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1. Effects of Fasting on THP1 Macrophage Metabolism and Inflammatory Profile

Author

Julia Rius-Bonet, Salvador Macip, Marta Massip-Salcedo, and Daniel Closa

Subjects
fasting, intermittent fasting, macrophages, inflammation, rheumatic diseases, Biology (General), QH301-705.5, Chemistry, QD1-999
Abstract

Fasting can affect the body’s inflammatory response, and this has been linked to potential health benefits, including improvements for people with rheumatic diseases. In this work, we evaluated, in vitro, how changes in nutrient availability alter the inflammatory response of macrophages. Macrophage-differentiated THP1 cells were cultured, deprived of FCS or subjected to cycles of FCS deprivation and restoration to mimic intermittent fasting. Changes in the macrophage phenotype, the cells’ response to inflammatory stimuli and the level of mitochondrial alteration were assessed. The results indicate that while periods of serum starvation are associated with a decrease in IL1β and TNFα expression, consistent with an anti-inflammatory response, intermittent serum starvation cycles promote a pro-inflammatory phenotype. Rapid changes in reducing capacity and mitochondrial response were also observed. Of note, while some changes, such as the production of oxygen free radicals, were reversed with refeeding, others, such as a decrease in reducing capacity, were maintained and even increased. This study shows that different fasting protocols can have diverging effects and highlights that time-limited nutrient changes can significantly affect macrophage functions in cell cultures. These findings help elucidate some of the mechanisms by which specific fasting dietary interventions could help control inflammatory diseases.

Published
2024
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2. A master of all trades – linking retinoids to different signalling pathways through the multi-purpose receptor STRA6

Author

Vinesh Dhokia and Salvador Macip

Subjects
Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671
Abstract

Abstract Retinoids are a group of vitamin A-related chemicals that are essential to chordate mammals. They regulate a number of basic processes, including embryogenesis and vision. From ingestion to metabolism and the subsequent cellular effects, retinoid levels are tightly regulated in the organism to prevent toxicity. One component of this network, the membrane receptor STRA6, has been shown to be essential in facilitating the cellular entry and exit of retinol. However, recent data suggests that STRA6 may not function merely as a retinoid transporter but also act as a complex signalling hub in its own right, being able to affect cell fate through the integration of retinoid signalling with other key pathways, such as those involving p53, JAK/STAT, Wnt/β catenin and calcium. This may open new therapeutic strategies in diseases like cancer, where these pathways are often compromised. Here, we look at the growing evidence regarding the novel roles of STRA6 beyond its well characterized classic functions.

Published
2021
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3. Targeted clearance of senescent cells using an antibody-drug conjugate against a specific membrane marker

Author

Marta Poblocka, Akang Leonard Bassey, Victoria M. Smith, Marta Falcicchio, Ana Sousa Manso, Mohammad Althubiti, XiaoBo Sheng, Andrew Kyle, Ruth Barber, Mark Frigerio, and Salvador Macip

Subjects
Medicine, Science
Abstract

Abstract A wide range of diseases have been shown to be influenced by the accumulation of senescent cells, from fibrosis to diabetes, cancer, Alzheimer’s and other age-related pathologies. Consistent with this, clearance of senescent cells can prolong healthspan and lifespan in in vivo models. This provided a rationale for developing a new class of drugs, called senolytics, designed to selectively eliminate senescent cells in human tissues. The senolytics tested so far lack specificity and have significant off-target effects, suggesting that a targeted approach could be more clinically relevant. Here, we propose to use an extracellular epitope of B2M, a recently identified membrane marker of senescence, as a target for the specific delivery of toxic drugs into senescent cells. We show that an antibody–drug conjugate (ADC) against B2M clears senescent cells by releasing duocarmycin into them, while an isotype control ADC was not toxic for these cells. This effect was dependent on p53 expression and therefore more evident in stress-induced senescence. Non-senescent cells were not affected by either antibody, confirming the specificity of the treatment. Our results provide a proof-of-principle assessment of a novel approach for the specific elimination of senescent cells using a second generation targeted senolytic against proteins of their surfaceome, which could have clinical applications in pathological ageing and associated diseases.

Published
2021
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4. PML-II regulates ERK and AKT signal activation and IFNα-induced cell death

Author

Xueqiong Meng, Yixiang Chen, Salvador Macip, and Keith Leppard

Subjects
Promyelocytic leukemia protein, PML-II, IFNα, Apoptotic signaling, ERK, AKT, Medicine, Cytology, QH573-671
Abstract

Abstract Background The requirement of promyelocytic leukaemia protein (PML) in interferon (IFN)-induced cell apoptosis is well-established. However, the exact mechanisms by which the multiple isoforms of PML protein participate in this process remain not well-understood. We previously demonstrated that PML isoform II (PML-II) positively regulates induced gene expression during a type I IFN response and evaluate here how PML-II contributes to IFNα-induced cell death. Methods HeLa cells were transiently depleted of PML-II by siRNA treatment and the response of these cells to treatment with IFNα assessed by molecular assays of mRNA and proteins associated with IFN and apoptosis responses. Results In HeLa cells, death during IFNα stimulation was reduced by prior PML-II depletion. PML-II removal also considerably decreased the induced expression of pro-apoptotic ISGs such as ISG54 (IFIT2), and substantially impaired or prevented expression of PUMA and TRAIL, proteins that are associated with the intrinsic and extrinsic apoptotic pathways respectively. Thirdly, PML-II depletion enhanced ERK and AKT pro-survival signaling activation suggesting that PML-II normally suppresses signaling via these pathways, and that lack of PML-II hence led to greater than normal activation of AKT signaling upon IFNα stimulation and consequently increased resistance to IFNα-induced apoptosis. Conclusions The positive contribution of PML-II to the expression of various IFNα-induced pro-apoptotic proteins and its inhibition of pro-survival signaling together provide a mechanistic explanation for reduced apoptosis under conditions of PML deficiency and may account for at least part of the role of PML as a tumor suppressor gene. Video Abstract

Published
2021
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5. Individual Freedom in the Initial Response to Covid-19

Author

Salvador Macip and Oriol Yuguero

Subjects
COVID-19, ethics, pandethics, syndemic, individual freedom, Public aspects of medicine, RA1-1270
Abstract

The COVID-19 pandemic has been a phenomenal challenge to global health care and will continue to be so in the upcoming months. Beyond its medical toll, COVID-19 has also exacerbated pre-existing social issues and created new inequalities. This has generated a series of ethical problems that will need to be carefully analyzed to avoid repeating similar mistakes in the context of other crises. Among those, we discuss here the bioethical implications of preserving individual freedom in the context of the early response to a pandemic and propose a global approach to the issue that could be applied in future health challenges.

Published
2022
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6. poly(I:C) synergizes with proteasome inhibitors to induce apoptosis in cervical cancer cells

Author

Xueqiong Meng, Xiaoxi Cui, Xiaoya Shao, Yanqi Liu, Yihao Xing, Victoria Smith, Shiqiu Xiong, Salvador Macip, and Yixiang Chen

Subjects
Cervical cancer, poly(I:C), Proteasome inhibitor, Combination, Apoptosis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Cervical cancer is one of the most common malignancies in women, with a poor survival rate. Thus, there is a need to define effective combination strategies to improve therapy. In this study, we report that dsRNA poly(I:C) up-regulated the expression of IFNβ and apoptosis-associated genes in cervical cancer cells, activating both intrinsic and extrinsic apoptotic pathways, and eventually inducing cell death. Similarly, proteasome inhibitors also effectively induced cervical cancer cell apoptosis, probably through prevention of p53 degradation, inhibiting NF-κB signal activation and decreasing BCL-2 expression. Importantly, the combination of poly(I:C) with proteasome inhibitors enhanced caspase-8 and caspase-9 activation, and synergistically induced cervical cancer cell apoptosis. Both activated p38 signals and increased ROS levels, and their combination extended these effects. Collectively, we show that the activation of multiple pro-apoptotic pathways by poly(I:C) and proteasome inhibitors underpin a synergistic effect on inducing cervical cancer cell death, suggesting a potential therapeutic combination with clinical relevance.

