Your search keyword '"Hassan, Moustapha"' showing total 77 results

1. Wharton's Jelly mesenchymal stem cell‐derived extracellular vesicles induce liver fibrosis‐resolving phenotype in alternatively activated macrophages.

Author

Torabi, Shukoofeh, Zarrabi, Morteza, Shekari, Faezeh, Poorkazem, Hedie, Lotfinia, Majid, Bencina, Stefan, Gramignoli, Roberto, Hassan, Moustapha, Najimi, Mustapha, and Vosough, Massoud

Subjects

CORD blood, HEPATIC fibrosis, MESENCHYMAL stem cells, EXTRACELLULAR vesicles, STROMAL cells

Abstract

The potential of extracellular vesicles (EVs) isolated from mesenchymal stromal cells in guiding macrophages toward anti‐inflammatory immunophenotypes, has been reported in several studies. In our study, we provided experimental evidence of a distinctive effect played by Wharton Jelly mesenchymal stromal cell‐derived EVs (WJ‐EVs) on human macrophages. We particularly analyzed their anti‐inflammatory effects on macrophages by evaluating their interactions with stellate cells, and their protective role in liver fibrosis. A three‐step gradient method was used to isolate monocytes from umbilical cord blood (UCB). Two subpopulations of WJ‐EVs were isolated by high‐speed (20,000 g) and differential ultracentrifugation (110,000 g). Further to their characterization, they were designated as EV20K and EV110K and incubated at different concentrations with UCB‐derived monocytes for 7 days. Their anti‐fibrotic effect was assessed by studying the differentiation and functional levels of generated macrophages and their potential to modulate the survival and activity of LX2 stellate cells. The EV20K triggers the polarization of UCB‐derived monocytes towards a peculiar M2‐like functional phenotype more effectively than the M‐CSF positive control. The EV20K treated macrophages were characterized by a higher expression of scavenger receptors, increased phagocytic capacity and production level of interleukin‐10 and transforming growth factor‐β. Conditioned medium from those polarized macrophages attenuated the proliferation, contractility and activation of LX2 stellate cells. Our data show that EV20K derived from WJ‐MSCs induces activated macrophages to suppress immune responses and potentially play a protective role in the pathogenesis of liver fibrosis by directly inhibiting HSC's activation. [ABSTRACT FROM AUTHOR]

Published

2024

2. P53/NANOG balance; the leading switch between poorly to well differentiated status in liver cancer cells.

Author

Ranjbar-Niavol, Fazeleh, Rezaei, Niloufar, Ying Zhao, Mirzaei, Hamed, Hassan, Moustapha, and Vosough, Massoud

Subjects

LIVER cells, LIVER cancer, CANCER cells, HEPATOCELLULAR carcinoma, DRUG target

Abstract

Enforcing a well-differentiated state on cells requires tumor suppressor p53 activation as a key player in apoptosis induction and well differentiation. In addition, recent investigations showed a significant correlation between poorly differentiated status and higher expression of NANOG. Inducing the expression of NANOG and decreasing p53 level switch the status of liver cancer cells from well differentiated to poorly status. In this review, we highlighted p53 and NANOG cross-talk in hepatocellular carcinoma (HCC) which is regulated through mitophagy and makes it a novel molecular target to attenuate cancerous phenotype in the management of this tumor. [ABSTRACT FROM AUTHOR]

Published

2024

3. Correction: Asadian et al. Rhenium Perrhenate (188 ReO4) Induced Apoptosis and Reduced Cancerous Phenotype in Liver Cancer Cells. Cells 2022, 11 , 305.

Author

Asadian, Samieh, Piryaei, Abbas, Gheibi, Nematollah, Aziz Kalantari, Bagher, Reza Davarpanah, Mohamad, Azad, Mehdi, Kapustina, Valentina, Alikhani, Mehdi, Moghbeli Nejad, Sahar, Keshavarz Alikhani, Hani, Mohamadi, Morteza, Shpichka, Anastasia, Timashev, Peter, Hassan, Moustapha, and Vosough, Massoud

Subjects

CELL survival, CYTOTOXINS, LIVER cells, LIVER cancer, CANCER cells

Abstract

This document is a correction notice for an article titled "Rhenium Perrhenate (188 ReO4) Induced Apoptosis and Reduced Cancerous Phenotype in Liver Cancer Cells." The correction addresses an error in Figure 1A of the original publication, where two images were unintentionally repeated and the control figures overlapped. The corrected figure has been provided, and the authors state that the scientific conclusions remain unaffected. The original publication has been updated accordingly. [Extracted from the article]

