Your search keyword '"hypoxia inducible factors"' showing total 207 results

1. Paradoxes: Cholesterol and Hypoxia in Preeclampsia.

Author

Hart, Nancy R.

Subjects

*PREECLAMPSIA, *NITRIC-oxide synthases, *PLACENTAL growth factor, *PARADOX, *HYPOXIA-inducible factor 1, *CHOLESTEROL, *BLOOD cholesterol, *HYPOXIA-inducible factors

Abstract

Preeclampsia, a hypertensive disease of pregnancy of unknown etiology, is intensely studied as a model of cardiovascular disease (CVD) not only due to multiple shared pathologic elements but also because changes that develop over decades in CVD appear and resolve within days in preeclampsia. Those affected by preeclampsia and their offspring experience increased lifetime risks of CVD. At the systemic level, preeclampsia is characterized by increased cellular, membrane, and blood levels of cholesterol; however, cholesterol-dependent signaling, such as canonical Wnt/βcatenin, Hedgehog, and endothelial nitric oxide synthase, is downregulated indicating a cholesterol deficit with the upregulation of cholesterol synthesis and efflux. Hypoxia-related signaling in preeclampsia also appears to be paradoxical with increased Hypoxia-Inducible Factors in the placenta but measurably increased oxygen in maternal blood in placental villous spaces. This review addresses the molecular mechanisms by which excessive systemic cholesterol and deficient cholesterol-dependent signaling may arise from the effects of dietary lipid variance and environmental membrane modifiers causing the cellular hypoxia that characterizes preeclampsia. [ABSTRACT FROM AUTHOR]

Published

2024

2. What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster.

Author

Quadros-Mennella, Princy S., Lucin, Kurt M., and White, Robin E.

Subjects

DROSOPHILA melanogaster, STROKE, HYPOXIA-inducible factor 1, TISSUE plasminogen activator, HYPOXIA-inducible factors, DROSOPHILIDAE, NOTCH effect, FRUIT flies

Abstract

Stroke, resulting in hypoxia and glucose deprivation, is a leading cause of death and disability worldwide. Presently, there are no treatments that reduce neuronal damage and preserve function aside from tissue plasminogen activator administration and rehabilitation therapy. Interestingly, Drosophila melanogaster, the common fruit fly, demonstrates robust hypoxic tolerance, characterized by minimal effects on survival and motor function following systemic hypoxia. Due to its organized brain, conserved neurotransmitter systems, and genetic similarity to humans and other mammals, uncovering the mechanisms of Drosophila's tolerance could be a promising approach for the development of new therapeutics. Interestingly, a key facet of hypoxic tolerance in Drosophila is organism-wide metabolic suppression, a response involving multiple genes and pathways. Specifically, studies have demonstrated that pathways associated with oxidative stress, insulin, hypoxia-inducible factors, NFκB, Wnt, Hippo, and Notch, all potentially contribute to Drosophila hypoxic tolerance. While manipulating the oxidative stress response and insulin signaling pathway has similar outcomes in Drosophila hypoxia and the mammalian middle cerebral artery occlusion (MCAO) model of ischemia, effects of Notch pathway manipulation differ between Drosophila and mammals. Additional research is warranted to further explore how other pathways implicated in hypoxic tolerance in Drosophila, such as NFκB, and Hippo, may be utilized to benefit mammalian response to ischemia. Together, these studies demonstrate that exploration of the hypoxic response in Drosophila may lead to new avenues of research for stroke treatment in humans. [ABSTRACT FROM AUTHOR]

Published

2024

3. In vitro investigation of the effect of disulfiram on hypoxia induced NFκB, epithelial to mesenchymal transition and cancer stem cells in glioblastoma cell lines

Author

Azar, Karim and Wang, Weiguang

Subjects

glioblastoma, hypoxia, cancer stem cells, NF?B, disulfiram, epithelial to mesenchymal transition, drug repurposing, hypoxia inducible factors

Abstract

Glioblastoma multiforme (GBM) is one of the most aggressive and lethal cancers with a poor prognosis. Advances in the treatment of GBM are limited due to several resistance mechanisms and limited drug delivery into the central nervous system (CNS) compartment by the blood-brain barrier (BBB) and by actions of the normal brain to counteract tumour-targeting medications. Hypoxia is common in malignant brain tumours such as GBM and plays a significant role in tumour pathobiology. It is widely accepted that hypoxia is a major driver of GBM malignancy. Although it has been confirmed that hypoxia induces GBM stem-like-cells (GSCs), which are highly invasive and resistant to all chemotherapeutic agents, the detailed molecular pathways linking hypoxia, GSC traits and chemoresistance remain obscure. Evidence shows that hypoxia induces cancer stem cell phenotypes via epithelial-to-mesenchymal transition (EMT), promoting therapeutic resistance in most cancers, including GBM. This study demonstrated that spheroid cultured GBM cells consist of a large population of hypoxic cells with CSC and EMT characteristics. GSCs are chemo-resistant and displayed increased levels of HIFs and NFκB activity. Similarly, the hypoxia cultured GBM cells manifested GSC traits, chemoresistance and invasiveness. These results suggest that hypoxia is responsible for GBM stemness, chemoresistance and invasiveness. GBM cells transfected with nuclear factor kappa B-p65 (NFκB-p65) subunit exhibited CSC and EMT markers indicating the essential role of NFκB in maintaining GSC phenotypes. The study also highlighted the significance of NFκB in driving chemoresistance, invasiveness, and the potential role of NFκB as the central regulator of hypoxia-induced stemness in GBM cells. GSC population has the ability of self-renewal, cancer initiation and development of secondary heterogeneous cancer. The very poor prognosis of GBM could largely be attributed to the existence of GSCs, which promote tumour propagation, maintenance, radio- and chemoresistance and local infiltration. In this study, we used Disulfiram (DS), a drug used for more than 65 years in alcoholism clinics, in combination with copper (Cu) to target the NFκB pathway, reverse chemoresistance and block invasion in GSCs. The obtained results showed that DS/Cu is highly cytotoxic to GBM cells and completely eradicated the resistant CSC population at low dose levels in vitro. DS/Cu inhibited the migration and invasion of hypoxia-induced CSC and EMT like GBM cells at low nanomolar concentrations. DS is an FDA approved drug with low toxicity to normal tissues and can pass through the BBB. Further research may lead to the quick translation of DS into cancer clinics and provide new therapeutic options to improve treatment outcomes in GBM patients.

Published

2022

4. Deciphering hypoxia signaling pathways at the transcriptional and post-transcriptional level in leukaemogenesis

Author

Kong, Kay, Kranc, Kamil, Tomlinson, Simon, and Ottersbach, Katrin

Subjects

haematopoietic stem cells, Acute myeloid leukaemia, leukaemic stem cells, hypoxia inducible factors, m6A-Seq, protein YTHDF2, YTHDF2, AML

Abstract

Haematopoietic stem cells (HSC) reside at the top of a hierarchy capable of reconstituting the blood system of an organism throughout its life. HSCs inhabit the bone marrow where the low partial pressure of oxygen and support cells form the HSC niche. Acute myeloid leukaemia (AML) is an aggressive cancer of the haematopoietic stem and progenitor cells with only 20% to 25% of AML patients surviving 5 years or longer following diagnosis, and relapse occurring in about 50% of patients who achieve remission following initial treatment. Leukaemic stem cells (LSC) in AML are capable of self-renewal and generation of leukaemic cells, competing with healthy HSCs in the HSC niche and remodelling the niche to support LSCs at the expense of normal haematopoiesis. Current therapies often fail to eradicate LSCs leading to relapse. N6-methyladenosine (m6A) is a prevalent internal RNA modification in mammalian cells which is implicated in both cancers and hypoxia responses. I developed a novel pipeline for the analysis of m6A-Seq utilising currently available tools and compared the pipeline to the popular MACS2 method for m6A-Seq analysis. The novel pipeline includes a means to test for di'erentially methylated genes, employing a linear model to filter transcripts whose m6A changes correlate closely with RNA template changes. This pipeline was validated in silico using data generated by the Kranc group and publicly available data. With this pipeline, I analysed m6A-Seq data from leukaemic and healthy cKit+ cells generated by the Kranc group and demonstrated di'erential m6A methylation in key genes implicated in leukaemogenesis. Combining published half-life data with results from m6A-Seq, I also found a correlation between width of peaks, their position, and half life of the transcript, providing a new angle of research. I analysed data generated by the Kranc lab in preleukaemic cells to produce a gene expression signature associated with hypoxia response. This gene signature was used to establish a diminished hypoxia response in leukaemic cells deficient in YTHDF2, an m6A reader which mediates the degradation of m6A-methylated mRNA. Combining my findings from leukaemic cells deficient in HIFs (hypoxia inducible factors), I showed despite a down-regulation of hypoxia response genes in YTHDF2-deficient LSCs, predicted HIF1 targets are upregulated, and YTHDF2-deficient LSCs specifically downregulate HIF1 targets which are upregulated under hypoxia responses. I also demonstrated that HIF1 and HIF2 targets overlap and the observed synergistic dysregulation of genes in HIF1 and HIF2 double deficient LSCs upon hypoxia response are mostly due to redundancy of HIF function. Finally, computational analyses of gene and protein expression combined with m6A methylation results from my pipeline revealed processes contributing to the suppression of leukaemia in YTHDF2-deficient LSCs, and I proposed a new model for the mechanisms underlying YTHDF2-deficiency in LSCs which is consistent with published literature, linking m6A regulation, hypoxia responses, and the unfolded protein response.

Published

2022

5. Corrigendum: What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster

Author

Princy S. Quadros-Mennella, Kurt M. Lucin, and Robin E. White

Subjects

hypoxia resistance, Drosophila melanogaster, oxidative stress, insulin, notch, hypoxia inducible factors, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Published

2024

6. What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster

Author

Princy S. Quadros-Mennella, Kurt M. Lucin, and Robin E. White

Subjects

hypoxia resistance, Drosophila melanogaster, oxidative stress, insulin, notch, hypoxia inducible factors, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Stroke, resulting in hypoxia and glucose deprivation, is a leading cause of death and disability worldwide. Presently, there are no treatments that reduce neuronal damage and preserve function aside from tissue plasminogen activator administration and rehabilitation therapy. Interestingly, Drosophila melanogaster, the common fruit fly, demonstrates robust hypoxic tolerance, characterized by minimal effects on survival and motor function following systemic hypoxia. Due to its organized brain, conserved neurotransmitter systems, and genetic similarity to humans and other mammals, uncovering the mechanisms of Drosophila’s tolerance could be a promising approach for the development of new therapeutics. Interestingly, a key facet of hypoxic tolerance in Drosophila is organism-wide metabolic suppression, a response involving multiple genes and pathways. Specifically, studies have demonstrated that pathways associated with oxidative stress, insulin, hypoxia-inducible factors, NFκB, Wnt, Hippo, and Notch, all potentially contribute to Drosophila hypoxic tolerance. While manipulating the oxidative stress response and insulin signaling pathway has similar outcomes in Drosophila hypoxia and the mammalian middle cerebral artery occlusion (MCAO) model of ischemia, effects of Notch pathway manipulation differ between Drosophila and mammals. Additional research is warranted to further explore how other pathways implicated in hypoxic tolerance in Drosophila, such as NFκB, and Hippo, may be utilized to benefit mammalian response to ischemia. Together, these studies demonstrate that exploration of the hypoxic response in Drosophila may lead to new avenues of research for stroke treatment in humans.