Published
2022
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7. Introduction: Transhumanism. Beyond the body

Author

Salvador Macip

Subjects
Communication. Mass media, P87-96, Information resources (General), ZA3040-5185
Abstract

Science allows us to understand the world we live in. Centuries of research have helped us learn more about our place in the universe, and we have discovered a perhaps even more fascinating mystery: how the organism we inhabit works and the reasons why it stops doing so. In this field, as in many others, we have gone from just admiring nature’s wonders to being able to control them.

Published
2022
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8. Hesitation about coronavirus vaccines in healthcare professionals and general population in Spain.

Author

Francesc Saigí-Rubió, Hans Eguia, Albert Espelt, Salvador Macip, and Marina Bosque-Prous

Subjects
Medicine, Science
Abstract

BackgroundThis study attempts to provide a picture of the hesitancy to vaccination against COVID-19 in Spain during the 2021 spring-autumn vaccination campaign, both in the general population and in healthcare professionals.MethodsThe participants were recruited using social media such as Facebook and Twitter, in addition to the cooperation of health personnel contacted with the collaboration of medical scientific societies. A cross-sectional study was carried out that included the response of an online questionnaire. The data were collected from April 30 to September 26, 2021. To assess the different associations between variables to be measured, we fit Poisson regression models with robust variance.ResultsResponses were obtained from 3,850 adults from the general population group and 502 health professionals. Of the overall sample, 48.6% of participants from the general population were vaccinated against COVID-19, whereas in the healthcare professionals, 94.8% were vaccinated. The prevalence of general population vaccination increased with age, and was higher in women than men. Most participants did not show a preference for any vaccine itself. However, the prevalence of people vaccinated with their preferred vaccine was higher for the ones vaccinated with Pfizer's vaccine. 6.5% of the general population reported being reticent to be vaccinated. People from younger age groups, people with lower educational levels and those who were not from a risk group showed greater reluctance to be vaccinated. No gender differences in reluctancy were found.ConclusionsHealth professionals were significantly less likely to refuse vaccination even though they had more doubts about the safety and efficacy of vaccines. On the other hand, younger people, those with a lower level of education and those who were not from a risk group were the most hesitant.

Published
2022
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9. Specific interactions of BCL-2 family proteins mediate sensitivity to BH3-mimetics in diffuse large B-cell lymphoma

Author

Victoria M. Smith, Anna Dietz, Kristina Henz, Daniela Bruecher, Ross Jackson, Lisa Kowald, Sjoerd J.L. van Wijk, Sandrine Jayne, Salvador Macip, Simone Fulda, Martin J.S. Dyer, and Meike Vogler

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

The BCL-2-specific inhibitor, ABT-199 (venetoclax) has exhibited remarkable clinical activity in nearly all cases of chronic lymphocytic leukemia. In contrast, responses are usually much less in diffuse large B-cell lymphoma (DLBCL), despite high level expression of BCL-2 in over 40% of cases, indicating that co-expression of related anti-apoptotic BCL-2 family proteins may limit the activity of ABT-199. We have investigated the roles of BCL-2 proteins in DLBCL cells using a panel of specific BCL-2 homology 3 (BH3)-mimetics and identified subgroups of these cells that exhibited marked and specific dependency on either BCL-2, BCL-XL or MCL-1 for survival. Dependency was associated with selective sequestration of the pro-apoptotic proteins BIM, BAX and BAK by the specific anti-apoptotic BCL-2 protein which was important for cellular survival. Sensitivity to BH3-mimetics was independent of genetic alterations involving the BCL-2 family and only partially correlated with protein expression levels. Treatment with ABT-199 displaced BAX and BIM from BCL-2, subsequently leading to BAK activation and apoptosis. In contrast, apoptosis induced by inhibiting BCL-XL with A1331852 was associated with a displacement of both BAX and BAK from BCL-XL and occurred independently of BIM. Finally, the MCL-1 inhibitor S63845 induced mainly BAX-dependent apoptosis mediated by a displacement of BAK, BIM and NOXA from MCL-1. In conclusion, our study indicates that in DLBCL, the heterogeneous response to BH3-mimetics is mediated by selective interactions between BAX, BAK and anti-apoptotic BCL-2 proteins.

Published
2020
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10. An Appraisal on the Value of Using Nutraceutical Based Senolytics and Senostatics in Aging

Author

Amanpreet Kaur, Salvador Macip, and Cordula M. Stover

Subjects
senescence, senolytics, senostatics, nutraceuticals, aging, Biology (General), QH301-705.5
Abstract

The average human life expectancy has increased globally, and continues to rise, owing to the substantive progress made in healthcare, medicine, sanitation, housing and education. This ultimately enriches society with a greater proportion of elderly people. Sustaining a healthy aged population is key to diminish the societal and economic impact of age-related infirmities. This is especially challenging because tissue function, and thus wellbeing, naturally progressively decline as humans age. With age increasing the risk of developing diseases, one of the therapeutic options is to interfere with the molecular and cellular pathways involved in age-related tissue dysfunction, which is in part caused by the accumulation of senescent cells. One strategy to prevent this could be using drugs that selectively kill these cells (senolytics). In parallel, some compounds have been identified that prevent or slow down the progression of senescence or some of its features (senostatics). Senolytic and senostatic therapies have been shown to be efficient in vivo, but they also have unwanted dose-dependent side effects, including toxicity. Important advances might be made using bioactive compounds from plants and foods (nutraceuticals) if, as is proposed, they offer similar effectiveness with fewer side effects. The focus of this review is on the use of nutraceuticals in interfering with cellular senescence.

Published
2020
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11. Differences in the molecular profile of endometrial cancers from British White and British South Asian women.

Author

Konstantinos Polymeros, David S Guttery, Roger Hew, Rachael Bishop, Elizabeth Stannard, Salvador Macip, Paul Symonds, and Esther L Moss

Subjects
Medicine, Science
Abstract

ObjectivesTo identify differences in the mutational profile of endometrial tumours between British White (BW) and South Asian (BSA) women.MethodsWe analysed primary tumours from matched cohorts of British White (BW) and British South Asian (BSA) women resident in Leicestershire diagnosed with EC. Next Generation Sequencing was performed to investigate mutational differences in a panel of 10 genes previously identified as being commonly mutated in EC. The presence of somatic Mismatch Repair (MMR) gene deficiencies was determined by immunohistochemistry.ResultsIn total, 57 tumours (27 BSA and 30 BW) were sequenced. There was no significant difference in the overall mutation frequency of the 10 genes analysed; however, numerous differences were observed between the groups. There was a positive association between PIK3CA and PTEN mutations in the BSA group, with 78% of PIK3CA-mutant tumours harbouring a PTEN mutation, whereas only 11% of PIK3CA wild-type (wt) tumours were PTEN mutant positive (p = 0.0012). In BW women, 90% of ARID1A mutant tumours had co-existent PI3K pathway mutations versus 50% of wild-type (wt) ARID1A patients (p = 0.0485). This trend was not significant in the BSA group (p = 0.66). The age at diagnosis was significantly higher in the BW group with a somatic MMR gene deficiency compared to those with no deficiency (72.8 years versus 59.6 years, p = 0.007), whereas this difference was not seen in the BSA group (64 years versus 60 years, p = 0.37).ConclusionWe have identified differences in the mutational profile of primary EC tumours from BW and BSA women. Further research is needed to confirm these findings and to explore their potential implications for early detection, treatment response and prognosis.

Published
2020
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12. Desemmascarar el càncer: Centenars de malalties, un sol nom

Author

Salvador Macip

Subjects
càncer, oncogèn, p53, supressors tumorals, teràpies personalitzades, Communication. Mass media, P87-96, Information resources (General), ZA3040-5185
Abstract

Tothom té una idea més o menys clara del que representa un càncer: un conjunt de cèl·lules que es divideixen sense control. Darrera aquesta imatge simplista s’amaga un dels problemes de salut més complexes i més greus que existeixen. És gràcies als avenços biomèdics dels últims vint anys que finalment estem reconeixent les grans diferències que hi ha entre els tipus de càncers coneguts, un descobriment que resultarà clau per a dissenyar teràpies més efectives en un futur proper.

