Your search keyword '"De Leon-Oliva, Diego"' showing total 16 results

1. Placental Tissue Calcification and Its Molecular Pathways in Female Patients with Late-Onset Preeclampsia.

Author

Ortega, Miguel A., Pekarek, Tatiana, De Leon-Oliva, Diego, Boaru, Diego Liviu, Fraile-Martinez, Oscar, García-Montero, Cielo, Bujan, Julia, Pekarek, Leonel, Barrena-Blázquez, Silvestra, Gragera, Raquel, Rodríguez-Benitez, Patrocinio, Hernández-Fernández, Mauricio, López-González, Laura, Díaz-Pedrero, Raul, Asúnsolo, Ángel, Álvarez-Mon, Melchor, García-Honduvilla, Natalio, Saez, Miguel A., De León-Luis, Juan A., and Bravo, Coral

Abstract

Preeclampsia (PE) is a complex multisystem disease characterized by hypertension of sudden onset (>20 weeks' gestation) coupled with the presence of at least one additional complication, such as proteinuria, maternal organ dysfunction, or uteroplacental dysfunction. Hypertensive states during pregnancy carry life-threatening risks for both mother and baby. The pathogenesis of PE develops due to a dysfunctional placenta with aberrant architecture that releases factors contributing to endothelial dysfunction, an antiangiogenic state, increased oxidative stress, and maternal inflammatory responses. Previous studies have shown a correlation between grade 3 placental calcifications and an elevated risk of developing PE at term. However, little is known about the molecular pathways leading to placental calcification. In this work, we studied the gene and protein expression of c-Jun N-terminal kinase (JNK), Runt-related transcription factor 2 (RUNX2), osteocalcin (OSC), osteopontin (OSP), pigment epithelium-derived factor (PEDF), MSX-2/HOX8, SOX-9, WNT-1, and β-catenin in placental tissue from women with late-onset PE (LO-PE). In addition, we employed von Kossa staining to detect mineral deposits in placental tissues. Our results show a significant increase of all these components in placentas from women with LO-PE. Therefore, our study suggests that LO-PE may be associated with the activation of molecular pathways of placental calcification. These results could be the starting point for future research to describe the molecular mechanisms that promote placental calcification in PE and the development of therapeutic strategies directed against it. [ABSTRACT FROM AUTHOR]

Published

2024

2. Abnormal Histopathological Expression of Klotho, Ferroptosis, and Circadian Clock Regulators in Pancreatic Ductal Adenocarcinoma: Prognostic Implications and Correlation Analyses.

Author

García-Montero, Cielo, Fraile-Martinez, Oscar, Cobo-Prieto, David, De Leon-Oliva, Diego, Boaru, Diego Liviu, De Castro-Martinez, Patricia, Pekarek, Leonel, Gragera, Raquel, Hernández-Fernández, Mauricio, Guijarro, Luis G., Toledo-Lobo, María Del Val, López-González, Laura, Díaz-Pedrero, Raul, Monserrat, Jorge, Álvarez-Mon, Melchor, Saez, Miguel A., and Ortega, Miguel A.

Subjects

PANCREATIC duct, PROGNOSIS, INVERSE relationships (Mathematics), STATISTICAL correlation, REGRESSION analysis, CIRCADIAN rhythms

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an extremely lethal tumor with increasing incidence, presenting numerous clinical challenges. The histopathological examination of novel, unexplored biomarkers offers a promising avenue for research, with significant translational potential for improving patient outcomes. In this study, we evaluated the prognostic significance of ferroptosis markers (TFRC, ALOX-5, ACSL-4, and GPX-4), circadian clock regulators (CLOCK, BMAL1, PER1, PER2), and KLOTHO in a retrospective cohort of 41 patients deceased by PDAC. Immunohistochemical techniques (IHC) and multiple statistical analyses (Kaplan–Meier curves, correlograms, and multinomial linear regression models) were performed. Our findings reveal that ferroptosis markers are directly associated with PDAC mortality, while circadian regulators and KLOTHO are inversely associated. Notably, TFRC emerged as the strongest risk marker associated with mortality (HR = 35.905), whereas CLOCK was identified as the most significant protective marker (HR = 0.01832). Correlation analyses indicate that ferroptosis markers are positively correlated with each other, as are circadian regulators, which also positively correlate with KLOTHO expression. In contrast, KLOTHO and circadian regulators exhibit inverse correlations with ferroptosis markers. Among the clinical variables examined, only the presence of chronic pathologies showed an association with the expression patterns of several proteins studied. These findings underscore the complexity of PDAC pathogenesis and highlight the need for further research into the specific molecular mechanisms driving disease progression. [ABSTRACT FROM AUTHOR]

Published

2024

3. Exacerbated Activation of the NLRP3 Inflammasome in the Placentas from Women Who Developed Chronic Venous Disease during Pregnancy.