Published

2024

7. Effects of Dietary Starch and Dextrin on Growth and Hypoxia Tolerance in Tiger Puffer (Takifugu rubripes)

Author

Shuqing SONG, Yuexing ZHANG, Qiang MA, Houguo XU, Yuliang WEI, and Mengqing LIANG

Subjects

acute hypoxia, carbohydrate, metabolism, hypoxia inducible factors, takifugu rubripes, Aquaculture. Fisheries. Angling, SH1-691

Abstract

Fish meal and fish oil are important sources of protein and lipid in feeds. The lack of fish meal and fish oil supply has become an important limiting factor for the aquaculture industry. The proportion of fish oil and fish meal used in commercial feeds for farmed fish and crustaceans is continually decreasing, while the carbohydrate content is increasing. Carbohydrates are one of the three major nutrients that provide energy for the body. They have a much lower production price than protein and fat. Starch is a polymeric carbohydrate made from glucose molecules; it is the most commonly used in aquatic feeds and can replace fish meal and fish oil to reduce feed cost. Therefore, it is important to fully explore the nutritional function of carbohydrates for aquaculture. Hypoxia is a common stress in aquaculture, and acute hypoxia may lead to massive mortality of cultured fish in a short period of time resulting in serious economic losses to aquaculture. Therefore, it is crucial to find ways to improve the acute hypoxia tolerance of fish. Fish mainly use glucose for energy under acute hypoxia. Hypoxia inhibits oxidative phosphorylation in mitochondria and activates the anaerobic glycolysis pathway. Glucose degrades to produce lactate and ATP. Carnivorous fishes have limited absorption and utilization capacities to feed carbohydrates, unlike omnivorous fishes. Dextrin is an intermediate starch hydrolysis product, with a molecular weight between starch and glucose; it has good adhesion properties and is more easily digested and absorbed than starch. Therefore, we hypothesized that the use of easily digestible carbohydrate in the feed is an effective way to improve the acute hypoxia tolerance of fish. Takifugu rubripes is loved by Japanese and Korean consumers owing to its delicious taste and high nutritional value. It is a characteristic species of Chinese mariculture fish. It is mainly cultured in a high-density factory, and the dissolved oxygen in the water often relies on water exchange and an oxygenation pump; its gill cover is degraded and is at risk of acute hypoxia. This study determined the effect of the addition of corn starch or dextrin (corn starch hydrolysate) to the feed on growth performance, acute hypoxia survival rate, metabolite content, and the hypoxia inducible factor (HIF) signaling pathway of T. rubripes after 8 weeks of feeding. There were no significant differences in weight gain, feed conversion ratio, hepatosomatic index, viscerosomatic index, condition factor, and body composition between the starch group and the dextrin group (P > 0.05). However, the survival rate during acute hypoxia of the dextrin group was significantly higher than that of the starch group (P < 0.05). There were no significant differences in the liver glycogen and lactate contents, and lactate dehydrogenase A4 (ldha) gene expression between the starch group and dextrin group (P > 0.05) during normoxia. However, the lactate content and ldha gene expression were significantly higher in the liver of the dextrin group than those in the starch group (P < 0.05) during hypoxia. This indicated that feeding dextrin strongly activated anaerobic glycolysis to provide more energy under hypoxia. The serum triglyceride (TG) content significantly increased in the dextrin group compared with the normoxia groups, although the TG content in the serum and liver significantly decreased in the starch group after acute hypoxia (P < 0.05). This suggested that feeding starch promoted lipid catabolism and oxygen consumption. There was no significant difference in the total soluble protein content of the muscle between the starch group and the dextrin group (P > 0.05) during normoxia. However, the total soluble protein content of the muscle decreased in the dextrin group compared with the starch group (P < 0.05) after acute hypoxia. Meanwhile, the total muscle soluble protein content, and the gene expression of liver v-akt murine thymoma viral oncogene homolog 1 (akt1), and mechanistic target of rapamycin kinase (mtor) significantly decreased in the dextrin group after hypoxia compared with the normoxia group. However, the liver mtor gene expression significantly increased in the starch group after hypoxia (P < 0.05). This data demonstrated that protein synthesis was inhibited in the dextrin group under hypoxia. Hypoxia inducible factor (HIF) is the most critical transcription factor in cellular response to hypoxic stress. The dextrin group had higher hypoxia inducible factor 1 subunit alpha like (hif-3α) gene expression in the liver and lower hypoxia inducible factor 1 subunit alpha a (hif-1α) gene expression in the muscle (P < 0.05) compared with the starch group during normoxia. The gene expression of liver hif-1α and hif-3α and muscle hif-1α and vascular endothelial growth factor A (vegfa) significantly increased in the dextrin group compared with the starch group (P < 0.05) during hypoxia. This proved that feeding dextrin strongly activated the HIF signaling pathway under hypoxia. In summary, replacing starch with easily digestible dextrin in the feed did not affect the growth performance. Instead, it activated the HIF signaling pathway and anaerobic glycolysis to provide more energy for fish. Meanwhile, feeding dextrin inhibited lipid catabolism and protein synthesis, and reduced oxygen consumption to improve the acute hypoxia tolerance of T. rubripes. The study provides important guidance for the formulation design of hypoxia-tolerant feed and healthy development of aquaculture.

Published

2023

8. Paradoxes: Cholesterol and Hypoxia in Preeclampsia

Author

Nancy R. Hart

Subjects

preeclampsia, hypoxia inducible factors, cholesterol, dietary lipids, Hedgehog (Hh), Wnt/βcatenin, Microbiology, QR1-502

Abstract

Preeclampsia, a hypertensive disease of pregnancy of unknown etiology, is intensely studied as a model of cardiovascular disease (CVD) not only due to multiple shared pathologic elements but also because changes that develop over decades in CVD appear and resolve within days in preeclampsia. Those affected by preeclampsia and their offspring experience increased lifetime risks of CVD. At the systemic level, preeclampsia is characterized by increased cellular, membrane, and blood levels of cholesterol; however, cholesterol-dependent signaling, such as canonical Wnt/βcatenin, Hedgehog, and endothelial nitric oxide synthase, is downregulated indicating a cholesterol deficit with the upregulation of cholesterol synthesis and efflux. Hypoxia-related signaling in preeclampsia also appears to be paradoxical with increased Hypoxia-Inducible Factors in the placenta but measurably increased oxygen in maternal blood in placental villous spaces. This review addresses the molecular mechanisms by which excessive systemic cholesterol and deficient cholesterol-dependent signaling may arise from the effects of dietary lipid variance and environmental membrane modifiers causing the cellular hypoxia that characterizes preeclampsia.

Published

2024

9. Environmental and behavioral regulation of HIF-mitochondria crosstalk.

Author

Burtscher, Johannes, Hohenauer, Erich, Burtscher, Martin, Millet, Grégoire P., and Egg, Margit

Subjects

*ENVIRONMENTAL regulations, *NEUROLOGICAL disorders, *CELL anatomy, *HYPOXEMIA, *MITOCHONDRIA, *DISEASE progression

Abstract

Reduced oxygen availability (hypoxia) can lead to cell and organ damage. Therefore, aerobic species depend on efficient mechanisms to counteract detrimental consequences of hypoxia. Hypoxia inducible factors (HIFs) and mitochondria are integral components of the cellular response to hypoxia and coordinate both distinct and highly intertwined adaptations. This leads to reduced dependence on oxygen, improved oxygen supply, maintained energy provision by metabolic remodeling and tapping into alternative pathways and increased resilience to hypoxic injuries. On one hand, many pathologies are associated with hypoxia and hypoxia can drive disease progression, for example in many cancer and neurological diseases. But on the other hand, controlled induction of hypoxia responses via HIFs and mitochondria can elicit profound health benefits and increase resilience. To tackle pathological hypoxia conditions or to apply health-promoting hypoxia exposures efficiently, cellular and systemic responses to hypoxia need to be well understood. Here we first summarize the well-established link between HIFs and mitochondria in orchestrating hypoxia-induced adaptations and then outline major environmental and behavioral modulators of their interaction that remain poorly understood. [Display omitted] • Hypoxia inducible factors – mitochondria crosstalk underlies adaptations to hypoxia. • Controlled induction of hypoxia responses yields potent health benefits. • Environmental and behavioral conditions modulate adaptations to hypoxia. • Understanding the determinants of adaptation efficiency/safety are key for clinical applications. [ABSTRACT FROM AUTHOR]

Published

2023

10. 双脱甲氧基姜黄素通过调节HIF⁃1α介导衰老诱导非小细胞肺癌 细胞凋亡并抑制细胞增殖.

Author

刘华英, 夏雪, 张孟维, and 罗琴琴

Abstract

Objective To investigate the regulatory effect of dimethoxycurcumin (BDMC) on the proliferation and apoptosis in non⁃small cell lung cancer cells and its mechanism. Methods Non⁃small cell lung cancer cell lines NCI⁃H1975 and NCI⁃H520 were treated with phosphate buffered saline (PBS) and 20 μmol/L BDMC. Cell viability was detected by CCK⁃8; cell proliferation was detected by carboxyfluorescein diacetate succinimide ester (CFSE); cell apoptosis was detected by acridine orange (AO) and Annexin V⁃FITC/PI staining; senescence⁃associated β⁃galactosidase (SA⁃β⁃Gal) staining assay was used to detect the activity of SA⁃β⁃Gal; the proportion of SA⁃β⁃Gal positive cells was detected by flow cytometer. Subsequently, NCI⁃H1975 and NCI⁃H520 cells were treated with 20 μmol/L BDMC, 20 μmol/L hypoxia inducible factor⁃1α (HIF⁃1α) inhibitor PX ⁃478, or a combination of both, respectively, and the cells treated with PBS served as the control group. The expression of HIF⁃1α and HIF⁃2α proteins was detected by Western blot, and the activity of SA⁃β⁃Gal was detected by SA⁃β⁃Gal staining assay. Results Compared with the PBS group, the cell viability of NCI⁃H1975 and NCI⁃H520 in BDMC group was significantly reduced (all P<0.05), the proportion of CFSE⁃positive proliferating cells was significantly reduced (all P<0.01), the number of AO⁃positive cells was significantly decreased (all P<0.01), the proportions of Annexin V+ PIcells and SA⁃β⁃Gal+ PIcells were significantly increased (allP<0.01), the SA⁃β⁃Gal activity was significantly increased (all P<0.001), the protein expression of HIF⁃1α was significantly increased (all P<0.001). Compared with BDMC group, the protein expression of HIF⁃1α in BDMC+PX⁃478 group were decreased (P<0.05), as well as the proportion of SA⁃β⁃Gal⁃positive cells. Conclusions BDMC may promote senescence of non⁃small cell lung cancer cells by up⁃regulating HIF⁃1α signaling pathway, and thus inhibit cell proliferation and promote apoptosis. [ABSTRACT FROM AUTHOR]

Published

2023

11. Estrogen Receptor β4 Regulates Chemotherapy Resistance and Induces Cancer Stem Cells in Triple Negative Breast Cancer.

Author

Bano, Ayesha, Stevens, Jessica H., Modi, Paulomi S., Gustafsson, Jan-Åke, and Strom, Anders M.

Subjects

*TRIPLE-negative breast cancer, *CANCER stem cells, *ESTROGEN receptors, *BREAST, *CANCER chemotherapy, *CELL populations, *LIGAND binding (Biochemistry)

Abstract

Triple Negative Breast Cancer (TNBC) has the worst prognosis among all breast cancers, and survival in patients with recurrence is rarely beyond 12 months due to acquired resistance to chemotherapy, which is the standard of care for these patients. Our hypothesis is that Estrogen Receptor β1 (ERβ1) increases response to chemotherapy but is opposed by ERβ4, which it preferentially dimerizes with. The role of ERβ1 and ERβ4 in influencing chemotherapy sensitivity has never been studied before. CRISPR/CAS9 was used to truncate ERβ1 Ligand Binding Domain (LBD) and knock down the exon unique to ERβ4. We show that the truncated ERβ1 LBD in a variety of mutant p53 TNBC cell lines, where ERβ1 ligand dependent function was inactivated, had increased resistance to Paclitaxel, whereas the ERβ4 knockdown cell line was sensitized to Paclitaxel. We further show that ERβ1 LBD truncation, as well as treatment with ERβ1 antagonist 2-phenyl-3-(4-hydroxyphenyl)-5,7-bis(trifluoromethyl)-pyrazolo[1,5-a] pyrimidine (PHTPP), leads to increase in the drug efflux transporters. Hypoxia Inducible Factors (HIFs) activate factors involved in pluripotency and regulate the stem cell phenotype, both in normal and cancer cells. Here we show that the ERβ1 and ERβ4 regulate these stem cell markers like SOX2, OCT4, and Nanog in an opposing manner; and we further show that this regulation is mediated by HIFs. We show the increase of cancer cell stemness due to ERβ1 LBD truncation is attenuated when HIF1/2α is knocked down by siRNA. Finally, we show an increase in the breast cancer stem cell population due to ERβ1 antagonist using both ALDEFLUORTM and SOX2/OCT4 response element (SORE6) reporters in SUM159 and MDA-MB-231 cell lines. Since most TNBC cancers are ERβ4 positive, while only a small proportion of TNBC patients are ERβ1 positive, we believe that simultaneous activation of ERβ1 with agonists and inactivation of ERβ4, in combination with paclitaxel, can be more efficacious and yield better outcome for chemotherapy resistant TNBC patients. [ABSTRACT FROM AUTHOR]

Published

2023

12. Slow twitch paraspinal muscle dysregulation in adolescent idiopathic scoliosis exhibiting HIF‐2α misexpression.

Author

Tam, Wai Kit, Cheung, Jason P. Y., Koljonen, Paul A., Kwan, Kenny Y. H., Cheung, Kenneth M.C., and Leung, Victor Y. L.