Published
2014
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13. The role of the HIF-1α transcription factor in increased cell division at physiological oxygen tensions.

Author

Samantha Carrera, Joana Senra, Maria Isabel Acosta, Mohammad Althubiti, Ester M Hammond, Petra J de Verdier, and Salvador Macip

Subjects
Medicine, Science
Abstract

HIF-1 is a transcription factor that mediates the cellular responses to low oxygen environments, mainly as a result of having an oxygen-labile subunit, HIF-1α. HIF-1α has been carefully studied in the context of severe hypoxic stresses (

Published
2014
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19. IFN-γ enhances CLL cell resistance to ABT-199 by regulating MCL-1 and BCL-2 expression via the JAK-STAT3 signaling pathway

Author

Xiaoya Shao, Xueqiong Meng, Haiping Yang, Xinxin Wang, Ling Qin, Guomin Shen, Xiaoping Xi, Huijuan Zhao, Salvador Macip, and Yixiang Chen

Subjects
Cancer Research, Oncology, Hematology
Abstract

Although clinical outcomes of CLL have improved with the use of BCL-2 inhibitor, ABT-199, acquired resistance eventually occurs in many cases, which leads to CLL disease progression. Thus, understanding the mechanisms that mediate this relapse is important to design improved therapies. Herein, we report that cytokine IFN-γ, secreted by dysfunctional T cells, enhanced CLL cells resistance to ABT-199. IFN-γ stimulation significantly increased the expression of BCL-2, MCL-1 and BCL-xL. Blocking JAK1/2-STAT3 signaling pathway impaired the expression of these anti-apoptotic proteins after IFN-γ stimulation. The combination of ABT-199 with JAK1/2 inhibitor Ruxolitinib or STAT3 inhibitors Stattic and C188-9 increased malignant B cell death. In summary, we show that IFN-γ enhanced CLL cells resistance to ABT-199 at least in part by up-regulating BCL-2, MCL-1 and BCL-xL expression

Published
2022

20. Data from BTK Modulates p53 Activity to Enhance Apoptotic and Senescent Responses

Author

Salvador Macip, Nickolai A. Barlev, George D.D. Jones, Kong-Peng Lam, Koon-Guan Lee, Hishyar Najeeb, Josep M. Escorsa, Jesvin Samuel, Miran Rada, and Mohammad Althubiti

Abstract

p53 is a tumor suppressor that prevents the emergence of transformed cells by inducing apoptosis or senescence, among other responses. Its functions are regulated tightly by posttranslational modifications. Here we show that Bruton's tyrosine kinase (BTK) is a novel modulator of p53. We found that BTK is induced in response to DNA damage and p53 activation. BTK induction leads to p53 phosphorylation, which constitutes a positive feedback loop that increases p53 protein levels and enhances the transactivation of its target genes in response to stress. Inhibiting BTK reduced both p53-dependent senescence and apoptosis. Further, BTK expression also upregulated DNA damage signals and apoptosis. We conclude that despite being involved in oncogenic signals in blood malignancies, BTK has antineoplastic properties in other contexts, such as the enhancement of p53's tumor suppressor responses. Along with evidence that BTK expression correlates with good prognosis in some epithelial tumors, our findings may encourage a reevaluation of the clinical uses of BTK inhibitors in cancer therapy. Cancer Res; 76(18); 5405–14. ©2016 AACR.

Published
2023

23. Snapshot imprinting as a tool for surface mapping and identification of novel biomarkers of senescent cells

Author

Elena Piletska, Dana Thompson, Rebecca Jones, Alvaro Garcia Cruz, Marta Poblocka, Francesco Canfarotta, Rachel Norman, Salvador Macip, Donald J. L. Jones, and Sergey Piletsky

Subjects
General Engineering, General Materials Science, Bioengineering, General Chemistry, Atomic and Molecular Physics, and Optics
Abstract

Cellular senescence has proved to be a strong contributor to ageing and age-related diseases, such as cancer and atherosclerosis. Therefore, the protein content of senescent cells is highly relevant to drug discovery, diagnostics and therapeutic applications. However, current technologies for the analysis of proteins are based on a combination of separation techniques and mass spectrometry, which require handling large sample sizes and a large volume of data and are time-consuming. This limits their application in personalised medicine. An easy, quick and inexpensive procedure is needed for qualitative and quantitative analysis of proteins expressed by a cell or tissue. Here, we describe the use of the "snapshot imprinting" approach for the identification of proteins differentially expressed by senescent cells. Molecularly imprinted polymer nanoparticles (MIPs) were formed in the presence of whole cells. Following trypsinolysis, protein epitopes protected by complex with MIPs were eluted from the nanoparticles and analysed by LC-MS/MS. In this work, "snapshot imprinting" was performed parallel to a standard proteomic "shaving approach", showing similar results. The analysis by "snapshot imprinting" identified three senescent-specific proteins: cell division cycle 7-related protein kinase, partitioning defective three homolog B and putative ATP-dependent RNA helicase DHX57, the abundance of which could potentially make them specific markers of senescence. Identifying biomarkers for the future elimination of senescent cells grants the potential for developing therapeutics for age-related diseases.

Published
2022

25. Targeted clearance of senescent cells using an antibody-drug conjugate against a specific membrane marker

Author

Akang Leonard Bassey, Ana Sousa Manso, Mohammad Althubiti, Mark Frigerio, Andrew F. Kyle, Victoria M. Smith, Marta Poblocka, Marta Falcicchio, Ruth C. Barber, XiaoBo Sheng, Salvador Macip, Universitat Oberta de Catalunya (UOC), University of Leicester, and Babraham Research Campus

Subjects
Senescence, Antibody-drug conjugate, Immunoconjugates, Science, Biology, Medical sciences, Epitope, Article, Cell Line, Duocarmycins, In vivo, Fibrosis, Senotherapeutics, target identification, Target identification, medicine, marcador biológico, Humans, identificació d'objectius, marcador biològic, Senolytic, Cellular Senescence, Ciències de la salut, identificación de objetivos, Multidisciplinary, medicine.disease, biological marker, Isotype, senescence cells, Ciencias de la salud, Gene Expression Regulation, cèl·lules senescents, biology.protein, Cancer research, Medicine, Antibody, Tumor Suppressor Protein p53, células senescentes, beta 2-Microglobulin
Abstract

A wide range of diseases have been shown to be influenced by the accumulation of senescent cells, from fibrosis to diabetes, cancer, Alzheimer’s and other age-related pathologies. Consistent with this, clearance of senescent cells can prolong healthspan and lifespan in in vivo models. This provided a rationale for developing a new class of drugs, called senolytics, designed to selectively eliminate senescent cells in human tissues. The senolytics tested so far lack specificity and have significant off-target effects, suggesting that a targeted approach could be more clinically relevant. Here, we propose to use an extracellular epitope of B2M, a recently identified membrane marker of senescence, as a target for the specific delivery of toxic drugs into senescent cells. We show that an antibody–drug conjugate (ADC) against B2M clears senescent cells by releasing duocarmycin into them, while an isotype control ADC was not toxic for these cells. This effect was dependent on p53 expression and therefore more evident in stress-induced senescence. Non-senescent cells were not affected by either antibody, confirming the specificity of the treatment. Our results provide a proof-of-principle assessment of a novel approach for the specific elimination of senescent cells using a second generation targeted senolytic against proteins of their surfaceome, which could have clinical applications in pathological ageing and associated diseases.