Published

2024

4. Chitosan‐coated nanoparticles in innovative cancer bio‐medicine.

Author

Rezaei, Niloufar, Zarkesh, Ibrahim, Fotouhi, Alireza, Alikhani, Hani Keshavarz, Hassan, Moustapha, and Vosough, Massoud

Subjects

CHITOSAN, NANOPARTICLES, CYTOTOXINS, PRODUCTION methods, ANTIBACTERIAL agents, BIODEGRADABLE plastics

Abstract

In the recent decade, nanoparticles (NPs) have had enormous implications in cancer biomedicine, including research, diagnosis, and therapy. However, their broad application still faces obstacles due to some practical limitations and requires further development. Recently, there has been more interest in the coated class of nanoparticles to address those challenges. Chitosan‐coated NPs are simple to produce, biodegradable, biocompatible, exhibit antibacterial activity, and have less cytotoxicity. This study provides an updated and comprehensive overview of the application of chitosan‐coated NPs as a promising class of NPs in cancer biomedicine. Additionally, we discussed chitosan‐coated lipid, metal, and polymer‐based nanoparticles in biomedical applications. Furthermore, different coating methods and production/characterization procedures were reviewed. Moreover, the biological and physicochemical advantages of chitosan‐coated NPs, including facilitated controlled release, greater physicochemical stability, improved cell/tissue interaction, and enhanced bioavailability of medications, were highlighted. Finally, the prospects of chitosan‐coated NPs in cancer biomedicine were discussed. [ABSTRACT FROM AUTHOR]

Published

2024

5. Bioengineering vascularized liver tissue for biomedical research and application.

Author

Davoodi, Parsa, Rezaei, Niloofar, Hassan, Moustapha, Hay, David C., and Vosough, Massoud

Subjects

BIOENGINEERING, MEDICAL research, LIVER, TISSUES, LIVER transplantation

Abstract

The liver performs a wide range of biological functions that are essential to body homeostasis. Damage to liver tissue can result in reduced organ function, and if chronic in nature can lead to organ scarring and progressive disease. Currently, donor liver transplantation is the only longterm treatment for end-stage liver disease. However, orthotopic organ transplantation suffers from several drawbacks that include organ scarcity and lifelong immunosuppression. Therefore, new therapeutic strategies are required. One promising strategy is the engineering of implantable and vascularized liver tissue. This resource could also be used to build the next generation of liver tissue models to better understand human health, disease and aging in vitro. This article reviews recent progress in the field of liver tissue bioengineering, including microfluidic-based systems, bio-printed vascularized tissue, liver spheroids and organoid models, and the induction of angiogenesis in vivo. [ABSTRACT FROM AUTHOR]

Published

2024

6. Circulating Tumor Cells as a Promising Tool for Early Detection of Hepatocellular Carcinoma.

Author

Salehi, Mahsa, Lavasani, Zohre Miri, Keshavarz Alikhani, Hani, Shokouhian, Bahare, Hassan, Moustapha, Najimi, Mustapha, and Vosough, Massoud

Subjects

HEPATOCELLULAR carcinoma, LIVER cancer, DELAYED diagnosis, DEATH rate, EARLY diagnosis

Abstract

Liver cancer is a significant contributor to the cancer burden, and its incidence rates have recently increased in almost all countries. Hepatocellular carcinoma (HCC) is the most common type of primary liver cancer and is the second leading cause of cancer-related deaths worldwide. Because of the late diagnosis and lack of efficient therapeutic modality for advanced stages of HCC, the death rate continues to increase by ~2–3% per year. Circulating tumor cells (CTCs) are promising tools for early diagnosis, precise prognosis, and follow-up of therapeutic responses. They can be considered to be an innovative biomarker for the early detection of tumors and targeted molecular therapy. In this review, we briefly discuss the novel materials and technologies applied for the practical isolation and detection of CTCs in HCC. Also, the clinical value of CTC detection in HCC is highlighted. [ABSTRACT FROM AUTHOR]

