Desarrollo de tratamientos experimentales para pacientes con retinosis pigmentaria / Development of experimental treatments for patients with retinitis pigmentosa

La retinosis pigmentaria es un grupo de enfermedades de origen hereditario que produce la degeneración de la retina y una disminución de la visión. La Organización Mundial de la Salud reporta alrededor de 1.300 millones de personas afectadas por algún tipo de deficiencia visual a nivel mundial. La prevalencia es de 1 por cada 4.000 habitantes y es la primera causa de ceguera de origen genético, frecuente en los varones con un porcentaje del 60% y el 40% en mujeres. Existe falta de información sobre esta patología en el mundo, principalmente sobre los tratamientos existentes para esta enfermedad, por lo que esta revisión bibliográfica tiene como objetivo actualizar los tratamientos existentes o en estudio e informar de las limitaciones que tiene cada una de estas terapias. Se realizó esta revisión de literatura científica mediante la consulta en bases de datos como PubMed y Web of Sciense; la búsqueda se limitó a artículos de los años 2018 al 2022. Existen varios tipos de terapia en estudios: terapia génica, estimulación eléctrica transcorneal, uso de neuroprotectores, terapia optogénica, trasplantes de células madre y terapia con oligonucleótidos, de los que se hablará en este artículo, tanto de sus beneficios como de las barreras existentes en cada tratamiento experimental. En conclusión, cada una de estas terapias promete un tratamiento viable en el futuro para grupos selectivos de personas con retinosis pigmentaria; sin embargo, algunas terapias han demostrado beneficio al inicio de la enfermedad, perdiendo su eficacia a largo plazo (AU)

Retinitis pigmentosa is a group of inherited diseases that lead to degeneration of the retina and decreased vision. The World Health Organization reports around 1300 million people affected by some type of visual impairment worldwide. The prevalence is 1 in every 4000 inhabitants and it is the first cause of blindness of genetic origin, frequent in men with a percentage of 60% and 40% in women. There is a lack of information on this pathology in the world, mainly on the existing treatments for this disease, so this bibliographic review aims to update the existing or under-study treatments and inform the limitations of each of these therapies. This review of scientific literature was carried out by consulting databases such as PubMed and Web of science, the search will be limited to articles from the years 2018 to 2022. There are several types of therapy in studies: gene therapy, transcorneal electrical stimulation, use of neuroprotectors, optogenic therapy, stem cell transplants and oligonucleotide therapy, which will be discussed in this article, both their benefits and the existing barriers in each experimental treatment. In conclusion, each of these therapies promises a viable treatment in the future for selective groups of people with retinitis pigmentosa, however, some therapies have shown benefit at the beginning of the disease, losing their efficacy in the long term (AU)

Development of experimental treatments for patients with retinitis pigmentosa.

Retinitis pigmentosa (RP) is a group of inherited diseases that lead to degeneration of the retina and decreased vision. The World Health Organization reports around 1,300 million people affected by some type of visual impairment worldwide. The prevalence is 1 in every 4000 inhabitants and it is the first cause of blindness of genetic origin, frequent in men with a percentage of 60% and 40% in women. There is a lack of information on this pathology in the world, mainly on the existing treatments for this disease, so this bibliographic review aims to update the existing or under-study treatments and inform the limitations of each of these therapies. This review of scientific literature was carried out by consulting databases such as PubMed and Web of science, the search will be limited to articles from the years 2018-2022. There are several types of therapy in studies: gene therapy, transcorneal electrical stimulation, use of neuroprotectors, optogenic therapy, stem cell transplants and oligonucleotide therapy, which will be discussed in this article, both their benefits and the existing barriers in each treatment experimental. In conclusion, each of these therapies promises a viable treatment in the future for selective groups of people with retinitis pigmentosa, however, some therapies have shown benefit at the beginning of the disease, losing their efficacy in the long term.

Experimental Treatments for Spinal Cord Injury: A Systematic Review and Meta-Analysis.