Published
2021

27. Cooperative stabilisation of 14-3-3σ protein–protein interactions via covalent protein modification

Author

Alisha Mohindra, Pietro Roversi, Salvador Macip, Richard G. Doveston, Sara Y. Chothia, Marta Falcicchio, Jaswir Basran, Jake A. Ward, and Universitat Oberta de Catalunya (UOC)

Subjects
Mechanism (biology), Chemistry, Cell growth, Neurodegeneration, interaction, Cooperativity, General Chemistry, medicine.disease, Ligand (biochemistry), proteins, Cell biology, Protein–protein interaction, chemistry.chemical_compound, Fusicoccin, medicine, stabilisation, Cysteine
Abstract

14-3-3 proteins are an important family of hub proteins that play important roles in many cellular processes via a large network of interactions with partner proteins. Many of these protein-protein interactions (PPI) are implicated in human diseases such as cancer and neurodegeneration. The stabilisation of selected 14-3-3 PPIs using drug-like 'molecular glues' is a novel therapeutic strategy with high potential. However, the examples reported to date have a number of drawbacks in terms of selectivity and potency. Here, we report that WR-1065, the active species of the approved drug amifostine, covalently modifies 14-3-3o at an isoform-unique cysteine residue, Cys38. This modification leads to isoform-specific stabilisation of two 14-3-3o PPIs in a manner that is cooperative with a well characterised molecular glue, fusicoccin A. Our findings reveal a novel stabilisation mechanism for 14-3-3o, an isoform with particular involvement in cancer pathways. This mechanism can be exploited to harness the enhanced potency conveyed by covalent drug molecules and dual ligand cooperativity. This is demonstrated in two cancer cell lines whereby the cooperative behaviour of fusicoccin A and WR-1065 leads to enhanced efficacy for inducing cell death and attenuating cell growth.

Published
2021

28. Relevance of the Bruton Tyrosine Kinase as a Target for COVID-19 Therapy

Author

Miran Rada, Salvador Macip, Zahraa Qusairy, and Marta Massip-Salcedo

Subjects
0301 basic medicine, Cancer Research, Antiviral Agents, Virus, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Piperidines, Neoplasms, Pandemic, Agammaglobulinaemia Tyrosine Kinase, Humans, Medicine, Bruton's tyrosine kinase, Molecular Targeted Therapy, Lung, Protein Kinase Inhibitors, Molecular Biology, biology, business.industry, Adenine, Mortality rate, COVID-19, Outbreak, Thrombosis, COVID-19 Drug Treatment, 030104 developmental biology, Oncology, chemistry, Pyrazines, 030220 oncology & carcinogenesis, Ibrutinib, Benzamides, Immunology, Cancer research, biology.protein, Acalabrutinib, business
Abstract

The outbreak of the novel coronavirus disease 2019 (COVID-19) has emerged as one of the biggest global health threats worldwide. As of October 2020, more than 44 million confirmed cases and more than 1,160,000 deaths have been reported globally, and the toll is likely to be much higher before the pandemic is over. There are currently little therapeutic options available and new potential targets are intensively investigated. Recently, Bruton tyrosine kinase (BTK) has emerged as an interesting candidate. Elevated levels of BTK activity have been reported in blood monocytes from patients with severe COVID-19, compared with those from healthy volunteers. Importantly, various studies confirmed empirically that administration of BTK inhibitors (acalabrutinib and ibrutinib) decreased the duration of mechanical ventilation and mortality rate for hospitalized patients with severe COVID-19. Herein, we review the current information regarding the role of BTK in severe acute respiratory syndrome coronavirus 2 infections and the suitability of its inhibitors as drugs to treat COVID-19. The use of BTK inhibitors in the management of COVID-19 shows promise in reducing the severity of the immune response to the infection and thus mortality. However, BTK inhibition may be contributing in other ways to inhibit the effects of the virus and this will need to be carefully studied.

Published
2020

29. Molecular imprinting as a tool for determining molecular markers: a lung cancer case

Author

Elena Piletska, Kirabo Magumba, Lesslly Joseph, Alvaro Garcia Cruz, Rachel Norman, Rajinder Singh, Antonella F. S. Tabasso, Donald J. L. Jones, Salvador Macip, Sergey Piletsky, University of Leicester, and Universitat Oberta de Catalunya (UOC)

Subjects
molecular markers, macardors moleculars, lungs--cancer, General Chemical Engineering, pulmones--cancer, cancer de pulmones, General Chemistry, proteins, lung cancer, marcadores moleculares, pulmons--càncer, cancer de pulmons, proteines, proteinas
Abstract

Determining which cancer patients will be sensitive to a given therapy is essential for personalised medicine. Thus, it is important to develop new tools that will allow us to stratify patients according to their predicted response to treatment. The aim of work presented here was to use molecular imprinting for determining the sensitivity of lung cancer cell lines to ionising radiation based on cell surface proteomic differences. Molecularly imprinted polymer nanoparticles (nanoMIPs) were formed in the presence of whole cells. Following trypsinolysis, protein epitopes protected by complexing with MIPs were eluted from the nanoparticles and analysed by LC-MS/MS. The analysis identified two membrane proteins, neutral amino acid transporter B (0) and 4F2 cell-surface antigen heavy chain, the abundance of which in the lung cancer cells could indicate resistance of these cells to radiotherapy. This proof-of-principle experiments shows that this technology can be used in the discovery of new biomarkers and in development of novel diagnostic and therapeutic tools for a personalised medicine approach to treating cancer.

Published
2022

30. Regulation of p53 by the 14-3-3 protein interaction network: new opportunities for drug discovery in cancer

Author

Richard G. Doveston, Jake A. Ward, Salvador Macip, and Marta Falcicchio

Subjects
Cancer Research, Drug discovery, Mechanism (biology), lcsh:Cytology, Immunology, Wild type, Cancer, Review Article, Cell Biology, Computational biology, Biology, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Cellular and Molecular Neuroscience, Drug development, Interaction network, Cancer cell, medicine, lcsh:QH573-671, Tumour-suppressor proteins, 14-3-3 protein
Abstract

Most cancers evolve to disable the p53 pathway, a key tumour suppressor mechanism that prevents transformation and malignant cell growth. However, only ~50% exhibit inactivating mutations of p53, while in the rest its activity is suppressed by changes in the proteins that modulate the pathway. Therefore, restoring p53 activity in cells in which it is still wild type is a highly attractive therapeutic strategy that could be effective in many different cancer types. To this end, drugs can be used to stabilise p53 levels by modulating its regulatory pathways. However, despite the emergence of promising strategies, drug development has stalled in clinical trials. The need for alternative approaches has shifted the spotlight to the 14-3-3 family of proteins, which strongly influence p53 stability and transcriptional activity through direct and indirect interactions. Here, we present the first detailed review of how 14-3-3 proteins regulate p53, with special emphasis on the mechanisms involved in their binding to different members of the pathway. This information will be important to design new compounds that can reactivate p53 in cancer cells by influencing protein–protein interactions. The intricate relationship between the 14-3-3 isoforms and the p53 pathway suggests that many potential drug targets for p53 reactivation could be identified and exploited to design novel antineoplastic therapies with a wide range of applications.

Published
2020

31. Transhumanism. Beyond the body

Author

Salvador Macip

Subjects
Multidisciplinary, History and Philosophy of Science, Philosophy, Humanities
Abstract

SScience allows us to understand the world we live in. Centuries of research have helped us learn more about our place in the universe, and we have discovered a perhaps even more fascinating mystery: how the organism we inhabit works and the reasons why it stops doing so. In this field, as in many others, we have gone from just admiring nature’s wonders to being able to control them.

Published
2021

32. MEK Pathway Inhibition Increases the Efficacy of a PI3K and HDAC Inhibitor in Endometrial Cancer Cells

Author

David S. Guttery, Esther L. Moss, Salvador Macip, and Konstantinos Polymeros

Subjects
business.industry, Endometrial cancer, HDAC inhibitor, Cancer research, Medicine, business, medicine.disease, PI3K/AKT/mTOR pathway
Abstract

Background: Endometrial cancer (EC) is the commonest gynaecologic malignancy in many countries and its incidence is rising. Although excellent prognosis is associated with early stage disease, response to systemic treatment for metastatic or recurrent EC is often low and treatment options are limited.Aims-Methods: The aim of the study was to propose improved targeted drug treatments suitable for subsequent testing in pre-clinical models of EC. Cell proliferation assay (MTS) was used to assess viability of EC cell lines following treatment with drug inhibitors and Western blotting to explore the effect of inhibitors in molecular pathways. Results: We identified that CUDC-907, a PI3K and HDAC inhibitor, was the most effective monotherapy treatment of a panel of drugs screened in EC cells. Moreover, several combination treatments showed synergism in EC cell lines, with the most efficacious being CUDC-907 combined with the MEK inhibitor PD0325901. This indicates that simultaneous inhibition of two main oncogenic pathways, PI3K and MEK, could improve drug sensitivity in EC.Conclusions: In summary, we propose a range of targeted inhibitory drugs, alone or in combination, showing in vitro efficacy in endometrial cancer cells, which could provide novel therapeutic strategies for advanced EC.