Author

Sánchez-Gil, María Asunción, Fraile-Martinez, Oscar, García-Montero, Cielo, De Leon-Oliva, Diego, Boaru, Diego Liviu, De Castro-Martinez, Patricia, Camacho-Alcázar, Adrían, De León-Luis, Juan A., Bravo, Coral, Díaz-Pedrero, Raúl, López-Gonzalez, Laura, Bujan, Julia, Cancelo, María J., Álvarez-Mon, Melchor, García-Honduvilla, Natalio, Saez, Miguel A., and Ortega, Miguel A.

Subjects

NLRP3 protein, INFLAMMASOMES, PLACENTA, CHRONIC diseases, PYRIN (Protein), PLACENTA diseases, PREGNANCY, WNT signal transduction, PROTEIN expression

Abstract

Chronic venous disease (CVD) comprises a spectrum of morphofunctional disorders affecting the venous system, affecting approximately 1 in 3 women during gestation. Emerging evidence highlights diverse maternofetal implications stemming from CVD, particularly impacting the placenta. While systemic inflammation has been associated with pregnancy-related CVD, preliminary findings suggest a potential link between this condition and exacerbated inflammation in the placental tissue. Inflammasomes are major orchestrators of immune responses and inflammation in different organs and systems. Notwithstanding the relevance of inflammasomes, specifically the NLRP3 (nucleotide-binding domain, leucine-rich-containing family, pyrin domain-containing-3)- which has been demonstrated in the placentas of women with different obstetric complications, the precise involvement of this component in the placentas of women with CVD remains to be explored. This study employs immunohistochemistry and real-time PCR (RT-qPCR) to examine the gene and protein expression of key components in both canonical and non-canonical pathways of the NLRP3 inflammasome (NLRP3, ASC—apoptosis-associated speck-like protein containing a C-terminal caspase recruitment domain—caspase 1, caspase 5, caspase 8, and interleukin 1β) within the placental tissue of women affected by CVD. Our findings reveal a substantial upregulation of these components in CVD-affected placentas, indicating a potential pathophysiological role of the NLRP3 inflammasome in the development of this condition. Subsequent investigations should focus on assessing translational interventions addressing this dysregulation in affected patient populations. [ABSTRACT FROM AUTHOR]

Published

2024

4. Vascular Calcification: Molecular Networking, Pathological Implications and Translational Opportunities.

Author

Ortega, Miguel A., De Leon-Oliva, Diego, Gimeno-Longas, Maria José, Boaru, Diego Liviu, Fraile-Martinez, Oscar, García-Montero, Cielo, de Castro, Amador Velazquez, Barrena-Blázquez, Silvestra, López-González, Laura, Amor, Silvia, García-Honduvilla, Natalio, Buján, Julia, Guijarro, Luis G., Castillo-Ruiz, Elisa, Álvarez-Mon, Miguel Ángel, Albillos, Agustin, Álvarez-Mon, Melchor, Diaz, Raul, and Saez, Miguel A.

Subjects

*ARTERIAL calcification, *PERICYTES, *NOTCH genes, *VASCULAR smooth muscle, *CELL anatomy, *PERIPHERAL vascular diseases, *MUSCLE cells

Abstract

Calcification is a process of accumulation of calcium in tissues and deposition of calcium salts by the crystallization of PO43− and ionized calcium (Ca2+). It is a crucial process in the development of bones and teeth. However, pathological calcification can occur in almost any soft tissue of the organism. The better studied is vascular calcification, where calcium salts can accumulate in the intima or medial layer or in aortic valves, and it is associated with higher mortality and cardiovascular events, including myocardial infarction, stroke, aortic and peripheral artery disease (PAD), and diabetes or chronic kidney disease (CKD), among others. The process involves an intricate interplay of different cellular components, endothelial cells (ECs), vascular smooth muscle cells (VSMCs), fibroblasts, and pericytes, concurrent with the activation of several signaling pathways, calcium, Wnt, BMP/Smad, and Notch, and the regulation by different molecular mediators, growth factors (GFs), osteogenic factors and matrix vesicles (MVs). In the present review, we aim to explore the cellular players, molecular pathways, biomarkers, and clinical treatment strategies associated with vascular calcification to provide a current and comprehensive overview of the topic. [ABSTRACT FROM AUTHOR]

Published

2024

5. Advanced Hydrogel-Based Strategies for Enhanced Bone and Cartilage Regeneration: A Comprehensive Review.

Author

De Leon-Oliva, Diego, Boaru, Diego Liviu, Perez-Exposito, Roque Emilio, Fraile-Martinez, Oscar, García-Montero, Cielo, Diaz, Raul, Bujan, Julia, García-Honduvilla, Natalio, Lopez-Gonzalez, Laura, Álvarez-Mon, Melchor, Saz, Jose V., de la Torre, Basilio, and Ortega, Miguel A.