Subjects

ADOLESCENT idiopathic scoliosis, MYOBLASTS, ENZYME-linked immunosorbent assay, GENE expression, REGULATOR genes, SPINE abnormalities, SPINAL surgery, ORTHOPEDIC braces

Abstract

Background: Adolescent idiopathic scoliosis (AIS) refers to a three‐dimensional spinal deformity which has a typical onset during adolescence. In most cases, the cause of the deformity cannot be clearly identified. Unbalanced paraspinal muscle activity in AIS patients was reported and hypoxia was implicated to regulate myogenesis. This study aims to investigate the association between myogenesis/muscle toning and HIF‐αs activity in the pathogenesis of AIS. Methods: HIF‐αs expression was examined by enzyme‐linked immunosorbent assay and western blot in paraspinal myoblasts isolated from 18 subjects who underwent deformity correction surgery. QPCR was conducted to measure the gene expression levels of perinatal muscle fiber markers MYH3, MYH8; slow twitch muscle fiber markers MHY7; fast twitch muscle fiber markers MYH4; and myogenic regulatory factors MYF5 and MYOG. Slow and fast twitch muscle fiber composition in concave/convex paraspinal musculature of AIS subjects was evaluated by immunostaining of myosin heavy chain type I (MyHC I) and myosin heavy chain type II (MyHC II). Results: Reduced HIF‐2α induction under hypoxia was found in paraspinal myoblast culture of 33% AIS subjects. We detected a suppression of perinatal and slow twitch muscle fiber associated genes, but not fast twitch muscle fiber‐associated genes and myogenic regulatory factors in HIF‐2α misexpressed AIS myoblasts. Distinct reduction of slow twitch muscle fiber was evidenced in convex paraspinal musculature, suggesting an asymmetric expression of slow twitch muscle fiber in HIF‐2α misexpressed AIS patients. Conclusions: This study indicates an association of abnormal HIF‐2α expression in paraspinal myoblasts and a disproportionate slow twitch muscle fiber content in the convexity of the curvature in a subset of AIS subjects, suggesting HIF‐2α dysregulation as a possible risk factor for AIS. The role of HIF‐2α in paraspinal muscle function during spinal growth and its relevance in AIS prognosis warrants further investigation. [ABSTRACT FROM AUTHOR]

Published

2022

13. HIF activation enhances FcγRIIb expression on mononuclear phagocytes impeding tumor targeting antibody immunotherapy

Author

Khiyam Hussain, Rena Liu, Rosanna C. G. Smith, Kri T. J. Müller, Mohammadmersad Ghorbani, Sofia Macari, Kirstie L. S. Cleary, Robert J. Oldham, Russell B. Foxall, Sonya James, Steven G. Booth, Tom Murray, Lekh N. Dahal, Chantal E. Hargreaves, Robert S. Kemp, Jemma Longley, James Douglas, Hannah Markham, Serena J. Chee, Richard J. Stopforth, Ali Roghanian, Matthew J. Carter, Christian H. Ottensmeier, Bjorn Frendéus, Ramsey I. Cutress, Ruth R. French, Martin J. Glennie, Jonathan C. Strefford, Stephen M. Thirdborough, Stephen A. Beers, and Mark S. Cragg

Subjects

Hypoxia, Hypoxia inducible factors, FcγRIIb, Fc gamma receptors, Tumor-associated macrophages, Monocytes, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Hypoxia is a hallmark of the tumor microenvironment (TME) and in addition to altering metabolism in cancer cells, it transforms tumor-associated stromal cells. Within the tumor stromal cell compartment, tumor-associated macrophages (TAMs) provide potent pro-tumoral support. However, TAMs can also be harnessed to destroy tumor cells by monoclonal antibody (mAb) immunotherapy, through antibody dependent cellular phagocytosis (ADCP). This is mediated via antibody-binding activating Fc gamma receptors (FcγR) and impaired by the single inhibitory FcγR, FcγRIIb. Methods We applied a multi-OMIC approach coupled with in vitro functional assays and murine tumor models to assess the effects of hypoxia inducible factor (HIF) activation on mAb mediated depletion of human and murine cancer cells. For mechanistic assessments, siRNA-mediated gene silencing, Western blotting and chromatin immune precipitation were utilized to assess the impact of identified regulators on FCGR2B gene transcription. Results We report that TAMs are FcγRIIbbright relative to healthy tissue counterparts and under hypoxic conditions, mononuclear phagocytes markedly upregulate FcγRIIb. This enhanced FcγRIIb expression is transcriptionally driven through HIFs and Activator protein 1 (AP-1). Importantly, this phenotype reduces the ability of macrophages to eliminate anti-CD20 monoclonal antibody (mAb) opsonized human chronic lymphocytic leukemia cells in vitro and EL4 lymphoma cells in vivo in human FcγRIIb+/+ transgenic mice. Furthermore, post-HIF activation, mAb mediated blockade of FcγRIIb can partially restore phagocytic function in human monocytes. Conclusion Our findings provide a detailed molecular and cellular basis for hypoxia driven resistance to antitumor mAb immunotherapy, unveiling a hitherto unexplored aspect of the TME. These findings provide a mechanistic rationale for the modulation of FcγRIIb expression or its blockade as a promising strategy to enhance approved and novel mAb immunotherapies.

Published

2022

14. Decoding lysine-11 signals in ubiquitination

Author

Grice, Guinevere and Lehner, Paul

Subjects

572, Ubiquitin, Proteasome, Hypoxia, HIF, Hypoxia Inducible Factors, PHD, Lysine 11, Prolyl hydroxylation, Mitophagy, V-ATPase, OGDH, LIAS, L2HG

Abstract

The diverse outcomes of ubiquitination primarily relate to the flexibility of ubiquitin in forming homo- or heterotypic chains on each of its seven lysine residues which in turn stimulate distinct downstream signaling pathways. These ubiquitin signals must be selectively initiated on the substrate protein and subsequently decoded to facilitate the desired cellular function. These initiation and decoding steps often involve additional post-translational modifications and ubiquitin receptor proteins, but the enzymes and ubiquitin chains involved for many ubiquitinated substrates are not clear. Here, I have explored the initiation and decoding of ubiquitin signals, focusing on lysine-11 (K11) linked polyubiquitin chains and their role in protein degradation. I established in vitro assays to understand how K11-chains are decoded and whether these chains act as a signal for proteasome-mediated degradation. Pure homotypic K11-chains did not bind the proteasome or its associated ubiquitin binding proteins, but did bind to the mitophagy ubiquitin receptors, MyosinVI and TAX1BP1. Heterotypic K11/K48 linkages not only bound the proteasome but also stimulated degradation of the cell cycle substrate, cyclin B1. To further explore the functions of K11-chains I focused on the hypoxia inducible transcription factor (HIF) pathway, as K11-ubiquitination had been implicated in proteasome-independent degradation of the transcription factor. I established an in vitro assay to initiate HIF ubiquitination, via prolyl hydroxylation, and determine the type of ubiquitin chains involved. Recombinant HIF isoforms were rapidly hydroxylated when incubated with cell extracts. Moreover, the levels of iron and small molecule metabolites within the lysates regulated HIF hydroxylation. However, this hydroxylation was insufficient to reproducibly promote HIF ubiquitination or determine the ubiquitin chains involved. While the nature of the polyubiquitin chains formed in the HIF pathway remain elusive, my studies identify distinct roles for homotypic and heterotypic K11-polyubiquitination in proteasome-mediated degradation.

Published

2018

15. V-ATPase regulation of Hypoxia Inducible transcription Factors

Author

Miles, Anna Louise and Nathan, James

Subjects

571.6, CCDC115, HIF, Iron, PHD, TMEM199, Vacuolar ATPase, Vma12p, Vma22p, Ferritinophagy, Prolyl hydroxylation, Transferrin, Transferrin receptor, Lysosomes, Acidification, Hypoxia Inducible Factors, V-ATPase, Proteasome, Hypoxic response pathway, Endo-lysosomal degradation, IRP2, IRE

Abstract

Metazoans have evolved conserved mechanisms to promote cell survival under low oxygen tensions by initiating a transcriptional cascade centered on the action of Hypoxia Inducible transcription Factors (HIFs). In aerobic conditions, HIFs are inactivated by ubiquitin-proteasome-mediated degradation of their a subunit, which is dependent on prolyl hydroxylation by 2-oxoglutarate (2-OG) and Fe(II)-dependent prolyl hydroxylases (PHDs). In hypoxia, HIF-$\alpha$ is no longer hydroxylated and is therefore stabilised, activating a global transcriptional response to ensure cell survival. Interestingly, HIFs can also be activated in aerobic conditions, however the mechanisms of this oxygen-independent regulation are poorly understood. Here, I have explored the role of the vacuolar H+-ATPase (V-ATPase), the major proton pump for acidifying intracellular vesicles and facilitating lysosomal degradation, in regulating HIF-$\alpha$ turnover. Unbiased forward genetic screens in near-haploid human cells identified that disruption of the V-ATPase leads to activation of HIFs in aerobic conditions. Rather than preventing the lysosomal degradation of HIF-$\alpha$, I found that V-ATPase inhibition indirectly affects the canonical proteasome-mediated degradation of HIF-$\alpha$ isoforms by altering the intracellular iron pool and preventing HIF-$\alpha$ prolyl hydroxylation. In parallel, I characterised two putative mammalian V-ATPase assembly proteins, TMEM199 and CCDC115, identified by the forward genetic screen and subsequent mass spectrometry analysis. I confirmed that both TMEM199 and CCDC115 are required for V-ATPase function, and established assays to determine how TMEM199 and CCDC115 associate with components of the core V-ATPase complex. Lastly, to measure how V-ATPase activity leads to changes in the labile iron pool, I developed an endogenous iron reporter using CRISPR-Cas9 knock-in technology. This approach confirmed that iron homeostasis is impaired during V-ATPase inhibition, and demonstrated that exogenous ferric iron can restore the labile iron pool in a transferrin-independent manner. Together my studies highlight a crucial link between V-ATPase activity, iron homeostasis, and the hypoxic response pathway.

Published

2018

16. Chronic Ketosis Modulates HIF1α-Mediated Inflammatory Response in Rat Brain

Author

Sethuraman, Aarti, Rao, Prahlad, Pranay, Atul, Xu, Kui, LaManna, Joseph C., Puchowicz, Michelle A., Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, Nemoto, Edwin M., editor, Harrison, Eileen M., editor, Pias, Sally C., editor, Bragin, Denis E., editor, Harrison, David K., editor, and LaManna, Joseph C., editor

Published

2021

17. Slow twitch paraspinal muscle dysregulation in adolescent idiopathic scoliosis exhibiting HIF‐2α misexpression

Author

Wai Kit Tam, Jason P. Y. Cheung, Paul A. Koljonen, Kenny Y. H. Kwan, Kenneth M.C. Cheung, and Victor Y. L. Leung

Subjects

adolescent idiopathic scoliosis, hypoxia, hypoxia inducible factors, paraspinal muscle, Orthopedic surgery, RD701-811

Abstract

Abstract Background Adolescent idiopathic scoliosis (AIS) refers to a three‐dimensional spinal deformity which has a typical onset during adolescence. In most cases, the cause of the deformity cannot be clearly identified. Unbalanced paraspinal muscle activity in AIS patients was reported and hypoxia was implicated to regulate myogenesis. This study aims to investigate the association between myogenesis/muscle toning and HIF‐αs activity in the pathogenesis of AIS. Methods HIF‐αs expression was examined by enzyme‐linked immunosorbent assay and western blot in paraspinal myoblasts isolated from 18 subjects who underwent deformity correction surgery. QPCR was conducted to measure the gene expression levels of perinatal muscle fiber markers MYH3, MYH8; slow twitch muscle fiber markers MHY7; fast twitch muscle fiber markers MYH4; and myogenic regulatory factors MYF5 and MYOG. Slow and fast twitch muscle fiber composition in concave/convex paraspinal musculature of AIS subjects was evaluated by immunostaining of myosin heavy chain type I (MyHC I) and myosin heavy chain type II (MyHC II). Results Reduced HIF‐2α induction under hypoxia was found in paraspinal myoblast culture of 33% AIS subjects. We detected a suppression of perinatal and slow twitch muscle fiber associated genes, but not fast twitch muscle fiber‐associated genes and myogenic regulatory factors in HIF‐2α misexpressed AIS myoblasts. Distinct reduction of slow twitch muscle fiber was evidenced in convex paraspinal musculature, suggesting an asymmetric expression of slow twitch muscle fiber in HIF‐2α misexpressed AIS patients. Conclusions This study indicates an association of abnormal HIF‐2α expression in paraspinal myoblasts and a disproportionate slow twitch muscle fiber content in the convexity of the curvature in a subset of AIS subjects, suggesting HIF‐2α dysregulation as a possible risk factor for AIS. The role of HIF‐2α in paraspinal muscle function during spinal growth and its relevance in AIS prognosis warrants further investigation.