Published
2021

33. Snapshot imprinting: Rapid identification of cancer cell surface proteins and epitopes using molecularly imprinted polymers

Author

Alan C. Spivey, Salvador Macip, Eric O. Aboagye, Stanislav S. Piletsky, Rajinder Singh, Donald J. L. Jones, Marta Braga, Elena V. Piletska, Sergey A. Piletsky, Thong Huy Cao, Marta Poblocka, Imperial College Healthcare NHS Trust- BRC Funding, and Medical Research Council

Subjects
Proteomics, Technology, Chemistry, Multidisciplinary, Cells, EGFR, Materials Science, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Materials Science, Multidisciplinary, Computational biology, Epitope, Epitopes, 0903 Biomedical Engineering, NANOPARTICLES, General Materials Science, HEAD, Imprinting (psychology), Nanoscience & Nanotechnology, Cancer, Science & Technology, 1007 Nanotechnology, Cluster of differentiation, Chemistry, Molecularly imprinted polymer, Molecular diagnostics, Transmembrane protein, Drug development, Molecularly imprinted polymers, Physical Sciences, Science & Technology - Other Topics, SECRETION, Molecular imprinting, STEM-CELLS, Biotechnology
Abstract

Proteomic mapping of cell surfaces is an invaluable tool for drug development and clinical diagnostics. This work describes a new ‘snapshot imprinting’ method designed to obtain proteomic maps of cell surfaces, with the aim of identifying cell surface markers and epitopes for diagnostic and therapeutic applications. The analysis of two cancer cell lines, HN5 and MDA-MB-468, is described herein as a proof of concept, along with the selective targeting of three identified epitopes of epidermal growth factor receptor using molecularly imprinted polymer nanoparticles. 438 proteins were identified using this technique, with 283 considered to be transmembrane or extracellular proteins. The major advantage of the molecular imprinting approach developed here is the ability to analyse cell surface proteins without tedious fractionation, affinity separation or labelling. We believe that this system of protein analysis may provide a basic molecular diagnostics toolbox for precise, personalised treatment of cancer and other diseases.

Published
2021

34. Specific interactions of BCL-2 family proteins mediate sensitivity to BH3-mimetics in diffuse large B-cell lymphoma

Author

Simone Fulda, Anna Dietz, Sandrine Jayne, Victoria M. Smith, Martin J. S. Dyer, Salvador Macip, Meike Vogler, Kristina Henz, Ross Jackson, Daniela Bruecher, Lisa Kowald, and Sjoerd J L van Wijk

Subjects
Bh3 mimetics, Venetoclax, Chronic lymphocytic leukemia, Bcl-2 family, Hematology, medicine.disease, Homology (biology), Lymphoma, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Apoptosis, hemic and lymphatic diseases, medicine, Cancer research, biological phenomena, cell phenomena, and immunity, Diffuse large B-cell lymphoma, 030215 immunology
Abstract

The BCL-2-specific inhibitor, ABT-199 (venetoclax) has exhibited remarkable clinical activity in nearly all cases of chronic lymphocytic leukemia. In contrast, responses are usually much less in diffuse large B-cell lymphoma (DLBCL), despite high level expression of BCL-2 in over 40% of cases, indicating that co-expression of related anti-apoptotic BCL-2 family proteins may limit the activity of ABT-199. We have investigated the roles of BCL-2 proteins in DLBCL cells using a panel of specific BCL-2 homology 3 (BH3)-mimetics and identified subgroups of these cells that exhibited marked and specific dependency on either BCL-2, BCL-XL or MCL-1 for survival. Dependency was associated with selective sequestration of the pro-apoptotic proteins BIM, BAX and BAK by the specific anti-apoptotic BCL-2 protein which was important for cellular survival. Sensitivity to BH3-mimetics was independent of genetic alterations involving the BCL-2 family and only partially correlated with protein expression levels. Treatment with ABT-199 displaced BAX and BIM from BCL-2, subsequently leading to BAK activation and apoptosis. In contrast, apoptosis induced by inhibiting BCL-XL with A1331852 was associated with a displacement of both BAX and BAK from BCL-XL and occurred independently of BIM. Finally, the MCL-1 inhibitor S63845 induced mainly BAX-dependent apoptosis mediated by a displacement of BAK, BIM and NOXA from MCL-1. In conclusion, our study indicates that in DLBCL, the heterogeneous response to BH3-mimetics is mediated by selective interactions between BAX, BAK and anti-apoptotic BCL-2 proteins.

Published
2019

35. Detecting and targeting senescent cells using molecularly imprinted nanoparticles

Author

Michael E. Kelly, Marta Poblocka, Elena V. Piletska, Sergey A. Piletsky, Mohammad Althubiti, Gabriella Kocsis-Fodor, Akang E. Ekpenyong-Akiba, Justyna Janus, Francesco Canfarotta, Laura Castilla-Vallmanya, Salvador Macip, H Bashar Abd, and Mireia Casulleras

Subjects
Senescence, Ageing, Fibrosis, In vivo, Extracellular, medicine, Cancer, General Materials Science, Biology, medicine.disease, In vitro, Epitope, Cell biology
Abstract

The progressive accumulation of senescent cells in tissues in response to damage importantly contributes to pathophysiological conditions such as fibrosis, diabetes, cancer, Alzheimer's and ageing. Consistent with this, eliminating senescent cells prolongs the lifespan and healthspan in animals and ameliorates certain diseases. Detecting and clearing senescent cells from human tissues could therefore have a significant diagnostic and prognostic impact. However, identifying senescent cells in vivo has proven to be complex. To address this, we characterized and validated a panel of novel membrane markers of senescence. Here, we show the application of molecularly imprinted nanoparticles (nanoMIPs) against an extracellular epitope of one of these markers, B2M, to detect senescent cells in vitro and in vivo. We show that nanoMIPs do not elicit toxic responses in the cells or in mice and successfully recognize old animals, which have a higher proportion of senescent cells in their organs. Importantly, nanoMIPs loaded with drugs can specifically kill senescent cells. Our results provide a proof-of-principle assessment of specific and safe nanotechnology-based approaches for senescent cell detection and clearance with potential clinical relevance.

Published
2019

36. Cooperative stabilisation of 14-3-3σ protein-protein interactions

Author

Marta, Falcicchio, Jake A, Ward, Sara Y, Chothia, Jaswir, Basran, Alisha, Mohindra, Salvador, Macip, Pietro, Roversi, and Richard G, Doveston

Subjects
Chemistry
Abstract

14-3-3 proteins are an important family of hub proteins that play important roles in many cellular processes via a large network of interactions with partner proteins. Many of these protein–protein interactions (PPI) are implicated in human diseases such as cancer and neurodegeneration. The stabilisation of selected 14-3-3 PPIs using drug-like ‘molecular glues’ is a novel therapeutic strategy with high potential. However, the examples reported to date have a number of drawbacks in terms of selectivity and potency. Here, we report that WR-1065, the active species of the approved drug amifostine, covalently modifies 14-3-3σ at an isoform-unique cysteine residue, Cys38. This modification leads to isoform-specific stabilisation of two 14-3-3σ PPIs in a manner that is cooperative with a well characterised molecular glue, fusicoccin A. Our findings reveal a novel stabilisation mechanism for 14-3-3σ, an isoform with particular involvement in cancer pathways. This mechanism can be exploited to harness the enhanced potency conveyed by covalent drug molecules and dual ligand cooperativity. This is demonstrated in two cancer cell lines whereby the cooperative behaviour of fusicoccin A and WR-1065 leads to enhanced efficacy for inducing cell death and attenuating cell growth., The aminothiol WR-1065 covalently modifies 14-3-3σ to stabilse its interactions with p53 and ERα. It enhances the effect of fusicoccin A via a cooperative mechanism that leads to 14-3-3 partner-protein specific activty against cancer cells.