Subjects

HYDROGELS, CARTILAGE, BONE regeneration, OSTEOARTHRITIS, EXTRACELLULAR matrix

Abstract

Bone and cartilage tissue play multiple roles in the organism, including kinematic support, protection of organs, and hematopoiesis. Bone and, above all, cartilaginous tissues present an inherently limited capacity for self-regeneration. The increasing prevalence of disorders affecting these crucial tissues, such as bone fractures, bone metastases, osteoporosis, or osteoarthritis, underscores the urgent imperative to investigate therapeutic strategies capable of effectively addressing the challenges associated with their degeneration and damage. In this context, the emerging field of tissue engineering and regenerative medicine (TERM) has made important contributions through the development of advanced hydrogels. These crosslinked three-dimensional networks can retain substantial amounts of water, thus mimicking the natural extracellular matrix (ECM). Hydrogels exhibit exceptional biocompatibility, customizable mechanical properties, and the ability to encapsulate bioactive molecules and cells. In addition, they can be meticulously tailored to the specific needs of each patient, providing a promising alternative to conventional surgical procedures and reducing the risk of subsequent adverse reactions. However, some issues need to be addressed, such as lack of mechanical strength, inconsistent properties, and low-cell viability. This review describes the structure and regeneration of bone and cartilage tissue. Then, we present an overview of hydrogels, including their classification, synthesis, and biomedical applications. Following this, we review the most relevant and recent advanced hydrogels in TERM for bone and cartilage tissue regeneration. [ABSTRACT FROM AUTHOR]

Published

2023

6. Exploring the Role of Mediterranean and Westernized Diets and Their Main Nutrients in the Modulation of Oxidative Stress in the Placenta: A Narrative Review.

Author

García-Montero, Cielo, Fraile-Martinez, Oscar, De Leon-Oliva, Diego, Boaru, Diego Liviu, Garcia-Puente, Luis M., De León-Luis, Juan A., Bravo, Coral, Diaz-Pedrero, Raul, Lopez-Gonzalez, Laura, Álvarez-Mon, Melchor, García-Honduvilla, Natalio, Saez, Miguel A., and Ortega, Miguel A.

Subjects

OXIDATIVE stress, MEDITERRANEAN diet, MONOUNSATURATED fatty acids, FETAL growth retardation, PLACENTA, UNSATURATED fatty acids, NUTRIENT uptake

Abstract

Oxidative stress is a major cellular event that occurs in the placenta, fulfilling critical physiological roles in non-pathological pregnancies. However, exacerbated oxidative stress is a pivotal feature of different obstetric complications, like pre-eclampsia, fetal growth restriction, and other diseases. Compelling evidence supports the relevant role of diet during pregnancy, with pleiotropic consequences for maternal well-being. The present review aims to examine the complex background between oxidative stress and placental development and function in physiological conditions, also intending to understand the relationship between different dietary patterns and the human placenta, particularly how this could influence oxidative stress processes. The effects of Westernized diets (WDs) and high-fat diets (HFDs) rich in ultra-processed foods and different additives are compared with healthy patterns such as a Mediterranean diet (MedDiet) abundant in omega 3 polyunsaturated fatty acids, monounsaturated fatty acids, polyphenols, dietary fiber, and vitamins. Although multiple studies have focused on the role of specific nutrients, mostly in animal models and in vitro, further observational and intervention studies focusing on the placental structure and function in women with different dietary patterns should be conducted to understand the precise influence of diet on this organ. [ABSTRACT FROM AUTHOR]

Published

2023

7. The RANK–RANKL–OPG System: A Multifaceted Regulator of Homeostasis, Immunity, and Cancer.

Author

De Leon-Oliva, Diego, Barrena-Blázquez, Silvestra, Jiménez-Álvarez, Laura, Fraile-Martinez, Oscar, García-Montero, Cielo, López-González, Laura, Torres-Carranza, Diego, García-Puente, Luis M., Carranza, Sara T., Álvarez-Mon, Miguel Ángel, Álvarez-Mon, Melchor, Diaz, Raul, and Ortega, Miguel A.