Published

2023

7. Progress and promise of cell sheet assisted cardiac tissue engineering in regenerative medicine.

Author

Abdolahzadeh, Hadis, Rad, Niloofar Khoshdel, Shpichka, Anastasia, Golroo, Reihaneh, Rahi, Kosar, Timashev, Peter, Hassan, Moustapha, and Vosough, Massoud

Published

2023

8. Cell and cell-derivative-based therapy for liver diseases: current approaches and future promises.

Author

Zahmatkesh, Ensieh, Khoshdel Rad, Niloofar, Hossein-Khannazer, Nikoo, Mohamadnejad, Mehdi, Gramignoli, Roberto, Najimi, Mustapha, Malekzadeh, Reza, Hassan, Moustapha, and Vosough, Massoud

Subjects

LIVER diseases, CELLULAR therapy, HUMAN stem cells, BIOPOLYMERS, EXTRACELLULAR matrix

Abstract

According to the recent updates from World Health Organization, liver diseases are the 12th most common cause of mortality. Currently, orthotopic liver transplantation (OLT) is the most effective and the only treatment for end-stage liver diseases. Owing to several shortcomings like finite numbers of healthy organ donors, lifelong immunosuppression, and complexity of the procedure, cell and cell-derivatives therapies have emerged as a potential therapeutic alternative for liver diseases. Various cell types and therapies have been proposed and their therapeutic effects evaluated in preclinical or clinical studies, including hepatocytes, hepatocyte-like cells (HLCs) derived from stem cells, human liver stem cells (HLSCs), combination therapies with various types of cells, organoids, and implantable cell-biomaterial constructs with synthetic and natural polymers or even decellularized extracellular matrix (ECM). In this review, we highlighted the current status of cell and cell-derivative-based therapies for liver diseases. Furthermore, we discussed future prospects of using HLCs, liver organoids, and their combination therapies. Promising application of stem cell-based techniques including iPSC technology has been integrated into novel techniques such as gene editing, directed differentiation, and organoid technology. iPSCs offer promising prospects to represent novel therapeutic strategies and modeling liver diseases. [ABSTRACT FROM AUTHOR]

Published

2023

9. Novel antigens for targeted radioimmunotherapy in hepatocellular carcinoma.

Author

Pourhamzeh, Mahsa, Asadian, Samieh, Mirzaei, Hamed, Minaei, Azita, Shahriari, Elahe, Shpichka, Anastasia, Es, Hamidreza Aboulkheyr, Timashev, Peter, Hassan, Moustapha, and Vosough, Massoud

Abstract

Liver cancer is the sixth common cancer and forth cause of cancer-related death worldwide. Based on usually advanced stages of hepatocellular carcinoma (HCC) at the time of diagnosis, therapeutic options are limited and, in many cases, not effective, and typically result in the tumor recurrence with a poor prognosis. Radioimmunotherapy (RIT) offers a selective internal radiation therapy approach using beta or alpha emitting radionuclides conjugated with tumor-specific monoclonal antibodies (mAbs), or specific selective peptides. When compared to chemotherapy or radiotherapy, radiolabeled mAbs against cancer-associated antigens could provide a high therapeutic and exclusive radiation dose for cancerous cells while decreasing the exposure-induced side effects to healthy tissues. The recent advances in cancer immunotherapy, such as blockade of immune-checkpoint inhibitors (ICIs), has changed the landscape of cancer therapy, and the efficacy of different classes of immunotherapy has been tested in many clinical trials. Taking into account the use of ICIs in the liver tumor microenvironment, combined therapies with different approaches may enhance the outcome in the future clinical studies. With the development of novel immunotherapy treatment options in the recent years, there has been a great deal of information about combining the diverse treatment modalities to boost the effectiveness of immunomodulatory drugs. In this opinion review, we will discuss the recent advancements in RIT. The current status of immunotherapy and internal radiotherapy will be updated, and we will propose novel approaches for the combination of both techniques. Potential target antigens for radioimmunotherapy in Hepatocellular carcinoma (HCC). HCC radioimmunotherapy target antigens are the most specific and commonly accessible antigens on the surface of HCC cells. CTLA-4 ligand and receptor, TAMs, PD-1/PD-L, TIM-3, specific IEXs/TEXs, ROBO1, and cluster of differentiation antigens CD105, CD147 could all be used in HCC radioimmunotherapy. Abbreviations: TAMs, tumor-associated macrophages; CTLA-4, cytotoxic T-lymphocyte associated antigen-4; PD-1, Programmed cell death protein 1; PD-L, programmed death-ligand1; TIM-3, T-cell immunoglobulin (Ig) and mucin-domain containing protein-3; IEXs, immune cell-derived exosomes; TEXs, tumor-derived exosomes. [ABSTRACT FROM AUTHOR]