Published
2021

37. PML-II regulates ERK and AKT signal activation and IFN alpha-induced cell death

Author

Salvador Macip, Xueqiong Meng, Keith N. Leppard, Yixiang Chen, and Universitat Oberta de Catalunya (UOC)

Subjects
0301 basic medicine, MAPK/ERK pathway, viruses, Apoptosis, Promyelocytic Leukemia Protein, Biochemistry, IFNa, TNF-Related Apoptosis-Inducing Ligand, 0302 clinical medicine, Interferon, Neoplasms, Gene expression, Protein Isoforms, RNA, Small Interfering, biology, Chemistry, virus diseases, RNA-Binding Proteins, Cell biology, ERK, 030220 oncology & carcinogenesis, QR180, Medicine, PML-II, medicine.drug, promyelocytic leukemia protein, Programmed cell death, Tumor suppressor gene, Cell Survival, MAP Kinase Signaling System, RC0254, QH301, 03 medical and health sciences, Promyelocytic leukemia protein, Proto-Oncogene Proteins, medicine, Humans, Molecular Biology, Protein kinase B, QH573-671, Research, AKT, Interferon-alpha, Cell Biology, Apoptotic signaling, apoptotic signaling, 030104 developmental biology, Gene Expression Regulation, biology.protein, Cytology, Apoptosis Regulatory Proteins, IFNα, Proto-Oncogene Proteins c-akt, HeLa Cells
Abstract

BackgroundThe requirement of promyelocytic leukaemia protein (PML) in interferon (IFN)-induced cell apoptosis is well-established. However, the exact mechanisms by which the multiple isoforms of PML protein participate in this process remain not well-understood. We previously demonstrated that PML isoform II (PML-II) positively regulates induced gene expression during a type I IFN response and evaluate here how PML-II contributes to IFNα-induced cell death.MethodsHeLa cells were transiently depleted of PML-II by siRNA treatment and the response of these cells to treatment with IFNα assessed by molecular assays of mRNA and proteins associated with IFN and apoptosis responses.ResultsIn HeLa cells, death during IFNα stimulation was reduced by prior PML-II depletion. PML-II removal also considerably decreased the induced expression of pro-apoptotic ISGs such as ISG54 (IFIT2), and substantially impaired or prevented expression of PUMA and TRAIL, proteins that are associated with the intrinsic and extrinsic apoptotic pathways respectively. Thirdly, PML-II depletion enhanced ERK and AKT pro-survival signaling activation suggesting that PML-II normally suppresses signaling via these pathways, and that lack of PML-II hence led to greater than normal activation of AKT signaling upon IFNα stimulation and consequently increased resistance to IFNα-induced apoptosis.ConclusionsThe positive contribution of PML-II to the expression of various IFNα-induced pro-apoptotic proteins and its inhibition of pro-survival signaling together provide a mechanistic explanation for reduced apoptosis under conditions of PML deficiency and may account for at least part of the role of PML as a tumor suppressor gene.

Published
2021

38. At the Crossroads of Life and Death: The Proteins That Influence Cell Fate Decisions

Author

Vinesh Dhokia, John A. Y. Moss, Salvador Macip, and Joanna L. Fox

Subjects
Cancer Research, Oncology
Abstract

When a cell is damaged, it must decide how to respond. As a consequence of a variety of stresses, cells can induce well-regulated programmes such as senescence, a persistent proliferative arrest that limits their replication. Alternatively, regulated programmed cell death can be induced to remove the irreversibly damaged cells in a controlled manner. These programmes are mainly triggered and controlled by the tumour suppressor protein p53 and its complex network of effectors, but how it decides between these wildly different responses is not fully understood. This review focuses on the key proteins involved both in the regulation and induction of apoptosis and senescence to examine the key events that determine cell fate following damage. Furthermore, we examine how the regulation and activity of these proteins are altered during the progression of many chronic diseases, including cancer.

Published
2022

39. Targeted Senolytic Strategies Based on the Senescent Surfaceome

Author

Marta Poblocka, Akang E. Ekpenyong-Akiba, and Salvador Macip

Subjects
business.industry, Drug delivery, Medicine, business, Bioinformatics, Senolytic, Epitope, Therapeutic strategy
Abstract

The clearance of senescent cells has the potential to become a therapeutic strategy that could be used in many pathologies, ranging from pulmonary fibrosis and diabetes to ageing itself. The initial genetic experiments performed in mouse models are now being recapitulated using chemical compounds that preferentially kill senescent cells, known as senolytics. Senolytic drugs hold an immense clinical potential but their lack of specificity could lead to side effects that would limit their use, especially when treating otherwise healthy aged individuals. Thus, it would be convenient to develop more targeted approaches to the elimination of senescent cells. Here, we discuss the ongoing efforts to design targeted senolytics, with special focus on the utilization of the extracellular epitopes displayed by the senescent surfaceome, and we summarize the avenues of research that have shown the most promising results so far: nanotechnology, cellular therapies and antibody-based drug delivery.

Published
2020

40. ¿Què ens fa humans?

Author

Salvador Macip and Salvador Macip

Abstract

Els humans disposem d'una capacitat única d'entendre la nostra existència. Conèixer les nostres característiques genètiques, bioquímiques i cel·lulars, en el context de la història, la cultura i l'evolució, ens pot ajudar a comprendre'ns millor com a espècie i a respondre, des de la metodologia científica, algunes de les preguntes que ha plantejat tradicionalment la filosofia. En aquest assaig, Macip proposa analitzar la condició humana a través del que anomena «biohumanisme racionalista», una eina que ens ha de permetre transgredir el determinisme biològic per assolir una vida en societat digna i justa.

Published
2022

41. Differential activation of pro-survival pathways in response to CD40LG/IL4 stimulation in chronic lymphocytic leukaemia cells

Author

Sandrine Jayne, Chloé Peubez, Salvador Macip, Martin J. S. Dyer, Gabriella Kocsis-Fodor, and Yixiang Chen

Subjects
Lymphocytic leukaemia, Cell Survival, business.industry, CD40 Ligand, Stimulation, Hematology, Leukemia, Lymphocytic, Chronic, B-Cell, Survival pathways, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, 030220 oncology & carcinogenesis, Cancer research, Humans, Medicine, Interleukin-4, business, Differential (mathematics), Interleukin 4, 030215 immunology
Published
2018

42. Amelioration of age‐related brain function decline by Bruton's tyrosine kinase inhibition

Author

Akang E. Ekpenyong-Akiba, Diana Jurk, Gabriella Kocsis-Fodor, Miran Rada, Yu Shi, Mohammad Althubiti, Sandra Germano, Marta Poblocka, Juan J. Canales, and Salvador Macip

Subjects
0301 basic medicine, Senescence, p53, Aging, DNA damage, healthspan, Progeroid syndromes, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, medicine, Agammaglobulinaemia Tyrosine Kinase, Bruton's tyrosine kinase, cellular senescence, Animals, Humans, Cognitive Dysfunction, Protein Kinase Inhibitors, Progeria, biology, progeria, Brain, Cell Biology, Original Articles, medicine.disease, Cell biology, 030104 developmental biology, chemistry, BTK, Ibrutinib, biology.protein, Phosphorylation, Original Article, Tyrosine kinase, 030217 neurology & neurosurgery
Abstract