Subjects

HOMEOSTASIS, BONE growth, EPITHELIAL cells, BONE resorption, DENDRITIC cells

Abstract

The RANK–RANKL–OPG system is a complex signaling pathway that plays a critical role in bone metabolism, mammary epithelial cell development, immune function, and cancer. RANKL is a ligand that binds to RANK, a receptor expressed on osteoclasts, dendritic cells, T cells, and other cells. RANKL signaling promotes osteoclast differentiation and activation, which leads to bone resorption. OPG is a decoy receptor that binds to RANKL and inhibits its signaling. In cancer cells, RANKL expression is often increased, which can lead to increased bone resorption and the development of bone metastases. RANKL-neutralizing antibodies, such as denosumab, have been shown to be effective in the treatment of skeletal-related events, including osteoporosis or bone metastases, and cancer. This review will provide a comprehensive overview of the functions of the RANK–RANKL–OPG system in bone metabolism, mammary epithelial cells, immune function, and cancer, together with the potential therapeutic implications of the RANK–RANKL pathway for cancer management. [ABSTRACT FROM AUTHOR]

Published

2023

8. Is Insulin Receptor Substrate4 (IRS4) a Platform Involved in the Activation of Several Oncogenes?

Author

Guijarro, Luis G., Justo Bermejo, Francisco Javier, Boaru, Diego Liviu, De Castro-Martinez, Patricia, De Leon-Oliva, Diego, Fraile-Martínez, Oscar, Garcia-Montero, Cielo, Alvarez-Mon, Melchor, Toledo-Lobo, María del Val, and Ortega, Miguel A.

Subjects

BIOMARKERS, PHOSPHOTRANSFERASES, SIGNAL peptides, CELL physiology, DRUG design, INSULIN, CELLULAR signal transduction, GENE expression, PROTEIN-tyrosine kinases, TUMORS, MITOGEN-activated protein kinases, CARRIER proteins

Abstract

Simple Summary: IRS4 (insulin receptor substrate4) belongs to a family of intracellular proteins that include IRS1 and IRS2 and whose physiological function is to transmit the effects of insulin and IGF1 inside the cell. IRS4 is the least studied of this family, and its expression has recently been shown to be increased in many types of cancer. IRS4 serves to connect different signaling pathways, such as MAP kinases and PI3K/AKT. In addition, it has been observed that it is capable of activating several oncogenes, such as BRK (breast tumor kinase) and feline sarcoma-related protein (FER). Increased IRS4 expression in cancer cells may be due to changes in the regulatory region of the gene or increased chromosomal aberrations. Our objective has been to carry out a review to assess the possibility that IRS4 behaves as a meeting point for different oncogene signaling pathways, which we have called the oncogene platform. The IRS (insulin receptor substrate) family of scaffold proteins includes insulin receptor substrate-4 (IRS4), which is expressed only in a few cell lines, including human kidney, brain, liver, and thymus and some cell lines. Its N-terminus carries a phosphotyrosine-binding (PTB) domain and a pleckstrin homology domain (PH), which distinguishes it as a member of this family. In this paper, we collected data about the molecular mechanisms that explain the relevance of IRS4 in the development of cancer and identify IRS4 differences that distinguish it from IRS1 and IRS2. Search engines and different databases, such as PubMed, UniProt, ENSEMBL and SCANSITE 4.0, were used. We used the name of the protein that it encodes "(IRS-4 or IRS4)", or the combination of these terms with the word "(cancer)" or "(human)", for searches. Terms related to specific tumor pathologies ("breast", "ovary", "colon", "lung", "lymphoma", etc.) were also used. Despite the lack of knowledge on IRS4, it has been reported that some cancers and benign tumors are characterized by high levels of IRS-4 expression. Specifically, the role of IRS-4 in different types of digestive tract neoplasms, gynecological tumors, lung cancers, melanomas, hematological tumors, and other less common types of cancers has been shown. IRS4 differs from IRS1 and IRS2 in that can activate several oncogenes that regulate the PI3K/Akt cascade, such as BRK and FER, which are characterized by tyrosine kinase-like activity without regulation via extracellular ligands. In addition, IRS4 can activate the CRKL oncogene, which is an adapter protein that regulates the MAP kinase cascade. Knowledge of the role played by IRS4 in cancers at the molecular level, specifically as a platform for oncogenes, may enable the identification and validation of new therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2023

9. Unraveling the New Perspectives on Antimicrobial Hydrogels: State-of-the-Art and Translational Applications.

Author

Ortega, Miguel A., De Leon-Oliva, Diego, Boaru, Diego Liviu, Fraile-Martinez, Oscar, García-Montero, Cielo, Diaz, Raul, Coca, Santiago, Barrena-Blázquez, Silvestra, Bujan, Julia, García-Honduvilla, Natalio, Saez, Miguel A., Álvarez-Mon, Melchor, and Saz, Jose V.