Published

2022

18. Effect of Hypoxia in the Transcriptomic Profile of Lung Fibroblasts from Idiopathic Pulmonary Fibrosis.

Author

Romero, Yair, Balderas-Martínez, Yalbi Itzel, Vargas-Morales, Miguel Angel, Castillejos-López, Manuel, Vázquez-Pérez, Joel Armando, Calyeca, Jazmín, Torres-Espíndola, Luz María, Patiño, Nelly, Camarena, Angel, Carlos-Reyes, Ángeles, Flores-Soto, Edgar, León-Reyes, Guadalupe, Sierra-Vargas, Martha Patricia, Herrera, Iliana, Luis-García, Erika Rubí, Ruiz, Víctor, Velázquez-Cruz, Rafael, and Aquino-Gálvez, Arnoldo

Subjects

*LUNGS, *IDIOPATHIC pulmonary fibrosis, *MYOFIBROBLASTS, *HYPOXEMIA, *TRANSCRIPTOMES, *FIBROBLASTS, *EXTRACELLULAR matrix

Abstract

Idiopathic pulmonary fibrosis (IPF) is an aging-associated disease characterized by exacerbated extracellular matrix deposition that disrupts oxygen exchange. Hypoxia and its transcription factors (HIF-1α and 2α) influence numerous circuits that could perpetuate fibrosis by increasing myofibroblasts differentiation and by promoting extracellular matrix accumulation. Therefore, this work aimed to elucidate the signature of hypoxia in the transcriptomic circuitry of IPF-derived fibroblasts. To determine this transcriptomic signature, a gene expression analysis with six lines of lung fibroblasts under normoxia or hypoxia was performed: three cell lines were derived from patients with IPF, and three were from healthy donors, a total of 36 replicates. We used the Clariom D platform, which allows us to evaluate a huge number of transcripts, to analyze the response to hypoxia in both controls and IPF. The control′s response is greater by the number of genes and complexity. In the search for specific genes responsible for the IPF fibroblast phenotype, nineteen dysregulated genes were found in lung fibroblasts from IPF patients in hypoxia (nine upregulated and ten downregulated). In this sense, the signaling pathways revealed to be affected in the pulmonary fibroblasts of patients with IPF may represent an adaptation to chronic hypoxia. [ABSTRACT FROM AUTHOR]

Published

2022

19. Corrigendum: What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster.

Subjects

DROSOPHILA melanogaster, DROSOPHILIDAE, FRUIT flies, OXIDATIVE stress

Abstract

This document is a corrigendum for an article titled "What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster." The corrigendum acknowledges an error in the published article, specifically with Supplementary Figure 1, which was intended to be the Graphical Abstract but was mistakenly omitted from the main article text. The authors apologize for the error and clarify that it does not affect the scientific conclusions of the article. The original article has been updated to include the correct figure. [Extracted from the article]

Published

2024

20. Investigating the effects of chemotherapy and radiation therapy in a prostate cancer model system using SERS nanosensors

Author

Camus, Victoria Louise, Campbell, Colin, Stewart, Grant, McLaren, Duncan, and Nailon, William

Subjects

616.99, intracellular redox potential, cancer tumour models, multicellular tumour spheroids, hypoxia regulators, Hypoxia Inducible Factors, Surface-Enhanced Raman Spectroscopy, SERS, patient-specific

Abstract

Intracellular redox potential (IRP) is a measure of how oxidising or reducing the environment is within a cell. It is a function of numerous factors including redox couples, antioxidant enzymes and reactive oxygen species. Disruption of the tightly regulated redox status has been linked to the initiation and progression of cancer. However, there is very limited knowledge about the quantitative nature of the redox potential and pH gradients that exist in cancer tumour models. Multicellular tumour spheroids (MTS) are three-dimensional cell cultures that possess their own microenvironments, similar to those found in tumours. From the necrotic core to the outer proliferating layer there exist gradients of oxygen, lactate, pH and drug penetration. Tumours also have inadequate vasculature resulting in a state of hypoxia. Hypoxia is a key player in metabolic dysregulation but can also provide cells with resistance against cancer treatments, particularly chemotherapy and radiation therapy. The primary hypoxia regulators are HIFs (Hypoxia Inducible Factors) which under low O2 conditions bind a hypoxia response element, inhibiting oxidative phosphorylation and upregulating glycolysis which has two significant implications: the first is an increase in levels of NADPH/NADH, the main electron donors found in cells which impacts the redox state, whilst the second is a decrease in intracellular pH (pHi) because of increased lactate production. Thus, redox state and intracellular pHi can be used as indicators of metabolic changes within 3D cultures and provide insight into cellular response to therapy. Surface-Enhanced Raman Spectroscopy (SERS) provides a real-time, high resolution method of measuring pHi and IRP in cell culture. It allows for quick and potentially portable analysis of MTS, providing a new platform for monitoring response to drugs and therapy in an unobtrusive manner. Redox and pH-active probes functionalised to Au nanoshells were readily taken up by prostate cancer cell lines and predominantly found to localise in the cytosol. These probes were characterised by density functional theory and spectroelectrochemistry, and their in vitro behaviour modelled by the chemical induction of oxidative and reductive stress. Next, targeting nanosensors to different zones of the MTS allowed for spatial quantification of redox state and pHi throughout the structure and the ability to map the effects of drug treatments on MTS redox biology. The magnitude of the potential gradient can be quantified as free energy (ΔG) and used as a measurement of MTS viability. Treatment of PC3 MTS with staurosporine, an apoptosis inducer, was accompanied by a decrease in free energy gradients over time, whereas treatment of MTS with cisplatin, a drug to which they are resistant, showed an increase in viability indicating a compensatory mechanism and hence resistance. Finally, using this technique the effects of ionising radiation on IRP and pHi in the tumour model was explored. Following exposure to a range of doses of x-ray radiation, as well as single and multi-fractionated regimes, IRP and pHi were measured and MTS viability assessed. Increased radiation dosage diminished the potential gradient across the MTS and decreased viability. Similarly, fractionation of a single large dose was found to enhance MTS death. This novel SERS approach therefore has the potential to not only be used as a mode of drug screening and tool for drug development, but also for pre-clinical characterisation of tumours enabling clinicians to optimise radiation regimes in a patient-specific manner.

Published

2016

21. HIF activation enhances FcγRIIb expression on mononuclear phagocytes impeding tumor targeting antibody immunotherapy.

Author

Hussain, Khiyam, Liu, Rena, Smith, Rosanna C. G., Müller, Kri T. J., Ghorbani, Mohammadmersad, Macari, Sofia, Cleary, Kirstie L. S., Oldham, Robert J., Foxall, Russell B., James, Sonya, Booth, Steven G., Murray, Tom, Dahal, Lekh N., Hargreaves, Chantal E., Kemp, Robert S., Longley, Jemma, Douglas, James, Markham, Hannah, Chee, Serena J., and Stopforth, Richard J.

Subjects

*MACROPHAGES, *AP-1 transcription factor, *CHRONIC lymphocytic leukemia, *STROMAL cells, *FC receptors, *CHRONIC leukemia

Abstract

Background: Hypoxia is a hallmark of the tumor microenvironment (TME) and in addition to altering metabolism in cancer cells, it transforms tumor-associated stromal cells. Within the tumor stromal cell compartment, tumor-associated macrophages (TAMs) provide potent pro-tumoral support. However, TAMs can also be harnessed to destroy tumor cells by monoclonal antibody (mAb) immunotherapy, through antibody dependent cellular phagocytosis (ADCP). This is mediated via antibody-binding activating Fc gamma receptors (FcγR) and impaired by the single inhibitory FcγR, FcγRIIb. Methods: We applied a multi-OMIC approach coupled with in vitro functional assays and murine tumor models to assess the effects of hypoxia inducible factor (HIF) activation on mAb mediated depletion of human and murine cancer cells. For mechanistic assessments, siRNA-mediated gene silencing, Western blotting and chromatin immune precipitation were utilized to assess the impact of identified regulators on FCGR2B gene transcription. Results: We report that TAMs are FcγRIIbbright relative to healthy tissue counterparts and under hypoxic conditions, mononuclear phagocytes markedly upregulate FcγRIIb. This enhanced FcγRIIb expression is transcriptionally driven through HIFs and Activator protein 1 (AP-1). Importantly, this phenotype reduces the ability of macrophages to eliminate anti-CD20 monoclonal antibody (mAb) opsonized human chronic lymphocytic leukemia cells in vitro and EL4 lymphoma cells in vivo in human FcγRIIb+/+ transgenic mice. Furthermore, post-HIF activation, mAb mediated blockade of FcγRIIb can partially restore phagocytic function in human monocytes. Conclusion: Our findings provide a detailed molecular and cellular basis for hypoxia driven resistance to antitumor mAb immunotherapy, unveiling a hitherto unexplored aspect of the TME. These findings provide a mechanistic rationale for the modulation of FcγRIIb expression or its blockade as a promising strategy to enhance approved and novel mAb immunotherapies. [ABSTRACT FROM AUTHOR]

Published

2022

22. UCHL1-dependent control of hypoxia-inducible factor transcriptional activity during liver fibrosis.

Author

Collins A, Scott R, Wilson CL, Abbate G, Ecclestone GB, Albanese AG, Biddles D, White S, French J, Moir J, Alrawashdeh W, Wilson C, Pandanaboyana S, Hammond JS, Thakkar R, Oakley F, Mann J, Mann DA, and Kenneth NS

Subjects

Animals, Humans, Mice, Cell Transdifferentiation genetics, Gene Expression Regulation, Hepatic Stellate Cells metabolism, Hepatic Stellate Cells pathology, Hypoxia-Inducible Factor 1, alpha Subunit metabolism, Hypoxia-Inducible Factor 1, alpha Subunit genetics, Liver Cirrhosis genetics, Liver Cirrhosis pathology, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism

Abstract

Liver fibrosis is the excessive accumulation of extracellular matrix proteins that occurs in most types of chronic liver disease. At the cellular level, liver fibrosis is associated with the activation of hepatic stellate cells (HSCs) which transdifferentiate into a myofibroblast-like phenotype that is contractile, proliferative and profibrogenic. HSC transdifferentiation induces genome-wide changes in gene expression that enable the cell to adopt its profibrogenic functions. We have previously identified that the deubiquitinase ubiquitin C-terminal hydrolase 1 (UCHL1) is highly induced following HSC activation; however, the cellular targets of its deubiquitinating activity are poorly defined. Here, we describe a role for UCHL1 in regulating the levels and activity of hypoxia-inducible factor 1 (HIF1), an oxygen-sensitive transcription factor, during HSC activation and liver fibrosis. HIF1 is elevated during HSC activation and promotes the expression of profibrotic mediator HIF target genes. Increased HIF1α expression correlated with induction of UCHL1 mRNA and protein with HSC activation. Genetic deletion or chemical inhibition of UCHL1 impaired HIF activity through reduction of HIF1α levels. Furthermore, our mechanistic studies have shown that UCHL1 elevates HIF activity through specific cleavage of degradative ubiquitin chains, elevates levels of pro-fibrotic gene expression and increases proliferation rates. As we also show that UCHL1 inhibition blunts fibrogenesis in a pre-clinical 3D human liver slice model of fibrosis, these results demonstrate how small molecule inhibitors of DUBs can exert therapeutic effects through modulation of HIF transcription factors in liver disease. Furthermore, inhibition of HIF activity using UCHL1 inhibitors may represent a therapeutic opportunity with other HIF-related pathologies., (© 2024 The Author(s).)

Published

2024

23. Can Erythropoietin Reduce Hypoxemic Neurological Damages in Neonates With Congenital Heart Defects?

Author

Ottolenghi, Sara, Milano, Giuseppina, Cas, Michele Dei, Findley, Tina O., Paroni, Rita, and Corno, Antonio F.