One of the hallmarks of aging is the progressive accumulation of senescent cells in organisms, which has been proposed to be a contributing factor to age‐dependent organ dysfunction. We recently reported that Bruton's tyrosine kinase (BTK) is an upstream component of the p53 responses to DNA damage. BTK binds to and phosphorylates p53 and MDM2, which results in increased p53 activity. Consistent with this, blocking BTK impairs p53‐induced senescence. This suggests that sustained BTK inhibition could have an effect on organismal aging by reducing the presence of senescent cells in tissues. Here, we show that ibrutinib, a clinically approved covalent inhibitor of BTK, prolonged the maximum lifespan of a Zmpste24−/− progeroid mice, which also showed a reduction in general age‐related fitness loss. Importantly, we found that certain brain functions were preserved, as seen by reduced anxiety‐like behaviour and better long‐term spatial memory. This was concomitant to a decrease in the expression of specific markers of senescence in the brain, which confirms a lower accumulation of senescent cells after BTK inhibition. Our data show that blocking BTK has a modest increase in lifespan in Zmpste24−/− mice and protects them from a decline in brain performance. This suggests that specific inhibitors could be used in humans to treat progeroid syndromes and prevent the age‐related degeneration of organs such as the brain., We showed that blocking Bruton's tyrosine kinase (BTK) dampens p53 activity and the induction of senescence in vitro. Here, we show that BTK inhibitors increase maximum lifespan and healthspan of progeroid mice. Moreover, they prevent the deterioration of certain cognitive functions and reduce the accumulation of senescent cells in the brain. This suggests that clinically available BTK inhibitors could ameliorate some features of ageing in susceptible patients.

Published
2019

43. Radiotherapy-Induced Senescence and its Effects on Responses to Treatment

Author

Donald J. L. Jones, Salvador Macip, A.F.S. Tabasso, and George D. D. Jones

Subjects
Senescence, Senescent cell, business.industry, medicine.medical_treatment, Neoplastic growth, 030218 nuclear medicine & medical imaging, Ionizing radiation, Radiation therapy, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Neoplasms, Cancer cell, Adjuvant therapy, Cancer research, Medicine, Humans, Radiology, Nuclear Medicine and imaging, business, Cellular Senescence
Abstract

Radiotherapy is still a treatment of choice for many malignancies, often in combination with other strategies. However, its efficacy is limited by the dose that can be safely administered without eliciting serious side-effects, as well as the fact that recurrence is common, particularly in large tumours. Combining radiotherapy with drugs that could sensitise cells to radiation and/or reduce the factors that promote the recovery of the surviving cancer cells is a promising approach. Ionising radiation has been shown to induce senescence and the accumulation of senescent cells creates a microenvironment that facilitates neoplastic growth. This provides a rationale to test the addition of anti-senescent drugs, some of which are already available in the clinic, to radiotherapy protocols. Here, we discuss the relevance of radiotherapy-induced senescent cell accumulation and the potential interventions to minimise its negative effects.

Published
2019

44. The Molecular Physiology of Ageing: New Targets for Regenerative Medicine

Author

Mohammad Althubiti and Salvador Macip

Subjects
Health span, Senescence, Ageing, Molecular physiology, Context (language use), Biology, Neuroscience, Phenotype, Regenerative medicine, Organism
Abstract

Ageing is a multifactorial process that affects almost every living organism. The fact that we have already uncovered many of the molecular pathways that determine the ageing phenotype in humans has allowed us to start studying strategies to slow down or prevent the deleterious effects of time in tissue physiology. Several ongoing lines of research are aimed at defining new therapies that could be used in regenerative medicine, based on the knowledge accumulated on the molecular physiology of ageing. Among those, the most promising focus on preventing the accumulation of old cells, also known as senescent cells. These have been shown to disrupt tissue physiology and to be responsible, at least in part, for many of the symptoms associated with ageing. Consistent with this, clearance of senescent cells results in prolonged lifespan and health span in mammals and thus could be a potent anti-ageing therapy. In this chapter, we will discuss these and other novel approaches for regenerative medicine being developed in the context of the current understanding of cellular ageing.

Published
2019

45. Alex and the Monsters: Together at Home! Coronavirus Days

Author

Jaume Copons, Salvador Macip, Tony Hernandez, Elena Rottier, Jaume Copons, Salvador Macip, Tony Hernandez, and Elena Rottier

Subjects
Monsters--Juvenile fiction, Boys--Juvenile fiction, Toys--Juvenile fiction, Monsters--Comic books, strips, etc, Friendship--Comic books, strips, etc, Restaurants--Comic books, strips, etc
Abstract

Hi! My name is Alex Pianola. Since the coronavirus lockdown began, I've been stuck at home with ten monsters and my parents. Gradually, I've realized that everyone else is in the same situation and we all I have to learn to do everyday things differently. I am eager to go outside, but thanks to the monsters and my friend Lidia, I've learned more about the virus and the whole point of the lockdown. We have to be responsible. We have to support our healthcare system, research and science, but we also need to take care of the planet and of each other, because we are all in the same boat. This special digital edition guide helps young readers learn to live with the coronavirus and play their part in stopping it from spreading. It encourages children to calmly reflect on what they are experiencing and teaches them how to cope with the anxiety that changes in routine can create. The information about COVID-19 is presented in a kid-friendly format and is easy to understand. Great care has been taken to ensure the accuracy of the scientific facts presented, thanks to the input of specialists such as Salvador Macip (doctor, scientist and writer), Toni Hernández (physicist, linguist and teacher) and Elena Rottier (psychologist). Together we will defeat the virus and there will be more Alex and the Monsters adventures!

Published
2020

46. Paper cremat : 10 contes per a 100 anys de Ray Bradbury

Author

Silvia Broome, Anna Carreras, Víctor García Tur, Inés Macpherson, Salvador Macip, Ramon Mas, Jordi Masó, Pep Prieto, Carme Torras, Andrea Jofre, Silvia Broome, Anna Carreras, Víctor García Tur, Inés Macpherson, Salvador Macip, Ramon Mas, Jordi Masó, Pep Prieto, Carme Torras, and Andrea Jofre

Subjects
Science fiction, Catalan, Short stories, Catalan, Catalan fiction--21st century
Abstract

Quan la Inés Macpherson em va proposar publicar aquest recull en homenatge al centenari del naixement de Ray Bradbury, vivíem en un món. Quan la versió digital vegi la llum, serem al bell mig d'un gran canvi. Quan arribi a les llibreries encarnat en paper, el món haurà canviat per sempre. Sembla un relat de Ray Bradbury. No ho és. M'atreveixo a dir, sense massa por a equivocar-me, que la realitat ha estat a l'altura del gran escriptor nord-americà. Enguany fa cent anys del seu naixement i sembla que la realitat s'hagi engrescat a oferir-nos una distopia curulla de trames, subtrames, girs inesperats, drames grotescos, tragicomèdies. Desenes de milers de morts; palaus de gel convertits en tanatoris; poliesportius, vaixells i trens convertits en hospitals; llars d'avis convertides en vaixells de la mort; fosses comunes a Brooklyn; militars condecorats a les rodes de premsa; països sencers tancats a casa; fronteres tancades; creuers en quarantena plens de malalts; una vida a Internet. Hi ha coses que no podem incloure en aquesta llista perquè ara mateix no ens les podem imaginar i quan tanquem aquesta edició encara no hauran passat. Poc abans d'enllestir aquest llibre he llegit un titular que deia que els Mossos d'Esquadra han irromput en una església de Sant Cugat del Vallès on s'estava celebrant una missa. Quan es va anunciar el pacte entre el PSOE i Podemos que va fer possible l'actual govern de l'Estat hi va haver qui, amb més humor que convicció, va dir que amb ells no hi hauria Setmana Santa. No n'hi ha hagut i les misses estan prohibides durant els dies en els quals el confinament és més estricte. Les llibreries estan tancades, ningú crema llibres —si més no, de moment— però quan puguin tornar a obrir potser hem de lamentar massa persianes abaixades per sempre. Les grans empreses d'Internet aprofiten per guanyar encara més avantatge i més d'un govern vol accedir a les dades de geolocalització dels nostres mòbils per assegurar-se que som on hem de ser. Aquests dies sempre som al llindar d'una nova i petita distopia, d'un nou fet que trastoca lleument allò que abans anomenàvem normalitat. Tornarem a sortir al carrer com fèiem abans però el món d'abans no tornarà. El proper Stefan Zweig que escrigui El món d'ahir escriurà una obra molt estranya. Els relats que llegireu en aquest recull us acompanyaran en les emocions i reflexions quan tot això passi, perquè hi estan estretament connectades d'una manera que costa imaginar. Hi trobareu angoixa, desconcert, por, terror, esgarrifança, tristesa, resignació i també una bona dosi d'esperança i confiança en el futur. Aquests contes, com el mateix Ray Bradbury, ens presenten mons possibles que semblen impossibles i ens confronten amb nosaltres mateixos.