Subjects

ANTI-infective agents, HYDROGELS in medicine, TRANSLATIONAL research, DRUG resistance in bacteria, BIOMATERIALS, BIOCOMPATIBILITY

Abstract

The growing impact of infections and the rapid emergence of antibiotic resistance represent a public health concern worldwide. The exponential development in the field of biomaterials and its multiple applications can offer a solution to the problems that derive from these situations. In this sense, antimicrobial hydrogels represent a promising opportunity with multiple translational expectations in the medical management of infectious diseases due to their unique physicochemical and biological properties as well as for drug delivery in specific areas. Hydrogels are three-dimensional cross-linked networks of hydrophilic polymers that can absorb and retain large amounts of water or biological fluids. Moreover, antimicrobial hydrogels (AMH) present good biocompatibility, low toxicity, availability, viscoelasticity, biodegradability, and antimicrobial properties. In the present review, we collect and discuss the most promising strategies in the development of AMH, which are divided into hydrogels with inherent antimicrobial activity and antimicrobial agent-loaded hydrogels based on their composition. Then, we present an overview of the main translational applications: wound healing, tissue engineering and regeneration, drug delivery systems, contact lenses, 3D printing, biosensing, and water purification. [ABSTRACT FROM AUTHOR]

Published

2023

10. Assessment of Tissue Expression of the Oxytocin–Vasopressin Pathway in the Placenta of Women with a First-Episode Psychosis during Pregnancy.

Author

Ortega, Miguel A., García-Montero, Cielo, Fraile-Martinez, Óscar, De Leon-Oliva, Diego, Boaru, Diego Liviu, Bravo, Coral, De Leon-Luis, Juan A., Saez, Miguel A., Asúnsolo, Angel, Romero-Gerechter, Ignacio, Sanz-Giancola, Alejandro, Diaz-Pedrero, Raul, Lopez-Gonzalez, Laura, Guijarro, Luis G., Barrena-Blázquez, Silvestra, Bujan, Julia, García-Honduvilla, Natalio, Alvarez-Mon, Melchor, Alvarez-Mon, Miguel Ángel, and Lahera, Guillermo

Subjects

GENE expression, PLACENTA, HORMONE receptors, PREGNANT women, PSYCHOSES, TROPHOBLAST, VASOPRESSIN

Abstract

Psychosis refers to a mental health condition characterized by a loss of touch with reality, comprising delusions, hallucinations, disorganized thought, disorganized behavior, catatonia, and negative symptoms. A first-episode psychosis (FEP) is a rare condition that can trigger adverse outcomes both for the mother and newborn. Previously, we demonstrated the existence of histopathological changes in the placenta of pregnant women who suffer an FEP in pregnancy. Altered levels of oxytocin (OXT) and vasopressin (AVP) have been detected in patients who manifested an FEP, whereas abnormal placental expression of these hormones and their receptors (OXTR and AVPR1A) has been proven in different obstetric complications. However, the precise role and expression of these components in the placenta of women after an FEP have not been studied yet. Thus, the purpose of the present study was to analyze the gene and protein expression, using RT-qPCR and immunohistochemistry (IHC), of OXT, OXTR, AVP, and AVPR1a in the placental tissue of pregnant women after an FEP in comparison to pregnant women without any health complication (HC-PW). Our results showed increased gene and protein expression of OXT, AVP, OXTR, and AVPR1A in the placental tissue of pregnant women who suffer an FEP. Therefore, our study suggests that an FEP during pregnancy may be associated with an abnormal paracrine/endocrine activity of the placenta, which can negatively affect the maternofetal wellbeing. Nevertheless, additional research is required to validate our findings and ascertain any potential implications of the observed alterations. [ABSTRACT FROM AUTHOR]

Published

2023

11. Chronic Venous Disease during Pregnancy Is Related to Inflammation of the Umbilical Cord: Role of Allograft Inflammatory Factor 1 (AIF-1) and Interleukins 10 (IL-10), IL-12 and IL-18.

Author

Sánchez-Trujillo, Lara, Fraile-Martinez, Oscar, García-Montero, Cielo, García-Puente, Luis M., Guijarro, Luis G., De Leon-Oliva, Diego, Boaru, Diego Liviu, Gardón-Alburquerque, David, del Val Toledo Lobo, María, Royuela, Mar, García-Tuñón, Ignacio, Rios-Parra, Antonio, De León-Luis, Juan A., Bravo, Coral, Álvarez-Mon, Melchor, Bujan, Julia, Saez, Miguel A., García-Honduvilla, Natalio, and Ortega, Miguel A.