Spinal cord injury (SCI) is characterized by a complex and prolonged injury process that exacerbates the damage induced by the primary injury and inhibits the potential for regeneration. SCI frequently results in the devastating loss of neurological functions and thus has serious consequences on patient quality of life. Current treatments are limited and focus on early interventions for the acute management of complications. Therefore, the development of novel treatments targeting ongoing injury processes is required to improve SCI outcomes. We aimed to systematically review studies published in the last 10 years that examined experimental treatments with neuroregenerative and neuroprotective capabilities for the improvement of SCI. We analyzed treatments from 44 studies that were identified through a systematic literature search using three databases: PubMed, Web of Science and EMBASE (searched through Ovid). We performed a meta-analysis for Basso-Beattie-Bresnahan (BBB) locomotion test data and collected immunohistochemistry results to demonstrate neuroregenerative and neuroprotective properties of the treatments, respectively. The two treatments that illustrated the most significant improvements in functional recovery using the BBB test were the combined use of tetrahedral framework nucleic acid (tFNA) with neural stem cells (NSCs) and Fortasyn® Connect (FC) supplementation. Both treatments also attenuated secondary injury processes as demonstrated through immunohistochemistry. Combined tFNA with NSCs and FC supplementation are promising treatments for the improvement of SCI as they both demonstrate neuroregenerative and neuroprotective properties. Further pre-clinical testing is required to validate and determine the long-term efficacies of these treatments for the improvement of SCI.

Excitation/Inhibition Modulators in Autism Spectrum Disorder: Current Clinical Research.

Autism spectrum disorder (ASD) is a group of neurodevelopmental disorders characterized by social and communication abnormalities. Heterogeneity in the expression and severity of the core and associated symptoms poses difficulties in classification and the overall clinical approach. Synaptic abnormalities have been observed in preclinical ASD models. They are thought to play a major role in clinical functional abnormalities and might be modified by targeted interventions. An imbalance in excitatory to inhibitory neurotransmission (E/I imbalance), through altered glutamatergic and GABAergic neurotransmission, respectively, is thought to be implicated in the pathogenesis of ASD. Glutamatergic and GABAergic agents have been tested in clinical trials with encouraging results as to efficacy and tolerability. Further studies are needed to confirm the role of E/I modulators in the treatment of ASD and on the safety and efficacy of the current agents.

Endometriosis Pain Management: a Review.

PURPOSE OF REVIEW: The purpose of this review is to summarize the up-to-date pain management options and recommendations for the challenging disease, endometriosis. RECENT FINDINGS: The mainstays of endometriosis advances of both surgical and medical management continue to evolve. Experimental pharmaceuticals include Gestirone, and aromatase inhibitors have shown promise but are still under scrutiny. Surgical techniques include laparoscopic uterosacral nerve ablation/resection and presacral neurectomy. No studies have directly compared medical versus surgical management, and as such, no one treatment modality can be recommend as superior to the other. Patients may initially be given a medical diagnosis and treated with nonsteroidal anti-inflammatory drugs, neurolepitcs, OCP, GNRH agonists/antagonists, and Danazol. Assessing the success of these regimens has proved difficult. Surgical management relies on various methods including excision/ablation of the lesions, nerve ablation, neurectomy, hysterectomy, and oophorectomy.

The past and future of novel, non-dopamine-2 receptor therapeutics for schizophrenia: A critical and comprehensive review.

Since the discovery of chlorpromazine in the 1950's, antipsychotic drugs have been the cornerstone of treatment of schizophrenia, and all attenuate dopamine transmission at the dopamine-2 receptor. Drug development for schizophrenia since that time has led to improvements in side effects and tolerability, and limited improvements in efficacy, with the exception of clozapine. However, the reasons for clozapine's greater efficacy remain unclear, despite the great efforts and resources invested therewith. We performed a comprehensive review of the literature to determine the fate of previously tested, non-dopamine-2 receptor experimental treatments. Overall we included 250 studies in the review from the period 1970 to 2017 including treatments with glutamatergic, serotonergic, cholinergic, neuropeptidergic, hormone-based, dopaminergic, metabolic, vitamin/naturopathic, histaminergic, infection/inflammation-based, and miscellaneous mechanisms. Despite there being several promising targets, such as allosteric modulation of the NMDA and α7 nicotinic receptors, we cannot confidently state that any of the mechanistically novel experimental treatments covered in this review are definitely effective for the treatment of schizophrenia and ready for clinical use. We discuss potential reasons for the relative lack of progress in developing non-dopamine-2 receptor treatments for schizophrenia and provide recommendations for future efforts pursuing novel drug development for schizophrenia.

Adaptive Designs for Non-inferiority Trials with Multiple Experimental Treatments.