Published
2020

47. Les grans epidèmies modernes (edició actualitzada) : La lluita de l'home contra els enemics invisibles

Author

Salvador Macip and Salvador Macip

Abstract

¿Podrem vèncer el coronavirus? La guia bàsica per entendre els virus i les pandèmies. Si podrem vèncer el coronavirus és una pregunta que ens afecta a tots, perquè les malalties infeccioses són un problema global. Comencen en un racó del planeta, però el nostre estil de vida fa que s'estenguin ràpidament. Per això les pandèmies continuaran sent freqüents, i sense la cooperació de la gent no podrem fer front a les infeccions amb garanties d'èxit. El primer que hem d'aconseguir és que els microbis deixin de ser uns grans desconeguts. Aquest llibre ens permetrà entendre millor què vol dir compartir el planeta amb tots aquests enemics invisibles i ens ajudarà a trobar plegats el punt d'equilibri entre l'alarma i la prudència que ens permeti sobreviure com a espècie molts mil·lennis més. Salvador Macip té un prestigiós historial com a investigador a la Gran Bretanya i als Estats Units, i no només té grans coneixements, sinó que a més sap explicar-los. El tema és apassionant. I vital, per tot el que hi ha en joc.

Published
2020

48. Viurem per sempre? : Com la biomedicina ens està canviant la vida

Author

Salvador Macip, Chris Willmott, Salvador Macip, and Chris Willmott

Abstract

En Pere és neuròleg. Puntual, metòdic i prudent. En Jordi, de caràcter optimista i provocador, és biòleg i investiga el càncer. Treballen a prop, cosa que afavoreix les trobades entre tots dos, que aprofiten per xerrar del que els apassiona: enginyeria genètica, medicina regenerativa amb cèl·lules mare, proves genòmiques... Allà on un veu els immensos beneficis per a la salut de les persones, l'altre hi veu els riscos d'una medicina amb un cost econòmic, social i ètic no sempre assumible. La revolució biomèdica que està en marxa farà que puguem viure per sempre?

Published
2020

49. Pro-survival signal inhibition by CDK inhibitor dinaciclib in Chronic Lymphocytic Leukaemia

Author

Ghalia Shelmani, Chris Clements, Yixiang Chen, Sandrine Jayne, Jesvin Samuel, Martin J. S. Dyer, Salvador Macip, and Sandra Germano

Subjects
0301 basic medicine, MAPK/ERK pathway, Cell Survival, Antineoplastic Agents, Apoptosis, Pyridinium Compounds, Pharmacology, Cyclic N-Oxides, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, Cyclin-dependent kinase, Cell Line, Tumor, hemic and lymphatic diseases, Humans, MCL1, Dinaciclib, Protein Kinase Inhibitors, neoplasms, Protein kinase B, PI3K/AKT/mTOR pathway, biology, Cell Cycle, Indolizines, Hematology, Bridged Bicyclo Compounds, Heterocyclic, Leukemia, Lymphocytic, Chronic, B-Cell, Cyclin-Dependent Kinases, 030104 developmental biology, chemistry, Caspases, 030220 oncology & carcinogenesis, Ibrutinib, biology.protein, CDK inhibitor, Signal Transduction
Abstract

Dinaciclib is a cyclin-dependent kinase inhibitor with clinical potential in different cancers, including chronic lymphocytic leukaemia (CLL). In order to better understand its cytotoxic action, we characterized its effects on signalling pathways important for the survival of CLL cells. We found that dinaciclib induced apoptosis through the activation of caspases 8 and 9, which was independent of the presence of cytokines to mimic the environment of proliferation centres or IGVH mutation status. Moreover, treatment with dinaciclib led to the inhibition of oncogenic pathways normally activated in stimulated CLL cells, such as STAT3, NF-κB, p38, PI3K/AKT and RAF/MEK/ERK. Dinaciclib was also able to block the expression of anti-apoptotic proteins of the BCL2 family such as MCL1 and BCL-xL (also termed BCL2L1). Finally, we showed that low concentrations of dinaciclib enhanced cell sensitivity to ibrutinib and the BCL2 inhibitor ABT-199, two drugs with known effects on CLL. Taken together, our data show that dinaciclib targets multiple pro-survival signalling pathways in CLL, which provides a mechanistic explanation for its potent induction of apoptosis. They also support a therapeutic application of cyclin-dependent kinase inhibitors in CLL in combination with other relevant targeted therapies.

Published
2016

50. Differences in the molecular profile of endometrial cancers from British White and British South Asian women

Author

Elizabeth Stannard, Salvador Macip, Rachael Bishop, Paul Symonds, David S. Guttery, Esther L. Moss, Konstantinos Polymeros, and Roger Hew

Subjects
0301 basic medicine, ARID1A, Colorectal cancer, DNA Mutational Analysis, Gene Identification and Analysis, medicine.disease_cause, Cohort Studies, Endocrinology, 0302 clinical medicine, Medicine and Health Sciences, Mutation frequency, Aged, 80 and over, Mutation, Multidisciplinary, biology, High-Throughput Nucleotide Sequencing, DNA, Neoplasm, Middle Aged, Oncology, 030220 oncology & carcinogenesis, Medicine, Immunohistochemistry, Female, Anatomy, Carcinoma, Endometrioid, Research Article, Adult, Histology, Substitution Mutation, Endocrine Disorders, Science, White People, Andrology, 03 medical and health sciences, Uterine Cancer, Germline mutation, Asian People, Diagnostic Medicine, Uterine cancer, Genetics, Diabetes Mellitus, Cancer Detection and Diagnosis, medicine, Humans, PTEN, Mutation Detection, Aged, business.industry, Biology and Life Sciences, Cancers and Neoplasms, medicine.disease, United Kingdom, Endometrial Neoplasms, DNA Repair Enzymes, 030104 developmental biology, Metabolic Disorders, biology.protein, Somatic Mutation, business, Gynecological Tumors
Abstract

ObjectivesTo identify differences in the mutational profile of endometrial tumours between British White (BW) and South Asian (BSA) women.MethodsWe analysed primary tumours from matched cohorts of British White (BW) and British South Asian (BSA) women resident in Leicestershire diagnosed with EC. Next Generation Sequencing was performed to investigate mutational differences in a panel of 10 genes previously identified as being commonly mutated in EC. The presence of somatic Mismatch Repair (MMR) gene deficiencies was determined by immunohistochemistry.ResultsIn total, 57 tumours (27 BSA and 30 BW) were sequenced. There was no significant difference in the overall mutation frequency of the 10 genes analysed; however, numerous differences were observed between the groups. There was a positive association between PIK3CA and PTEN mutations in the BSA group, with 78% of PIK3CA-mutant tumours harbouring a PTEN mutation, whereas only 11% of PIK3CA wild-type (wt) tumours were PTEN mutant positive (p = 0.0012). In BW women, 90% of ARID1A mutant tumours had co-existent PI3K pathway mutations versus 50% of wild-type (wt) ARID1A patients (p = 0.0485). This trend was not significant in the BSA group (p = 0.66). The age at diagnosis was significantly higher in the BW group with a somatic MMR gene deficiency compared to those with no deficiency (72.8 years versus 59.6 years, p = 0.007), whereas this difference was not seen in the BSA group (64 years versus 60 years, p = 0.37).ConclusionWe have identified differences in the mutational profile of primary EC tumours from BW and BSA women. Further research is needed to confirm these findings and to explore their potential implications for early detection, treatment response and prognosis.

Published
2020

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