Subjects

INTERLEUKINS, INTERLEUKIN-10, CHRONIC diseases, UMBILICAL cord, HOMOGRAFTS, PREGNANCY, INTERLEUKIN receptors

Abstract

Chronic venous disease (CVD) is a common condition that affects the veins in the lower limbs, resulting in a variety of symptoms, such as swelling, pain, and varicose veins (VVs). The plenty hormonal, hemodynamic and mechanical changes occurred in pregnancy make women especially vulnerable to suffer from this condition in this period. Previous works have identified that CVD is associated with an increased inflammatory milieu and significant damage in maternofetal tissues, such as the umbilical cord. However, the inflammatory status of this structure in these patients has not been studied yet. Thus, the aim of the present study was to examine gene and protein expression of a set of inflammatory markers—Allograft inflammatory factor 1 (AIF-1), the proinflammatory cytokines interleukin 12A (IL-12A) and IL-18 and the anti-inflammatory product IL-10—in the umbilical cord of women with CVD during pregnancy (N = 62) and healthy pregnant women (HC; N = 52) by the use of real time qPCR and immunohistochemistry (IHC). Our results demonstrate that the umbilical cord tissue from CVD women exhibit an increased expression of AIF-1, IL-12A and IL-18 along with a decrease in IL-10. Therefore, our study suggests an inflammatory status of this structure related to CVD. Further studies should be conducted to evaluate the expression of other inflammatory markers, as well as to analyze the maternofetal impact of these findings. [ABSTRACT FROM AUTHOR]

Published

2023

12. AIF1: Function and Connection with Inflammatory Diseases.

Author

De Leon-Oliva, Diego, Garcia-Montero, Cielo, Fraile-Martinez, Oscar, Boaru, Diego Liviu, García-Puente, Luis, Rios-Parra, Antonio, Garrido-Gil, Maria J., Casanova-Martín, Carlos, García-Honduvilla, Natalio, Bujan, Julia, Guijarro, Luis G., Alvarez-Mon, Melchor, and Ortega, Miguel A.

Subjects

*CALCIUM-binding proteins, *NEUROLOGICAL disorders, *MACROPHAGE activation, *PHAGOCYTOSIS, *CELL physiology, *MICROFILAMENT proteins

Abstract

Simple Summary: Allograft inflammatory factor 1 (AIF1) is a calcium-binding protein that participates in intracellular processes such as phagocytosis, membrane ruffling and F-actin remodeling. Due to its multiple functions, AIF1 is linked with the activation of macrophages and several diseases such as kidney disease, rheumatoid arthritis, cancer, cardiovascular diseases, metabolic diseases, neurological disorders and transplants. In this review, we present a comprehensive review of the known structure, functions and role of AIF1 in inflammatory diseases. Macrophages are a type of immune cell distributed throughout all tissues of an organism. Allograft inflammatory factor 1 (AIF1) is a calcium-binding protein linked to the activation of macrophages. AIF1 is a key intracellular signaling molecule that participates in phagocytosis, membrane ruffling and F-actin polymerization. Moreover, it has several cell type-specific functions. AIF1 plays important roles in the development of several diseases: kidney disease, rheumatoid arthritis, cancer, cardiovascular diseases, metabolic diseases and neurological disorders, and in transplants. In this review, we present a comprehensive review of the known structure, functions and role of AIF1 in inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2023

13. Patients with Chronic Spinal Cord Injury and a Long Period of Evolution Exhibit an Altered Cytokine Production by CD4 and CD8 T Cell Populations.

Author

Girón, Sergio Haro, Gómez-Lahoz, Ana M., Sanz, Jorge Monserrat, Fraile-Martínez, Oscar, Jiménez, Diego J., Garcia-Montero, Cielo, de Leon-Oliva, Diego, Ortega, Miguel A., Atienza-Perez, Mar, Diaz, David, Lopez-Dolado, Elisa, and Álvarez-Mon, Melchor

Subjects

CELL populations, SPINAL cord injuries, T cells, CD8 antigen, CD4 antigen, CYTOKINES