The increase in the popularity of non-inferiority clinical trials represents the increasing need to search for substitutes for some reference (standard) treatments. A new treatment would be preferred to the standard treatment if the benefits of adopting it outweigh a possible clinically insignificant reduction in treatment efficacy (non-inferiority margin). Statistical procedures have recently been developed for treatment comparisons in non-inferiority clinical trials that have multiple experimental (new) treatments. An ethical concern for non-inferiority trials is that some patients undergo the less effective treatments; this problem is more serious when multiple experimental treatments are included in a balanced trial in which the sample sizes are the same for all experimental treatments. With the aim of giving fewer patients the inferior treatments, we propose a response-adaptive treatment allocation scheme that is based on the doubly adaptive biased coin design. The proposed adaptive design is also shown to be superior to the balanced design in terms of testing power.

Right to try? fosfoetanolamina, di bella e stamina: uma análise Ítalo-Brasileira / Right to try? phosphoethanolamine, di bella and stamina cases: an Italo-Brazilian analysis

Este trabalho possui como objetivo a análise do fornecimento judicial de medicamentos em fase de teste laboratorial, por meio de um estudo comparado dos casos italianos di Bella e Stamina e do caso brasileiro da fosfoetanolamina da Universidade de São Paulo. Para tanto, foram considerados os percursos judiciais dos três casos, as opiniões doutrinárias e repercussões médicas anunciadas pela mídia e pelos órgãos oficiais interessados. Como resultado, observou-se, no Brasil, uma tendência jurisprudencial que desponta, ainda que não confirmada, no sentido de que a realização do direito à saúde não pode prescindir da segurança médica, afastando-se, em princípio, a obrigação do Estado de fornecer tratamentos experimentais por meio de sua rede de saúde. Na Itália, por outro lado, após a experiência judicial e médica negativa decorrente de dois casos emblemáticos, a Corte Constitucional italiana (Corte Costituzionale) parece ter mudado de orientação, no sentido da não obrigação do fornecimento de tratamento experimental por parte do Servizio Sanitario Nazionale. No âmbito das ações com pretensão de curas compassivas, as normas técnicas, representadas pelas boas práticas clínicas, surgem como zíper de união entre o direito, a ciência e a ética.

This paper reports on an analysis of court orders that determine experimental therapies and provides a comparative study of the Italian Di Bella and Stamina cases and the Brazilian Phosphoethanolamine case. The judicial sentences on the three cases were considered, along with their medical outcome and media repercussion. As a result of the comparison, it was observed that the Brazilian Constitutional Court is tending towards the non-recognition of a “right to try”, even though the Court’s official opinion remains to be seen. In Italy, on the other hand, after the negative judicial and medical experience concerning two emblematic cases, the opinion of the Italian Constitutional Court seems to have changed, indicating that the State is no longer forced to provide experimental therapies through the public health system. In the scope of these judicial lawsuits that claim compassionate cures, the technical framework, represented by the good clinical practices guidelines, comes about as the “zipper” that binds together law, science and ethics.

New experimental treatments for core social domain in autism spectrum disorders.

Current therapeutics in autism spectrum disorders (ASD) only treat the associated symptoms, without addressing core social dysfunctions. A paradigm shift in research of the pathogenesis of ASD, its synaptic abnormalities and altered signaling in multiple dynamic systems, have led to new experimental treatments for treating the core social abnormalities of ASD. NMDA antagonists, especially memantine, have been introduced in clinical trials addressing glutamatergic transmission in children and adolescents with ASD. GABAergic signaling has been targeted in trials using the GABAB receptor agonist arbaclofen for ASD patients with promising results. Oxytocin has been recognized as implicated in social development and affiliative behaviors. Preliminary findings from clinical trials using oxytocin in children with ASD show encouraging improvements in social cognition, but larger studies are needed. In two of the single gene disorders associated with ASD, Insulin Growth Factor (IGF-1) is a new treatment that has been tested in Rett syndrome and Phelan-McDermid syndrome (Chromosome 22 deletion syndrome). IGF-1 has been demonstrated to reverse the reduction in the number of excitatory synapses and the density of neurons that characterize these conditions in animal studies and it is being introduced as an experimental treatment. As a novel approach to verify treatment efficacy, neural processing modifications were recently evaluated by fMRI after a pivotal response training intervention. Another study of neural changes in response to treatment examined variations in EEG signaling in patients after an Early Start Denver Model (ESDM) intervention.

Moving beyond methods: the need for a diverse programme in climate change research.

Understanding effects of climate change on ecosystems will require a diverse range of approaches. We proposed using downscaled climate models to generate realistic weather scenarios as experimental treatments. Kreyling et al. propose a gradient approach to determine the shape of response functions. These approaches are different, but highly complementary.