Subjects

CONGENITAL heart disease, CEREBRAL anoxia-ischemia, CLINICAL medicine, NEWBORN infants, ERYTHROPOIETIN, MYELIN proteins, HEART

Abstract

Congenital heart defects (CHD), the most common cause of birth defects with increasing birth prevalence, affect nearly 1% of live births worldwide. Cyanotic CHD are characterized by hypoxemia, with subsequent reduced oxygen delivery to the brain, especially critical during brain development, beginning in the fetus and continuing through the neonatal period. Therefore, neonates with CHD carry a high risk for neurological comorbidities, even more frequently when there are associated underlying genetic disorders. We review the currently available knowledge on potential prevention strategies to reduce brain damage induced by hypoxemia during fetal development and immediately after birth, and the role of erythropoietin (EPO) as a potential adjunctive treatment. Maternal hyper-oxygenation had been studied as a potential therapeutic to improve fetal oxygenation. Despite demonstrating some effectiveness, maternal hyper-oxygenation has proven to be impractical for extensive clinical application, thus prompting the investigation of specific pathways for pharmacological intervention. Among those, the role of antioxidant pathways and Hypoxia Inducible Factors (HIF) have been studied for their involvement in the protective response to hypoxic injury. One of the proteins induced by HIF, EPO, has properties of being anti-apoptotic, antioxidant, and protective for neurons, astrocytes, and oligodendrocytes. In human trials, EPO administration in neonates with hypoxic ischemic encephalopathy (HIE) significantly reduced the neurological hypoxemic damages in several reported studies. Currently, it is unknown if the mechanisms of pathophysiology of cyanotic CHD are like HIE. Neonates with cyanotic CHD are exposed to both chronic hypoxemia and episodes of acute ischemia-reperfusion injury when undergo cardiopulmonary bypass surgery requiring aortic cross-clamp and general anesthesia. Our review supports future trials to evaluate the potential efficiency of EPO in reducing the hypoxemic neurologic damages in neonates with CHD. Furthermore, it suggests the need to identify early biomarkers of hypoxia-induced neurological damage, which must be sensitive to the neuroprotective effects of EPO. [ABSTRACT FROM AUTHOR]

Published

2021

24. Can Erythropoietin Reduce Hypoxemic Neurological Damages in Neonates With Congenital Heart Defects?

Author

Sara Ottolenghi, Giuseppina Milano, Michele Dei Cas, Tina O. Findley, Rita Paroni, and Antonio F. Corno

Subjects

brain, congenital heart defects, erythropoietin, heart, hypoxemia, hypoxia inducible factors, Therapeutics. Pharmacology, RM1-950

Abstract

Congenital heart defects (CHD), the most common cause of birth defects with increasing birth prevalence, affect nearly 1% of live births worldwide. Cyanotic CHD are characterized by hypoxemia, with subsequent reduced oxygen delivery to the brain, especially critical during brain development, beginning in the fetus and continuing through the neonatal period. Therefore, neonates with CHD carry a high risk for neurological comorbidities, even more frequently when there are associated underlying genetic disorders. We review the currently available knowledge on potential prevention strategies to reduce brain damage induced by hypoxemia during fetal development and immediately after birth, and the role of erythropoietin (EPO) as a potential adjunctive treatment. Maternal hyper-oxygenation had been studied as a potential therapeutic to improve fetal oxygenation. Despite demonstrating some effectiveness, maternal hyper-oxygenation has proven to be impractical for extensive clinical application, thus prompting the investigation of specific pathways for pharmacological intervention. Among those, the role of antioxidant pathways and Hypoxia Inducible Factors (HIF) have been studied for their involvement in the protective response to hypoxic injury. One of the proteins induced by HIF, EPO, has properties of being anti-apoptotic, antioxidant, and protective for neurons, astrocytes, and oligodendrocytes. In human trials, EPO administration in neonates with hypoxic ischemic encephalopathy (HIE) significantly reduced the neurological hypoxemic damages in several reported studies. Currently, it is unknown if the mechanisms of pathophysiology of cyanotic CHD are like HIE. Neonates with cyanotic CHD are exposed to both chronic hypoxemia and episodes of acute ischemia-reperfusion injury when undergo cardiopulmonary bypass surgery requiring aortic cross-clamp and general anesthesia. Our review supports future trials to evaluate the potential efficiency of EPO in reducing the hypoxemic neurologic damages in neonates with CHD. Furthermore, it suggests the need to identify early biomarkers of hypoxia-induced neurological damage, which must be sensitive to the neuroprotective effects of EPO.

Published

2021

25. Effect of Hypoxia in the Transcriptomic Profile of Lung Fibroblasts from Idiopathic Pulmonary Fibrosis

Author

Yair Romero, Yalbi Itzel Balderas-Martínez, Miguel Angel Vargas-Morales, Manuel Castillejos-López, Joel Armando Vázquez-Pérez, Jazmín Calyeca, Luz María Torres-Espíndola, Nelly Patiño, Angel Camarena, Ángeles Carlos-Reyes, Edgar Flores-Soto, Guadalupe León-Reyes, Martha Patricia Sierra-Vargas, Iliana Herrera, Erika Rubí Luis-García, Víctor Ruiz, Rafael Velázquez-Cruz, and Arnoldo Aquino-Gálvez

Subjects

hypoxia inducible factors, microarray, IPF fibroblasts, Cytology, QH573-671

Abstract

Idiopathic pulmonary fibrosis (IPF) is an aging-associated disease characterized by exacerbated extracellular matrix deposition that disrupts oxygen exchange. Hypoxia and its transcription factors (HIF-1α and 2α) influence numerous circuits that could perpetuate fibrosis by increasing myofibroblasts differentiation and by promoting extracellular matrix accumulation. Therefore, this work aimed to elucidate the signature of hypoxia in the transcriptomic circuitry of IPF-derived fibroblasts. To determine this transcriptomic signature, a gene expression analysis with six lines of lung fibroblasts under normoxia or hypoxia was performed: three cell lines were derived from patients with IPF, and three were from healthy donors, a total of 36 replicates. We used the Clariom D platform, which allows us to evaluate a huge number of transcripts, to analyze the response to hypoxia in both controls and IPF. The control′s response is greater by the number of genes and complexity. In the search for specific genes responsible for the IPF fibroblast phenotype, nineteen dysregulated genes were found in lung fibroblasts from IPF patients in hypoxia (nine upregulated and ten downregulated). In this sense, the signaling pathways revealed to be affected in the pulmonary fibroblasts of patients with IPF may represent an adaptation to chronic hypoxia.

Published

2022

26. Dysregulated expression of hypoxia-inducible factors augments myofibroblasts differentiation in idiopathic pulmonary fibrosis

Author

Arnoldo Aquino-Gálvez, Georgina González-Ávila, Laura Lorena Jiménez-Sánchez, Héctor Aquiles Maldonado-Martínez, José Cisneros, Fernanda Toscano-Marquez, Manuel Castillejos-López, Luz María Torres-Espíndola, Rafael Velázquez-Cruz, Víctor Hugo Olivera Rodríguez, Edgar Flores-Soto, Héctor Solís-Chagoyán, Carlos Cabello, Joaquín Zúñiga, and Yair Romero

Subjects

Hypoxia inducible factors, αSMA, Lung fibroblasts, HIF-1α, HIF-2α, HIF-3α, Methylation, Diseases of the respiratory system, RC705-779

Abstract

Abstract Background Idiopathic pulmonary fibrosis (IPF) is an age-related, progressive and lethal disease, whose pathogenesis is associated with fibroblasts/myofibroblasts foci that produce excessive extracellular matrix accumulation in lung parenchyma. Hypoxia has been described as a determinant factor in its development and progression. However, the role of distinct members of this pathway is not completely described. Methods By western blot, quantitative PCR, Immunohistochemistry and Immunocitochemistry were evaluated, the expression HIF alpha subunit isoforms 1, 2 & 3 as well, as their role in myofibroblast differentiation in lung tissue and fibroblast cell lines derived from IPF patients. Results Hypoxia signaling pathway was found very active in lungs and fibroblasts from IPF patients, as demonstrated by the abundance of alpha subunits 1 and 2, which further correlated with the increased expression of myofibroblast marker αSMA. In contrast, HIF-3α showed reduced expression associated with its promoter hypermethylation. Conclusions This study lends further support to the involvement of hypoxia in the pathogenesis of IPF, and poses HIF-3α expression as a potential negative regulator of these phenomena.

Published

2019

27. Centhaquine Restores Renal Blood Flow and Protects Tissue Damage After Hemorrhagic Shock and Renal Ischemia

Author

Amaresh K. Ranjan, Zhong Zhang, Seema Briyal, and Anil Gulati

Subjects

acute kidney injury, hypoxia inducible factors, shock, resuscitation, hemorrhage, centhaquine, Therapeutics. Pharmacology, RM1-950

Abstract

Background: Centhaquine (CQ) (Lyfaquin®) is in late stage clinical development as a safe and effective first-in-class resuscitative agent for hemorrhagic shock patients (NCT02408731, NCT04056065, and NCT04045327). Acute kidney injury (AKI) is known to be associated with hemorrhagic shock. Hence, effect of CQ on protection of kidneys from damage due to hemorrhagic shock was investigated.Methods: To assess effect of CQ on AKI in shock, we created a rat model with hemorrhagic shock and AKI. Renal arteries were clamped and de-clamped to induce AKI like ischemia/reperfusion model and hemorrhage was carried out by withdrawing blood for 30 min. Rats were resuscitated with CQ (0.02 mg/kg) for 10 min. MAP, heart rate (HR), and renal blood flow (RBF) were monitored for 120 min.Results: CQ produced a significant improvement in RBF compared to vehicle (p< 0.003) even though MAP and HR was similar in CQ and vehicle groups. Blood lactate level was lower (p = 0.0064) in CQ than vehicle at 120 min post-resuscitation. Histopathological analysis of tissues indicated greater renal damage in vehicle than CQ. Western blots showed higher HIF-1α (p = 0.0152) and lower NGAL (p = 0.01626) levels in CQ vs vehicle. Immunofluorescence in the kidney cortex and medulla showed significantly higher (p< 0.045) expression of HIF-1α and lower expression of Bax (p< 0.044) in CQ. Expression of PHD 3 (p< 0.0001) was higher, while the expression of Cytochrome C (p = 0.01429) was lower in the cortex of CQ than vehicle.Conclusion: Results show CQ (Lyfaquin®) increased renal blood flow, augmented hypoxia response, decreased tissue damage and apoptosis following hemorrhagic shock induced AKI, and may be explored to prevent/treat AKI.Translational Statement: Centhaquine (CQ) is safe for human use and currently in late stage clinical development as a first-in-class resuscitative agent to treat hemorrhagic shock. In the current study, we have explored a novel role of CQ in protection from hemorrhagic shock induced AKI, indicating its potential to treat/prevent AKI.

Published

2021

28. Co-localisation of intra-nuclear membrane type-1 matrix metalloproteinase and hypoxia inducible factor-2α in osteosarcoma and prostate carcinoma cells.

Author

CHAN, COREY D., HAAGENSEN, EMMA J., TENSAOUT, HAYEIT A., RENNIE, KATHERINE J., GAMIE, ZAKAREYA, BARRY, JAMES, BIRCH, MARK A., GERRAND, CRAIG H., NISAR, SOHAIL, ROBSON, CRAIG N., LUNEC, JOHN, and RANKIN, KENNETH S.

Subjects

*OSTEOSARCOMA, *PROSTATE, *HYPOXEMIA, *SUBCELLULAR fractionation, *PROTEIN-protein interactions, *CASTRATION-resistant prostate cancer

Abstract

Increased membrane type-1 matrix metalloproteinase (MT1-MMP) expression in osteosarcoma is predictive of poor prognosis and directs bone metastasis in prostate carcinoma. MT1-MMP subcellular localisation varies with oxygen tension, and, therefore, the aim of the present study was to assess protein interactions between MT1-MMP and the hypoxia inducible factors (HIF-1α and HIF-2α). MT1-MMP protein expression was investigated across a panel of cancer cell lines, including a positive and negative control. The hypoxia-induced alteration in subcellular location of MT1-MMP, HIF-1α and HIF-2α in the U2OS osteosarcoma cell line was assessed using subcellular fractionation. A proximity ligation assay was utilised to assess protein to protein interactions in the osteosarcoma U2OS and prostate carcinoma PC3 cell lines. U2OS and PC3 cells exhibited a significantly increased intra-nuclear interaction between MT1-MMP and HIF-2α in response to hypoxia. The role of this warrants further investigation as it may unveil novel opportunities to target MT1-MMP, which is of particular significance for osteosarcoma since current treatment options are limited. [ABSTRACT FROM AUTHOR]

Published

2021

29. Corrigendum: What can the common fruit fly teach us about stroke?: lessons learned from the hypoxic tolerant Drosophila melanogaster .

Author

Quadros-Mennella PS, Lucin KM, and White RE

Abstract

[This corrects the article DOI: 10.3389/fncel.2024.1347980.]., (Copyright © 2024 Quadros-Mennella, Lucin and White.)

Published

2024

30. Role of Deranged Energy Deprivation Signaling in the Pathogenesis of Cardiac and Renal Disease in States of Perceived Nutrient Overabundance.