Abstract

Spinal cord injury (SCI) is a disabling neurological condition coursing with serious multisystem affections and morbidities. Changes in immune cell compartments have been consistently reported in previous works, representing a critical point of study for understanding the pathophysiology and progression of SCI from acute to chronic stages. Some relevant variations in circulating T cells have been noticed in patients with chronic SCI, although the number, distribution, and function of these populations remain to be fully elucidated. Likewise, the characterization of specific T cell subpopulations and their related cytokine production can aid in understanding the immunopathological role of T cells in SCI progression. In this sense, the objective of the present study was to analyze and quantify the total number of different cytokine-producers T cells in the serum of patients with chronic SCI (n = 105) in comparison to healthy controls (n = 38) by polychromatic flow cytometry. Having this goal, we studied CD4 and CD8 lymphocytes as well as naïve, effector, and effector/central memory subpopulations. SCI patients were classified according to the duration of the lesion in chronic SCI with a short period of evolution (SCI-SP) (comprised between 1 and 5 years since initial injury), early chronic phase (SCI-ECP) (between 5 and 15 years since initial injury) and late-chronic phase (SCI-LCP) (>15 years since initial injury). Our results show that patients with chronic SCI exhibited an altered immune profile of cytokine-producer T cells, including CD4/CD8 naïve, effector, and memory subpopulations in comparison to HC. In particular, IL-10 and IL-9 production seems to be importantly altered, especially in patients with SCI-LCP, whereas changes in IL-17, TNF-α, and IFN-γ T cell populations have also been reported in this and other chronic SCI groups. In conclusion, our study demonstrates an altered profile of cytokine-producer T cells in patients with chronic SCI, with marked changes throughout the course of the disease. In more detail, we have observed significant variations in cytokine production by circulating naive, effector, and effector/central memory CD4 and CD8 T cells. Future studies should be directed to explore the possible clinical consequences of these changes or develop additional translational approaches in these groups of patients. [ABSTRACT FROM AUTHOR]

Published

2023

14. Understanding HAT1: A Comprehensive Review of Noncanonical Roles and Connection with Disease.

Author

Ortega, Miguel A., De Leon-Oliva, Diego, Garcia-Montero, Cielo, Fraile-Martinez, Oscar, Boaru, Diego Liviu, del Val Toledo Lobo, María, García-Tuñón, Ignacio, Royuela, Mar, García-Honduvilla, Natalio, Bujan, Julia, Guijarro, Luis G., Alvarez-Mon, Melchor, and Alvarez-Mon, Miguel Ángel

Subjects

*MITOCHONDRIAL proteins, *GENE expression, *RNA interference, *HISTONE acetyltransferase, *CHRONIC obstructive pulmonary disease, *APTAMERS

Abstract

Histone acetylation plays a vital role in organizing chromatin, regulating gene expression and controlling the cell cycle. The first histone acetyltransferase to be identified was histone acetyltransferase 1 (HAT1), but it remains one of the least understood acetyltransferases. HAT1 catalyzes the acetylation of newly synthesized H4 and, to a lesser extent, H2A in the cytoplasm. However, 20 min after assembly, histones lose acetylation marks. Moreover, new noncanonical functions have been described for HAT1, revealing its complexity and complicating the understanding of its functions. Recently discovered roles include facilitating the translocation of the H3H4 dimer into the nucleus, increasing the stability of the DNA replication fork, replication-coupled chromatin assembly, coordination of histone production, DNA damage repair, telomeric silencing, epigenetic regulation of nuclear lamina-associated heterochromatin, regulation of the NF-κB response, succinyl transferase activity and mitochondrial protein acetylation. In addition, the functions and expression levels of HAT1 have been linked to many diseases, such as many types of cancer, viral infections (hepatitis B virus, human immunodeficiency virus and viperin synthesis) and inflammatory diseases (chronic obstructive pulmonary disease, atherosclerosis and ischemic stroke). The collective data reveal that HAT1 is a promising therapeutic target, and novel therapeutic approaches, such as RNA interference and the use of aptamers, bisubstrate inhibitors and small-molecule inhibitors, are being evaluated at the preclinical level. [ABSTRACT FROM AUTHOR]

Published

2023

15. Prognostic Value of Malondialdehyde (MDA) in the Temporal Progression of Chronic Spinal Cord Injury.

Author

Haro Girón, Sergio, Monserrat Sanz, Jorge, Ortega, Miguel A., Garcia-Montero, Cielo, Fraile-Martínez, Oscar, Gómez-Lahoz, Ana M., Boaru, Diego Liviu, de Leon-Oliva, Diego, Guijarro, Luis G., Atienza-Perez, Mar, Diaz, David, Lopez-Dolado, Elisa, and Álvarez-Mon, Melchor

Subjects

SPINAL cord injuries, PROGNOSIS, RECEIVER operating characteristic curves, MALONDIALDEHYDE, OXIDATIVE stress

