This neurosensory tissue is particularly susceptible to genetic and environmental alterations due to its highly active metabolism, external location, and daily light irradiation. Therefore, the disturbance of the balance between retinal resilience systems and endogenous and exogenous stress factors eventually leads to several alterations that underlie the pathogenesis of many IRDs, such as mitochondrial dysfunction, misregulated autophagy, and activation of cell death pathways. CERKL (CERamide Kinase-Like) mutations cause two different IRDs in humans: Retinitis Pigmentosa and Cone-Rod Dystrophy. While the precise role of CERKL remains unclear, numerous studies have proposed CERKL as a resilience gene against oxidative stress, by participating in the formation of stress granules, regulation of the antioxidant protein TRX2 and inhibition of oxidative stress-induced apoptosis, among other functions. Previous work from our research group led to the generation of the CerklKD/KO mouse model, characterised by a strong deficiency in the expression of Cerkl. This model mimics the disease progression of CERKL-associated Retinitis Pigmentosa-affected patients, showing a slow and progressive loss of photoreceptors and, ultimately, vision impairment. Taking advantage of the CerklKD/KO mouse model, we aimed to dissect CERKL function in mitochondrial metabolism and dynamics. Our findings describe a pool of CERKL isoforms colocalizing with mitochondria. In addition, we observed accumulation of fragmented mitochondria and mitochondrial bioenergetics dysfunction in CerklKD/KO retinas. Moreover, mitochondrial distribution and trafficking were reduced in retinal and hippocampal neurons upon Cerkl depletion, reflecting the important role of CERKL in the regulation of mitochondrial network morphology and energy production. Furthermore, we sought to analyse the impact of CERKL downregulation on stress response and activation of photoreceptor death mechanisms upon light/oxidative stress. Data collected from CERKL silencing and overexpression experiments in ARPE-19 cells (derived from retinal pigment epithelium) revealed that CERKL exerts a protective role maintaining the mitochondrial network morphology against oxidative damage. Additionally, using CerklKD/KO albino mouse models, we assessed immediate (early) or after two weeks (late) retinal stress response to light injury, using data from transcriptomics, metabolomics, and immunohistochemistry images. Our results showed that Cerkl depletion causes an exacerbated response to stress in basal conditions, through alterations in glutathione metabolism and stress granule production. Consequently, upon light-stress exposure, CerklKD/KO retinas cannot cope with additional stress factors, resulting in increased ROS levels and the subsequent activation of several cell death mechanisms. To sum up, our studies indicate that Cerkl gene is a novel player in regulating mitochondrial organization and metabolism, together with light-challenged retinal homeostasis, thus suggesting that CERKL mutations cause blindness by impairing the mitochondrial homeostasis and oxidative stress response in the retina. These findings contributed to determine early phenotypic biomarkers of the Cerkl-depleted mouse retina, which will be compared and confirmed with those observed in retinal organoids derived from CERKLR257X patient-derived hiPSCs (currently under differentiation). Altogether, these studies will allow us to test the feasibility of genetic rescue using a proof-of-principle AAV-based gene augmentation therapy for CERKL-associated IRDs, as well as novel gene delivery systems using gold nanoparticles as vectors. The principal area of cooperation of this Thesis in the Sustainable Development Goals (SDGs) is related to the SDG 3: “Good health and well-being” according to the point 3.8: “Achieve universal health coverage, including financial risk protection, access to quality essential health-care services and access to safe, effective, quality and affordable essential medicines and vaccines for all”. Moreover, an important part of our findings was result of fruitful collaborations with groups with high expertise in other areas. Therefore, the objectives of this work are also related to SDG 17: “Partnerships for the goals” according to the point 17.6: “Knowledge sharing and cooperation for access to science, technology and innovation”. Finally, this PhD Thesis has been directed, supervised and tutorized by women, Dr Gemma Marfany and Dr Serena Mirra, and our research group has also been mostly composed of female scientists during many years, contributing to SDG 5: “Gender equity and empowering of girls and women” according to the point 5.5: “Assure effective and full participation of women and equity in leadership opportunities at all deciding levels in politic, economic and public life”.
[spa] La retina, el tejido neurosensorial que transduce luz en señales nerviosas, es particularmente susceptible a alteraciones genéticas y ambientales, las cuales pueden sobrepasar los sistemas de resiliencia celular, provocando alteraciones patogénicas causantes de distrofias hereditarias de retina (IRDs). En humanos, mutaciones en el gen CERKL (CERamide Kinase-Like) causan Retinosis Pigmentaria y Distrofia de Conos y Bastones, dos IRDs caracterizadas por la muerte progresiva de fotorreceptores y pérdida de visión. Aunque su función exacta es de hiPSCs de pacientes. Así podremos evaluar el potencial rescate fenotípico tras aplicar terapia basada en AAV-CERKL.desconocida, se ha propuesto que CERKL es un gen de resiliencia a estrés oxidativo. Usando el modelo CerklKD/KO, que expresa menos del 10% de Cerkl –y sufre la muerte progresiva de fotorreceptores con la consiguiente pérdida de visión–, nuestro objetivo ha sido la disección de la función de CERKL en el metabolismo y dinámica mitocondriales, tanto en condiciones basales como en respuesta al estrés oxidativo/lumínico. Hemos descrito la localización de un conjunto de isoformas de CERKL en mitocondria, además de la acumulación de mitocondrias fragmentadas y disfuncionales en retinas CerklKD/KO. Asimismo, las neuronas CerklKD/KO presentan alteraciones en la distribución y tráfico mitocondriales. Además, la sobreexpresión de CERKL in vitro protege la red mitocondrial del estrés oxidativo, reflejando la importancia de CERKL en la regulación de la morfología y bioenergética mitocondriales. También hemos evaluado la respuesta a estrés lumínico en ratones albinos CerklKD/KO, observando una respuesta exacerbada en condiciones basales, con alteraciones en el metabolismo del glutatión y producción de gránulos de estrés. Consecuentemente, ante estrés lumínico, las retinas CerklKD/KO no pueden sobrellevar un daño adicional, causando un incremento en especies reactivas de oxígeno y activación de mecanismos de muerte celular. En conclusión, nuestros estudios postulan el gen CERKL como un nuevo regulador de la organización y metabolismo mitocondriales, así como de la homeostasis retinal frente a estrés lumínico, indicando que las mutaciones en CERKL causan ceguera al desestabilizar estos sistemas en la retina. Estos resultados han contribuido a determinar biomarcadores tempranos en las retinas CerklKD/KO, que serán comparados y confirmados con los observados en organoides de retina derivados de hiPSCs de pacientes. Así podremos evaluar el potencial rescate fenotípico tras aplicar terapia basada en AAV-CERKL.
Teràpia genètica; Terapia genética; Gene therapy; Malalties de la retina; Enfermedades de la retina; Retinal diseases; Mitocondris; Mitocondrias; Mitochondria; Estrès (Fisiologia); Estrés (Fisiología); Stress (Physiology)
575 - General genetics. General cytogenetics. Immunogenetics. Evolution. Phylogeny
Ciències Experimentals i Matemàtiques
Programa de Doctorat en Genètica