Author

Packer, Milton

Subjects

*PATHOLOGY, *SODIUM-glucose cotransporter 2 inhibitors, *KIDNEY diseases, *HEART diseases, *CHRONIC kidney failure, *KIDNEY failure, *HEART disease diagnosis, *KIDNEY disease diagnosis, *OXYGEN consumption, *MOTIVATION (Psychology), *AUTOPHAGY, *CELLULAR signal transduction, *OXIDATIVE stress, *TYPE 2 diabetes, *DISEASE susceptibility, *TRANSFERASES

Abstract

Sodium-glucose cotransporter 2 inhibitors reduce the risk of serious heart failure and adverse renal events, but the mechanisms that underlie this benefit are not understood. Treatment with SGLT2 inhibitors is distinguished by 2 intriguing features: ketogenesis and erythrocytosis. Both reflect the induction of a fasting-like and hypoxia-like transcriptional paradigm that is capable of restoring and maintaining cellular homeostasis and survival. In the face of perceived nutrient and oxygen deprivation, cells activate low-energy sensors, which include sirtuin-1 (SIRT1), AMP-activated protein kinase (AMPK), and hypoxia inducible factors (HIFs; especially HIF-2α); these enzymes and transcription factors are master regulators of hundreds of genes and proteins that maintain cellular homeostasis. The activation of SIRT1 (through its effects to promote gluconeogenesis and fatty acid oxidation) drives ketogenesis, and working in concert with AMPK, it can directly inhibit inflammasome activation and maintain mitochondrial capacity and stability. HIFs act to promote oxygen delivery (by stimulating erythropoietin and erythrocytosis) and decrease oxygen consumption. The activation of SIRT1, AMPK, and HIF-2α enhances autophagy, a lysosome-dependent degradative pathway that removes dangerous constituents, particularly damaged mitochondria and peroxisomes, which are major sources of oxidative stress and triggers of cellular dysfunction and death. SIRT1 and AMPK also act on sodium transport mechanisms to reduce intracellular sodium concentrations. It is interesting that type 2 diabetes mellitus, obesity, chronic heart failure, and chronic kidney failure are characterized by the accumulation of intracellular glucose and lipid intermediates that are perceived by cells as indicators of energy overabundance. The cells respond by downregulating SIRT1, AMPK, and HIF-2α, thus leading to an impairment of autophagic flux and acceleration of cardiomyopathy and nephropathy. SGLT2 inhibitors reverse this maladaptive signaling by triggering a state of fasting and hypoxia mimicry, which includes activation of SIRT1, AMPK, and HIF-2α, enhanced autophagic flux, reduced cellular stress, decreased sodium influx into cells, and restoration of mitochondrial homeostasis. This mechanistic framework clarifies the findings of large-scale randomized trials and the close association of ketogenesis and erythrocytosis with the cardioprotective and renoprotective benefits of these drugs. [ABSTRACT FROM AUTHOR]

Published

2020

31. Tumor Microenvironment

Author

Ribatti, Domenico and Ribatti, Domenico

Published

2016

32. The Defining Characteristics of Pulmonary Arterial Hypertension

Author

Kumar, Rahul, Robinson, Jeffrey C., Tuder, Rubin M., Maron, Bradley A., editor, Zamanian, Roham T., editor, and Waxman, Aaron B., editor

Published

2016

33. Role of Nitric Oxide in the Regulation of the Pro-tumourigenic Hypoxic Phenotype: From Instigation to Mitigation

Author

Postovit, Lynne-Marie and Bonavida, Benjamin, editor

Published

2015

34. Insight into Hypoxia Stemness Control

Author

Miriam Di Mattia, Annunziata Mauro, Maria Rita Citeroni, Beatrice Dufrusine, Alessia Peserico, Valentina Russo, Paolo Berardinelli, Enrico Dainese, Annamaria Cimini, and Barbara Barboni

Subjects

hypoxia, O2 tension, hypoxia inducible factors, intracellular signaling, metabolism, stemness, Cytology, QH573-671

Abstract

Recently, the research on stemness and multilineage differentiation mechanisms has greatly increased its value due to the potential therapeutic impact of stem cell-based approaches. Stem cells modulate their self-renewing and differentiation capacities in response to endogenous and/or extrinsic factors that can control stem cell fate. One key factor controlling stem cell phenotype is oxygen (O2). Several pieces of evidence demonstrated that the complexity of reproducing O2 physiological tensions and gradients in culture is responsible for defective stem cell behavior in vitro and after transplantation. This evidence is still worsened by considering that stem cells are conventionally incubated under non-physiological air O2 tension (21%). Therefore, the study of mechanisms and signaling activated at lower O2 tension, such as those existing under native microenvironments (referred to as hypoxia), represent an effective strategy to define if O2 is essential in preserving naïve stemness potential as well as in modulating their differentiation. Starting from this premise, the goal of the present review is to report the status of the art about the link existing between hypoxia and stemness providing insight into the factors/molecules involved, to design targeted strategies that, recapitulating naïve O2 signals, enable towards the therapeutic use of stem cell for tissue engineering and regenerative medicine.

Published

2021

35. Iron regulatory protein 2 modulates the switch from aerobic glycolysis to oxidative phosphorylation in mouse embryonic fibroblasts.

Author

Huihui Li, Yutong Liu, Longcheng Shang, Jing Cai, Jing Wu, Wei Zhang, Xiaojiang Pu, Weichen Dong, Tong Qiao, and Kuanyu Li

Subjects

*IRON regulatory proteins, *HOMEOSTASIS, *ENERGY metabolism, *DIMERIZATION, *GENE expression, *ELECTRON transport

Abstract

The importance of the role of iron regulatory proteins (IRPs) in mitochondrial iron homeostasis and function has been raised. To understand how an IRP affects mitochondrial function, we used globally Irp2-depleted mouse embryonic fibroblasts (MEFs) and found that Irp2 ablation significantly induced the expression of both hypoxia-inducible factor subunits, Hif1α and Hif2α. The increase of Hif1α up-regulated its targeted genes, enhancing glycolysis, and the increase of Hif2α down-regulated the expression of iron-sulfur cluster (Fe-S) biogenesis-related and electron transport chain (ETC)-related genes, weakening mitochondrial respiration. Inhibition of Hif1α by genetic knockdown or a specific inhibitor prevented Hif1α-targeted gene expression, leading to decreased aerobic glycolysis. Inhibition of Hif2α by genetic knockdown or selective disruption of the heterodimerization of Hif2α and Hif1β restored the mitochondrial ETC and coupled oxidative phosphorylation (OXPHOS) by enhancing Fe-S biogenesis and increasing ETCrelated gene expression. Our results indicate that Irp2 modulates the metabolic switch from aerobic glycolysis to OXPHOS that is mediated by Hif1α and Hif2α in MEFs. [ABSTRACT FROM AUTHOR]

Published

2019

36. Endothelial Hypoxia-Inducible Factor-2α Is Required for the Maintenance of Airway Microvasculature.

Author

Cain, Corey, Jiang, Xinguo, Tian, Wen, Tu, Allen B., Pasupneti, Shravani, Shuffle, Eric, Dahms, Petra, Zhang, Patrick, Dinh, Thanh T., Liu, Bo, Butcher, Eugene C., Nicolls, Mark R., Giaccia, Amato J., Cai, Haoliang, Simon, M. Celeste, and Semenza, Gregg L.

Subjects

*HYPOXIA-inducible factor 1, *HYPOXIA-inducible factors, *ENDOTHELIAL cells, *ANIMAL genetics, *HUMAN genetics, *LUNG diseases

Abstract

Supplemental Digital Content is available in the text. Background: Hypoxia-inducible factors (HIFs), especially HIF-1α and HIF-2α, are key mediators of the adaptive response to hypoxic stress and play essential roles in maintaining lung homeostasis. Human and animal genetics studies confirm that abnormal HIF correlates with pulmonary vascular pathology and chronic lung diseases, but it remains unclear whether endothelial cell HIF production is essential for microvascular health. The large airway has an ideal circulatory bed for evaluating histological changes and physiology in genetically modified rodents. Methods: The tracheal microvasculature of mice, with conditionally deleted or overexpressed HIF-1α or HIF-2α, was evaluated for anatomy, perfusion, and permeability. Angiogenic signaling studies assessed vascular changes attributable to dysregulated HIF expression. An orthotopic tracheal transplantation model further evaluated the contribution of individual HIF isoforms in airway endothelial cells. Results: The genetic deletion of Hif-2α but not Hif-1α caused tracheal endothelial cell apoptosis, diminished pericyte coverage, reduced vascular perfusion, defective barrier function, overlying epithelial abnormalities, and subepithelial fibrotic remodeling. HIF-2α promoted microvascular integrity in airways through endothelial angiopoietin-1/TIE2 signaling and Notch activity. In functional tracheal transplants, HIF-2α deficiency in airway donors accelerated graft microvascular loss, whereas HIF-2α or angiopoietin-1 overexpression prolonged transplant microvascular perfusion. Augmented endothelial HIF-2α in transplant donors promoted airway microvascular integrity and diminished alloimmune inflammation. Conclusions: Our findings reveal that the constitutive expression of endothelial HIF-2α is required for airway microvascular health. [ABSTRACT FROM AUTHOR]

Published

2019

37. Cobalt treatment does not prevent glomerular morphological alterations in type 1 diabetic rats.

Author

Singh, Gaaminepreet and Krishan, Pawan

Abstract

Early renal morphological alterations including glomerular hypertrophy and mesangial expansion occur in diabetic kidney disease and correlate with various clinical manifestations of diabetes. The present study was designed to investigate the influence of pharmacological modulation of HIF-1α (hypoxia inducible factor-1 alpha) protein levels, on these glomerular changes in rodent model of type 1 diabetes. Male wistar rats were made diabetic (Streptozotocin 45 mg/kg; i.p.) and afterwards treated with HIF activator cobalt chloride for 4 weeks. Renal function was assessed by serum creatinine, albumin, proteinuria levels, oxidative stress: reduced glutathione levels and catalase activity, and renal tissue HIF-1α protein levels were determined by ELISA assay. Histological analysis of kidney sections was done by haematoxylin and eosin (glomeruli diameter), periodic acid Schiff (mesangial expansion and glomerulosclerosis) and sirius red (fibrosis, tubular dilation) staining. Diabetes rats displayed reduced serum albumin levels, marked proteinuria, lower kidney reduced glutathione content, glomerular hypertrophy, glomerulosclerosis, mesangial expansion, tubular dilation and renal fibrosis. Cobalt chloride treatment normalised renal HIF-1α protein levels, reduced development of proteinuria and tubulo-interstitial fibrosis, but the glomerular morphological alterations such as glomerulosclerosis, mesangial expansion, increased glomerular diameter and tubular vacoulations were not abrogated in diabetic kidneys. Glomerular morphological abnormalities might precede the development of proteinuria and renal fibrosis in experimental model of type 1 diabetes. Pharmacological modulation of renal HIF-1α protein levels does not influence glomerular and tubular dilatory changes in diabetic kidney disease. [ABSTRACT FROM AUTHOR]

Published

2018

38. NAP counteracts hyperglycemia/hypoxia induced retinal pigment epithelial barrier breakdown through modulation of HIFs and VEGF expression.

Author

D'Amico, Agata G., Maugeri, Grazia, Rasà, Daniela M., La Cognata, Valentina, Saccone, Salvatore, Federico, Concetta, Cavallaro, Sebastiano, and D'Agata, Velia

Subjects

*HYPERGLYCEMIA treatment, *HYPOXEMIA, *RHODOPSIN, *EPITHELIUM, *NEUROPROTECTIVE agents, *EDEMA, *DIABETES complications, *THERAPEUTICS, *DISEASE risk factors

Abstract

Diabetic macular edema (DME) is a common complication leading to a central vision loss in patients with diabetes. In this eye pathology, the hyperglycaemic/hypoxic microenvironment of pigmented epithelium is responsible for outer blood retinal barrier integrity changes. More recently, we have shown that a small peptide derived from the activity-dependent neuroprotective protein (ADNP), known as NAP, counteracts damages occurring during progression of diabetic retinopathy by modulating HIFs/VEGF pathway. Here, we have investigated for the first time the role of this peptide on outer blood retinal barrier (BRB) integrity exposed to hyperglycaemic/hypoxic insult mimicking a model in vitro of DME. To characterize NAP role on disease's pathogenesis, we have analyzed its effect on HIFs/VEGF system in human retinal pigmented epithelial cells, ARPE-19, grown in high glucose and low oxygen tension. The results have shown that NAP prevents outer BRB breakdown by reducing HIF1a/HIF2a, VEGF/VEGFRs, and increasing HIF3a expression, moreover it is able to reduce the percentage of apoptotic cells by modulating the expression of two death related genes, BAX and Bcl2. Further investigations are needed to determine the possible use of NAP in DME treatment. [ABSTRACT FROM AUTHOR]

Published

2018

39. A Cardioprotective Role of Nerium oleander with the Expression of Hypoxia Inducible Factor 2A mRNA by Increasing Antioxidant Enzymes in Rat Heart Tissue.