Abstract

Background: Oxidative stress is a major signature of spinal cord injury (SCI). The altered levels of various oxidative stress markers have been demonstrated in acute and chronic SCI. However, the variation of these markers in patients with chronic SCI depending on the time since the initial injury has not been explored yet. Objective: Our aim was to measure plasma levels of malondialdehyde (MDA), a marker of lipid peroxidation in patients with SCI stratified in different periods of suffering the injury (0–5 years, 5–10 years, and more than 10 years). Patients and methods: This cross-sectional study enrolled patients with SCI (N = 105) from different periods of the lesion and healthy control (HC) subjects (N = 38): short period (SCI SP, N = 31, time of evolution less than 5 years); early chronic (SCI ECP, N = 32, time of evolution 5–15 years); and late chronic (SCI LCP, N = 42, time of evolution more than 15 years). The plasma levels of MDA were measured using a commercially available colorimetric assay. Results: Patients with SCI had significantly higher plasma levels of MDA than HC subjects. Receiver operating characteristic (ROC) curve analysis for plasma MDA levels in patients with SCI demonstrated areas under the curve (AUC) of 1 (HC vs. SCI-SP); 0.998 (HC vs. SCI-ECP); and 0.964 (HC vs. SCI-LCP). Additionally, three ROC curves were used to compare the different concentrations of MDA between the subgroups of patients with SCI, and the resulting AUCs were: 0.896 (SCI-SP vs. SCI-ECP); 0.840 (SCI-ECP vs. SCI-LCP); and 0.979 (SCI-SP vs. SCI-LCP). Conclusion: Plasma concentration of MDA can be considered as an oxidative stress biomarker to assess the prognosis of SCI in chronic stages. [ABSTRACT FROM AUTHOR]

Published

2023

16. Abnormal Characterization and Distribution of Circulating Regulatory T Cells in Patients with Chronic Spinal Cord Injury According to the Period of Evolution.

Author

Gómez-Lahoz, Ana M., Girón, Sergio Haro, Sanz, Jorge Monserrat, Fraile-Martínez, Oscar, Garcia-Montero, Cielo, Jiménez, Diego J., de Leon-Oliva, Diego, Ortega, Miguel A., Atienza-Perez, Mar, Diaz, David, Lopez-Dolado, Elisa, and Álvarez-Mon, Melchor

Subjects

REGULATORY T cells, SPINAL cord injuries, T cells

Abstract

Simple Summary: Immune dysfunction is a major feature of chronic spinal cord injuries (SCIs). It is associated with many of the complications observed in these patients, such as increased vulnerability to infections and other medical challenges. The role of regulatory T cells (Tregs) after SCI is beginning to be more acutely understood; however, little is known about their implications at chronic stages. By using flow cytometry, we characterized circulating Tregs from chronic SCI patients according to the time of initial injury (1–5 years; 5–15 years; and >15 years). Our results demonstrate significant changes in the immunological phenotypes of these cells, especially in patients with long periods of evolution (5–15 years and >15 years with chronic SCI). Despite the fact that a deeper understanding of the immune dysfunction caused by chronic SCI is still required, the characterization of circulating leukocytes such as Tregs and other populations can open up the possibility of finding translational biomarkers or therapeutic approaches that may aid in the clinical management of chronic SCI. Spinal cord injury (SCI) is a progressive and complex neurological disorder accompanied by multiple systemic challenges. Peripheral immune dysfunction is a major event occurring after SCI, especially in its chronic phase. Previous works have demonstrated significant changes in different circulating immune compartments, including in T cells. However, the precise characterization of these cells remains to be fully unraveled, particularly when considering important variants such as the time since the initial injury. In the present work, we aimed to study the level of circulating regulatory T cells (Tregs) in SCI patients depending on the duration of evolution. For this purpose, we studied and characterized peripheral Tregs from 105 patients with chronic SCI using flow cytometry, with patients classified into three major groups depending on the time since initial injury: short period chronic (SCI-SP, <5 years since initial injury); early chronic (SCI-ECP, from 5–15 years post-injury) and late chronic SCI (SCI-LCP, more than 15 years post-injury. Our results show that both the SCI-ECP and SCI-LCP groups appeared to present increased proportions of CD4+ CD25+/low Foxp3+ Tregs in comparison to healthy subjects, whereas a decreased number of these cells expressing CCR5 was observed in SCI-SP, SCI-ECP, and SCI-LCP patients. Furthermore, an increased number of CD4+ CD25+/high/low Foxp3 with negative expression of CD45RA and CCR7 was observed in SCI-LCP patients when compared to the SCI-ECP group. Taken together, these results deepen our understanding of the immune dysfunction reported in chronic SCI patients and how the time since initial injury may drive this dysregulation. [ABSTRACT FROM AUTHOR]

Published

2023