Author

Hitit, Mustafa, Corum, Orhan, Corum, Duygu Durna, Donmez, Huseyin, Cetin, Gul, Dik, Burak, and Er, Ayse

Subjects

*CARDIOTONIC agents, *OLEANDER, *HYPOXIA-inducible factors, *MESSENGER RNA, *ANTIOXIDANTS

Abstract

Background: Nerium oleander (NO) distillate is used to either protect heart cells against oxidative stress or reduce the risk of cardiovascular disease by regulating the production of reactive oxygen species. Hypoxia-inducible factors (HIFs) regulate cellular antioxidant defense mechanisms under hypoxic conditions in which heart cells survive; however, the key responsible mechanism of NO distillate for cardioprotection remains elusive. The objective of this study was to evaluate the effects on heart tissue at different time intervals after administering NO distillate intraperitoneally (IP) while considering the transcriptional regulation of HIFs and representative antioxidant enzymes. Materials, Methods & Results: The NO plant was chopped, and distillated water was added. The mixture was distilled, and the distillate separated and collected into tubes, after which it was lyophilized to obtain dry material. Twenty male Wistar albino rats (2-3 month-old, 250-300 g each) were used in the study. The rats were randomly divided into four groups. The control group (n = 5) received IP injections of saline; the remaining 15 rats received IP injections of a single dose of 7.5 mL NO distillate. The NO distillate injected rats were divided into three groups according to the time from injection to harvest the heart tissue samples. The tissues were collected at 0 h (control; n = 5), 2 h (group 2; n = 5), 4 h (group 3; n = 5), and 8 h (group 4; n = 5) after injection and under general anesthesia (60 mg/kg ketamine, IP + 10 mg/kg xylazine, IP). Quantitative polymerase chain reaction (qPCR) was used to assess the expression profiles of the genes of interest in the heart tissues. Hypoxanthine phosphoribosyltransferase was used as the reference gene. The expression of manganese superoxide dismutase (MnSOD) mRNA was in a steady state level between the control group and group 2 (P > 0.05); however, it significantly increased in group 3 and 4 compared with that in the control (P < 0.05). Expression of catalase (CAT) mRNA was significantly higher in group 2 than in the control group (P < 0.05) although it was lower in group 3 and 4 than in group 2 (P < 0.05); however, it appeared to be similar among the control group, group 3, and group 4 (P > 0.05). Copper (Cu) SOD mRNA was equally expressed in both the control group and group 2 (P > 0.05) but was lower in group 3 and 4 than in group 2 (P < 0.05). Expressions of HIF1A, HIF2A, and HIF3A mRNA were detected in the rat heart tissues in the control and 2, 4, and 8 h after administration of NO distillate. Expression of HIF1A mRNA was in a steady state and did not differ among groups 2, 3, and 4 (P > 0.05). Similarly, the expression of HIF2A mRNA did not change between the control group and group 2 (P > 0.05); however, it was higher in group 3 than in the control (P < 0.05) and tended to be higher in group 3 than in group 2 (P = 0.063). HIF3A mRNA expression did not change significantly in the heart tissue of any of the groups (P > 0.05). Discussion: The present study using rats determined that MnSOD, CAT, CuSOD, HIF1A, HIF2A, and HIF3A mRNA are expressed in the heart tissues after administration of NO distillate. The increased expression of HIF2A mRNA after 4 h in accordance with a rise in CAT mRNA after 2 h, and MnSOD mRNA after 4 and 8 h might confirm the role of HIF2A mRNA in oxidative stress defense by regulating antioxidant enzymes; consequently, this study may expand our understanding of uses of NO distillate with respect to molecular pathways. [ABSTRACT FROM AUTHOR]

Published

2018

40. Role of ROS/Kv/HIF Axis in the Development of Hypoxia-Induced Pulmonary Hypertension.

Author

Wu, Wen, Li, Yan, and Xu, Dunquan

Subjects

*OBSTRUCTIVE lung diseases, *PULMONARY hypertension, *HYPOXEMIA, *POTASSIUM channels, *REACTIVE oxygen species, *HYPERTENSION

Abstract

Hypoxic pulmonary hypertension (HPH) is a common complication in patients with chronic obstructive pulmonary disease (COPD), sleep-disordered breathing, or dwellers in high altitude. The exact mechanisms underlying the development of HPH still remain unclear. Reactive oxygen species (ROS), hypoxia inducible factors (HIF), and potassium channels (K V ) are believed as the main factors during the development of HPH. We propose that the “ROS/Kv/HIF axis” may play an important initiating role in the development of HPH. Being formed under a hypoxic condition, ROS affects the expression and function of HIFs or K V , and consequently triggers multiple downstream signaling pathways and genes expression that participate in promoting pulmonary vasoconstriction and arterial remodeling. Thus, further study determining the initiating role of “ROS/Kv/HIF axis” in the development of HPH could provide theoretic evidences to better understand the underlying mechanisms of HPH, and help identify new potential targets in the treatment of HPH. [ABSTRACT FROM AUTHOR]

Published

2017

41. The vacuolar-ATPase complex and assembly factors, TMEM199 and CCDC115, control HIF1α prolyl hydroxylation by regulating cellular iron levels

Author

Anna L Miles, Stephen P Burr, Guinevere L Grice, and James A Nathan

Subjects

Vacuolar ATPase, Hypoxia Inducible factors, Iron, HIF, Vma12, Vma22, Medicine, Science, Biology (General), QH301-705.5

Abstract

Hypoxia Inducible transcription Factors (HIFs) are principally regulated by the 2-oxoglutarate and Iron(II) prolyl hydroxylase (PHD) enzymes, which hydroxylate the HIFα subunit, facilitating its proteasome-mediated degradation. Observations that HIFα hydroxylation can be impaired even when oxygen is sufficient emphasise the importance of understanding the complex nature of PHD regulation. Here, we use an unbiased genome-wide genetic screen in near-haploid human cells to uncover cellular processes that regulate HIF1α. We identify that genetic disruption of the Vacuolar H+ ATPase (V-ATPase), the key proton pump for endo-lysosomal acidification, and two previously uncharacterised V-ATPase assembly factors, TMEM199 and CCDC115, stabilise HIF1α in aerobic conditions. Rather than preventing the lysosomal degradation of HIF1α, disrupting the V-ATPase results in intracellular iron depletion, thereby impairing PHD activity and leading to HIF activation. Iron supplementation directly restores PHD catalytic activity following V-ATPase inhibition, revealing important links between the V-ATPase, iron metabolism and HIFs.

Published

2017

42. Int6/eIF3e Is Essential for Proliferation and Survival of Human Glioblastoma Cells

Author

Julie Sesen, Anne Cammas, Sarah J. Scotland, Bertand Elefterion, Anthony Lemarié, Stefania Millevoi, Lijoy K. Mathew, Cathy Seva, Christine Toulas, Elizabeth Cohen-Jonathan Moyal, and Nicolas Skuli

Subjects

glioma, glioblastoma, proliferation, apoptosis, eukaryotic translation initiation factor, Int6, eIF3e, Hypoxia Inducible Factors, HIF-1α, HIF-2α, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Glioblastomas (GBM) are very aggressive and malignant brain tumors, with frequent relapses despite an appropriate treatment combining surgery, chemotherapy and radiotherapy. In GBM, hypoxia is a characteristic feature and activation of Hypoxia Inducible Factors (HIF-1α and HIF-2α) has been associated with resistance to anti-cancer therapeutics. Int6, also named eIF3e, is the “e” subunit of the translation initiation factor eIF3, and was identified as novel regulator of HIF-2α. Eukaryotic initiation factors (eIFs) are key factors regulating total protein synthesis, which controls cell growth, size and proliferation. The functional significance of Int6 and the effect of Int6/EIF3E gene silencing on human brain GBM has not yet been described and its role on the HIFs is unknown in glioma cells. In the present study, we show that Int6/eIF3e suppression affects cell proliferation, cell cycle and apoptosis of various GBM cells. We highlight that Int6 inhibition induces a diminution of proliferation through cell cycle arrest and increased apoptosis. Surprisingly, these phenotypes are independent of global cell translation inhibition and are accompanied by decreased HIF expression when Int6 is silenced. In conclusion, we demonstrate here that Int6/eIF3e is essential for proliferation and survival of GBM cells, presumably through modulation of the HIFs.

Published

2014

43. The Importance of Physioxia in Mesenchymal Stem Cell Chondrogenesis and the Mechanisms Controlling Its Response

Author

Girish Pattappa, Brian Johnstone, Johannes Zellner, Denitsa Docheva, and Peter Angele

Subjects

mesenchymal stem cells, chondrogenesis, hypoxia, cartilage, hypertrophy, hypoxia inducible factors, early osteoarthritis, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Articular cartilage covers the surface of synovial joints and enables joint movement. However, it is susceptible to progressive degeneration with age that can be accelerated by either previous joint injury or meniscectomy. This degenerative disease is known as osteoarthritis (OA) and it greatly affects the adult population. Cell-based tissue engineering provides a possible solution for treating OA at its earliest stages, particularly focal cartilage lesions. A candidate cell type for treating these focal defects are Mesenchymal Stem Cells (MSCs). However, present methods for differentiating these cells towards the chondrogenic lineage lead to hypertrophic chondrocytes and bone formation in vivo. Environmental stimuli that can stabilise the articular chondrocyte phenotype without compromising tissue formation have been extensively investigated. One factor that has generated intensive investigation in MSC chondrogenesis is low oxygen tension or physioxia (2⁻5% oxygen). In vivo articular cartilage resides at oxygen tensions between 1⁻4%, and in vitro results suggest that these conditions are beneficial for MSC expansion and chondrogenesis, particularly in suppressing the cartilage hypertrophy. This review will summarise the current literature regarding the effects of physioxia on MSC chondrogenesis with an emphasis on the pathways that control tissue formation and cartilage hypertrophy.

Published

2019

44. Hypoxia-induced suppression of c-Myc by HIF-2α in human pulmonary endothelial cells attenuates TFAM expression.

Author

Zarrabi, Ali J., Kao, Derrick, Nguyen, Dustin T., Loscalzo, Joseph, and Handy, Diane E.

Subjects

*HYPOXIA-inducible factor genetics, *ENDOTHELIAL cells, *TRANSCRIPTION factors, *GENE expression, *TUMOR suppressor genes, *MITOCHONDRIAL DNA analysis, *PHYSIOLOGY

Abstract

The adaptive response to hypoxia is mediated in large part by stabilization of the hypoxia-inducible factors, HIF-1α and HIF-2α. A hallmark of this response is the metabolic shift to decreased oxidative phosphorylation and increased glycolysis. We hypothesized that hypoxic responses would include a suppression of mitochondrial gene expression. We determined the effects of hypoxia on TFAM, a key mitochondrial transcription factor, in normal pulmonary artery endothelial cells. Hypoxia decreased gene expression of TFAM and that of its upstream regulator, the transcriptional co-activator PGC1β . Although HIF-1α and HIF-2α pathways both contributed to hypoxia-mediated PGC1β suppression, TFAM suppression was regulated solely by HIF-2α-dependent mechanisms. We found that HIF-2α suppresses TFAM by decreasing c-Myc expression. In addition, we show a role for c-Jun in this pathway, linking HIF-2α with attenuation of c-Jun activation. Taken together, these findings establish a new link between HIF-2α and MAPK-signaling that mediates the adaptive regulation of mitochondrial gene expression under low oxygen tension. [ABSTRACT FROM AUTHOR]

Published

2017

45. HIF signalling: The eyes have it.

Author

Peet, D.J., Kittipassorn, T., Wood, J.P., Chidlow, G., and Casson, R.J.

Subjects

*HYPOXIA-inducible factors, *CELLULAR signal transduction, *GENE expression, *EYE development, *EYE physiology

Abstract

The hypoxia inducible factors (HIFs) promote changes in gene expression in response to hypoxia, and mediate key physiological responses such as angiogenesis. They play important roles in development and normal physiology, as well as in ischaemic and other pathologies. The human eye is a complex organ, with tight regulation of vascularisation and oxygen delivery, with the highly specialised retina containing both highly vascularised and avascular regions. This review, written to honour the significant contribution of Lorenz Poellinger to this field, covers the role of the HIFs in normal development of the eye, specifically the vasculature, as well as their roles in numerous retinal pathologies, including ischaemic retinopathies, and age-related macular degeneration (AMD). The characterisation of the HIFs in the eye has improved our understanding of the development, function, and numerous pathologies of the eye, and should inform future therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2017

46. Hypoxia Inducible Factor-2Alpha and Prolinhydroxylase 2 Polymorphisms in Patients with Acute Respiratory Distress Syndrome (ARDS).

Author

Dötsch, Annika, Eisele, Lewin, Rabeling, Miriam, Rump, Katharina, Walstein, Kai, Bick, Alexandra, Cox, Linda, Engler, Andrea, Bachmann, Hagen S., Jöckel, Karl-Heinz, Adamzik, Michael, Peters, Jürgen, and Schäfer, Simon T.

Subjects

*ADULT respiratory distress syndrome treatment, *ADULT respiratory distress syndrome, *HYPOXEMIA, *GENETIC polymorphisms, *HUMAN genetic variation, *PATIENTS

Abstract

Hypoxia-inducible-factor-2α (HIF-2α) and HIF-2 degrading prolyl-hydroxylases (PHD) are key regulators of adaptive hypoxic responses i.e., in acute respiratory distress syndrome (ARDS). Specifically, functionally active genetic variants of HIF-2α (single nucleotide polymorphism (SNP) [ch2:46441523(hg18)]) and PHD2 (C/T; SNP rs516651 and T/C; SNP rs480902) are associated with improved adaptation to hypoxia i.e., in high-altitude residents. However, little is known about these SNPs' prevalence in Caucasians and impact on ARDS-outcome. Thus, we tested the hypotheses that in Caucasian ARDS patients SNPs in HIF-2α or PHD2 genes are (1) common, and (2) independent risk factors for 30-day mortality. After ethics-committee approval, 272 ARDS patients were prospectively included, genotyped for PHD2 (Taqman SNP Genotyping Assay) and HIF-2α-polymorphism (restriction digest + agarose-gel visualization), and genotype dependent 30-day mortality was analyzed using Kaplan-Meier-plots and multivariate Cox-regression analyses. Frequencies were 99.62% for homozygous HIF-2a CC-carriers (CG: 0.38%; GG: 0%), 2.3% for homozygous PHD2 SNP rs516651 TT-carriers (CT: 18.9%; CC: 78.8%), and 3.7% for homozygous PHD2 SNP rs480902 TT-carriers (CT: 43.9%; CC: 52.4%). PHD2 rs516651 TT-genotype in ARDS was independently associated with a 3.34 times greater mortality risk (OR 3.34, CI 1.09-10.22; p = 0.034) within 30-days, whereas the other SNPs had no significant impact (p = ns). The homozygous HIF-2α GG-genotype was not present in our Caucasian ARDS cohort; however PHD2 SNPs exist in Caucasians, and PHD2 rs516651 TT-genotype was associated with an increased 30-day mortality suggesting a relevance for adaptive responses in ARDS. [ABSTRACT FROM AUTHOR]

Published

2017

47. Role of hypoxia-inducible factors (HIF) in the maintenance of stemness and malignancy of colorectal cancer.

Author

Vadde, Ramakrishna, Vemula, Sarojamma, Jinka, Rajeswari, Merchant, Neha, Bramhachari, Pallaval Veera, and Nagaraju, Ganji Purnachandra

Subjects

*HYPOXIA-inducible factors, *COLON cancer, *OXYGENATION (Chemistry), *NEOPLASTIC cell transformation, *CANCER stem cells

Abstract

Hypoxia is a condition of insufficient tissue oxygenation, which is observed during normal development as well as tumorigenesis and its response at the cellular level is primarily mediated through hypoxia inducible factors (HIFs). HIFs have a significant role in the maintenance of stemness in both stem cells as well as in cancer stem cells (CSC) by acting as transcription factors. The CSCs are proposed to be the driving force of colon tumorigenesis and malignancy. These HIFs play a significant role in a wide range of diseases including colon cancer. HIF’s signaling functions with stemness, and maintaining Wnt/β-catenin signaling pathways. Due to HIFs functional significance in stemness maintenance in malignancy, targeting HIFs might provide a new approach for development of new therapy for colon cancer. In this review, we will be briefing on the colon and its stem cells, various molecular signaling pathways involved in stemness preservation, and the role hypoxia and its HIFs in the maintenance of stemness in colon stem cells and colon cancer stem cells. [ABSTRACT FROM AUTHOR]

Published

2017

48. Mitochondrial Reactive Oxygen Species and Kidney Hypoxia in the Development of Diabetic Nephropathy.

Author

SCHIFFER, TOMAS A. and FRIEDERICH-PERSSON, MALOU

Subjects

DIABETIC nephropathies, REACTIVE oxygen species, HYPOXEMIA, PROTEIN kinases, MITOCHONDRIAL pathology

Abstract

The underlying mechanisms in the development of diabetic nephropathy are currently unclear and likely consist of a series of dynamic events from the early to late stages of the disease. Diabetic nephropathy is currently without curative treatments and it is acknowledged that even the earliest clinical manifestation of nephropathy is preceded by an established morphological renal injury that is in turn preceded by functional and metabolic alterations. An early manifestation of the diabetic kidney is the development of kidney hypoxia that has been acknowledged as a common pathway to nephropathy. There have been reports of altered mitochondrial function in the diabetic kidney such as altered mitophagy, mitochondrial dynamics, uncoupling, and cellular signaling through hypoxia inducible factors and AMP-kinase. These factors are also likely to be intertwined in a complex manner. In this review, we discuss how these pathways are connected to mitochondrial production of reactive oxygen species (ROS) and how they may relate to the development of kidney hypoxia in diabetic nephropathy. From available literature, it is evident that early correction and/or prevention of mitochondrial dysfunction may be pivotal in the prevention and treatment of diabetic nephropathy. [ABSTRACT FROM AUTHOR]

Published

2017

49. Sauerstoffabhängige Regulation des Wilms-Tumor Gens WT1 in Neuroblastomzellen

Author

Catanese, Lorenzo

Subjects

neuroblastoma, hypoxia inducible factors, hypoxia, HIF, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit::610 Medizin und Gesundheit, WT1

Abstract

Sauerstoffmangel (Hypoxie) f��rdert ein aggressives Wachstum von Tumoren. Dies gilt insbesondere f��r das Neuroblastom, den h��ufigsten extrakraniellen soliden Tumor des Kindesalters. Neuroblastome sind Malignome des peripheren sympathischen Nervensystems, deren Tumorzellen von der embryonalen Neuralleiste abstammen. In Neuroblastomen korreliert die Akkumulation von Hypoxie-induzierbarem-Faktor-2�� (HIF-2��) mit einem hochmalignen Tumorph��notyp und einem ung��nstigen klinischen Verlauf. Hypoxie-induzierbare-Faktoren (HIF) bilden eine Familie von heterodimeren Transkriptionsfaktoren, die bei der zellul��ren Adaptation an ein niedriges Sauerstoffniveau in normalem Gewebe und in Tumoren eine zentrale Rolle spielen. Neben der Anreicherung von HIF-2�� ist auch eine hohe Expression von Wilms-Tumor-Gen 1 (WT1) mit einer schlechten Prognose von Neuroblastomen assoziiert. WT1 kodiert einen Transkriptionsfaktor, der urspr��nglich als Suppressor f��r das Wachstum von Nierentumoren bei Kindern (Wilms-Tumor, Nephroblastom) charakterisiert wurde. Neuere Untersuchungen haben ergeben, dass WT1 in vielen malignen Tumoren verst��rkt exprimiert wird und dort m��glicherweise onkogene Eigenschaften besitzt. Vor diesem Hintergrund sollte in der vorliegenden Arbeit ��berpr��ft werden, ob die Expression von WT1 in Neuroblastomzellen sauerstoffabh��ngig reguliert wird. Weiterhin sollte gegebenenfalls der molekulare Mechanismus analysiert werden, ��ber den ein Sauerstoffmangel die WT1-Expression stimuliert. Im Rahmen der durchgef��hrten Untersuchungen konnte gezeigt werden, dass die Expression von WT1 in Kelly-Neuroblastomzellen tats��chlich durch Hypoxie stimuliert wird. Der Knockdown von HIF-2�� mittels RNA-Interferenz bzw. Deletion von HIF-2�� mittels CRISPR/Cas9 bewirkte eine signifikante Abnahme der WT1 Expression in hypoxischen Kelly-Zellen. Die Inaktivierung von HIF-1�� hatte hingegen keinen signifikanten Einfluss auf das WT1 Niveau. Weiterhin wurde in silico ein HIF-Bindungsmotiv innerhalb eines DNase-sensitiven Bereichs in Intron 3 des WT1 Gens identifiziert. Mittels Chromatin-Immunpr��zipitation (ChIP) und Elektromobilit��tsshiftassays konnte eine Bindung von HIF-2 an diese Sequenz experimentell nachgewiesen werden. In Reportergenassays, die an transient transfizierten Kelly-Zellen durchgef��hrt wurden, ��bertrug ein 256 bp langes DNA-Fragment unter Einschluss des HIF-Bindungsmotivs aus Intron 3 des WT1-Gens eine Hypoxieempfindlichkeit auf die ansonsten hypoxieresistenten SV40- und WT1-Promotoren. Funktionell konnte nachgewiesen werden, dass WT1 die Migration von SK-NA-S-Neuroblastomzellen stimuliert. R2-Datenanalysen von gro��en Kohorten von Neuroblastompatienten zeigten, dass sowohl HIF-2�� als auch WT1 in Subgruppen von Neuroblastompatienten mit einer erh��hten Mortalit��t assoziiert sind. Mit diesen Ergebnissen wird erstmalig ein sauerstoffempfindlicher Enhancer in Intron 3 des WT1 Gens identifiziert. Unter hypoxischen Bedingungen bewirkt die Bindung von HIF-2 an das Enhancerelement eine WT1-Expression in Kelly-Neuroblastomzellen. Dieser neu entdeckte molekulare Mechanismus spielt m��glicherweise in der Pathophysiologie von Neuroblastomen eine Rolle., Oxygen shortage (hypoxia) favors aggressive tumor growth. This is particularly relevant to neuroblastoma, the most common extracranial solid tumor in childhood. Neuroblastoma arises from neural crest-derived cells in the peripheral sympathetic nervous system. High levels of hypoxia-inducible factor (HIF) 2�� in neuroblastoma correlate with an undifferentiated tumor phenotype and poor clinical outcome. Hypoxiainducible factors constitute a family of heterodimeric transcription factors that play a pivotal role in the adaptation of normal and tumor tissues to low oxygen conditions. Recent studies have shown that high expression levels of the Wilms tumor gene 1 (WT1) in neuroblastoma are associated with an aggressive tumor growth and poor prognosis. WT1 was initially identified as a tumor suppressor gene preventing the formation of childhood tumors of the kidney (Wilms tumor, nephroblastoma). However, WT1 is highly expressed in various types of cancer suggesting that it may have oncogenic properties in certain tissues. It was the purpose of this study to test whether WT1 expression in neuroblastoma cells is regulated by oxygen and, if so, to analyze the underlying molecular mechanism. Exposure of Kelly neuroblastoma cells to low ambient oxygen did indeed stimulate expression of the WT1 gene. Silencing of HIF-2�� by RNA interference and knockout of HIF-2�� using CRISPR/Cas9 genome editing significantly reduced WT1 levels in hypoxic Kelly cells. In contrast, inactivation of HIF-1�� had no significant effect on WT1 expression in hypoxic Kelly cells. In silico analyses revealed a HIF binding motif within a cluster of DNase hypersensitivity in intron 3 of the WT1 gene. Binding of HIF-2 to this sequence was experimentally proven by chromatin immunoprecipitation (ChIP) and electromobility shift assay. A 256 bp DNA sequence encompassing the identified HIF binding site conferred oxygen sensitivity to otherwise hypoxia resistant WT1 and SV40 promoter constructs in transiently transfected Kelly cells. In functional assays, WT1 was found to enhance the migratory capacity of SK-NA-S neuroblastoma cells. R2 data analysis of cohorts of neuroblastoma patients showed that HIF-2�� and WT1 are independently associated with increased mortality. In summary, these results identify an oxygen sensitive enhancer in intron 3 of the WT1 gene. Binding of HIF-2 to this newly discovered enhancer element stimulates WT1 expression in hypoxic Kelly neuroblastoma cells. It is suggested that this novel regulatory mechanism might play a role in the pathophysiology of neuroblastoma.

Published

2022

50. Metabolic Regulation of Hypoxia-Inducible Transcription Factors: The Role of Small Molecule Metabolites and Iron

Author

Peter S. J. Bailey and James A. Nathan

Subjects

hypoxia inducible factors, HIF, prolyl hydroxylase, PHD, 2-OG dependent dioxygenase, 2-hydroxyglutarate, 2-HG, iron metabolism, TCA cycle, Biology (General), QH301-705.5

Abstract

Hypoxia-inducible transcription factors (HIFs) facilitate cellular adaptations to low-oxygen environments. However, it is increasingly recognised that HIFs may be activated in response to metabolic stimuli, even when oxygen is present. Understanding the mechanisms for the crosstalk that exists between HIF signalling and metabolic pathways is therefore important. This review focuses on the metabolic regulation of HIFs by small molecule metabolites and iron, highlighting the latest studies that explore how tricarboxylic acid (TCA) cycle intermediates, 2-hydroxyglutarate (2-HG) and intracellular iron levels influence the HIF response through modulating the activity of prolyl hydroxylases (PHDs). We also discuss the relevance of these metabolic pathways in physiological and disease contexts. Lastly, as PHDs are members of a large family of 2-oxoglutarate (2-OG) dependent dioxygenases that can all respond to metabolic stimuli, we explore the broader role of TCA cycle metabolites and 2-HG in the regulation of 2-OG dependent dioxygenases, focusing on the enzymes involved in chromatin remodelling.

Published

2018