Published

2023

10. Hepatogenesis and hepatocarcinogenesis: Alignment of the main signaling pathways.

Author

Shokouhian, Bahare, Aboulkheyr Es, Hamidreza, Negahdari, Babak, Tamimi, Atena, Shahdoust, Maryam, Shpichka, Anastasia, Timashev, Peter, Hassan, Moustapha, and Vosough, Massoud

Subjects

CELLULAR signal transduction, GENE expression profiling, CELL differentiation, CANCER cells, HEPATOCELLULAR carcinoma

Abstract

Development is a symphony of cells differentiation in which different signaling pathways are orchestrated at specific times and periods to form mature and functional cells from undifferentiated cells. The similarity of the gene expression profile in malignant and undifferentiated cells is an interesting topic that has been proposed for many years and gave rise to the differentiation‐therapy concept, which appears a rational insight and should be reconsidered. Hepatocellular carcinoma (HCC), as the sixth common cancer and the third leading cause of cancer death worldwide, is one of the health‐threatening complications in communities where hepatotropic viruses are endemic. Sedentary lifestyle and high intake of calories are other risk factors. HCC is a complex condition in which various dimensions must be addressed, including heterogeneity of cells in the tumor mass, high invasiveness, and underlying diseases that limit the treatment options. Under these restrictions, recognizing, and targeting common signaling pathways during liver development and HCC could expedite to a rational therapeutic approach, reprograming malignant cells to well‐differentiated ones in a functional state. Accordingly, in this review, we highlighted the commonalities of signaling pathways in hepatogenesis and hepatocarcinogenesis, and comprised an update on the current status of targeting these pathways in laboratory studies and clinical trials. [ABSTRACT FROM AUTHOR]

Published

2022

11. Cardiovascular Complications in Hematopoietic Stem Cell Transplanted Patients.

Author

Zhao, Ying, He, Rui, Oerther, Sandra, Zhou, Weiying, Vosough, Massoud, and Hassan, Moustapha

Abstract

Hematopoietic stem cell transplantation (HSCT) is the only curative treatment for many patients suffering from hematologic malignancies, solid tumors, inborn errors of metabolism or genetic disorders. Despite decades of successful HSCT, clinical outcomes are still far from satisfactory due to treatment-related complications, including graft-versus-host disease (GvHD) and cardiovascular complications (CVC). CVC may affect patients in the acute period post-HSCT; however, the occurrence is far higher among long-term survivors. Induction treatment using cardiotoxic treatments, e.g., anthracyclines and radiotherapy, conditioning regimens containing cyclophosphamide, and post-HSCT comorbidities, including GvHD, are factors contributing to CVC. Cardiac function evaluation prior to and post-transplantation is an important strategy for choosing the proper conditioning regimen, HSCT protocol and post-HSCT supportive care. Cardiac systolic function evaluation by echocardiography, in addition to serum cardiac biomarkers, such as troponins and brain natriuretic peptides, is recommended as a routine follow-up for HSCT patients. Angiotensin-converting enzyme inhibitors, angiotensin-II-receptor blockers, and beta-blockers, which are mostly used for the treatment of chemotherapy-induced cardiotoxicity, might be used as treatments for HSCT-related CVC. In summary, the present review reveals the urgent need for further investigations concerning HSCT-related CVC both at the preclinical and clinical levels due to the lack of knowledge about CVC and its underlying mechanisms. [ABSTRACT FROM AUTHOR]

Published

2022

12. Conjugated Linoleic Acid Treatment Attenuates Cancerous features in Hepatocellular Carcinoma Cells.

Author

Miri-Lavasani, Zohre, Torabi, Shukoofeh, Solhi, Roya, Shokouhian, Bahareh, Afsharian, Parvaneh, Heydari, Zahra, Piryaei, Abbas, Farzaneh, Zahra, Hossein-khannazer, Nikoo, Es, Hamidreza Aboulkheyr, Zahmatkesh, Ensieh, Nussler, Andreas, Hassan, Moustapha, Najimi, Mustapha, and Vosough, Massoud

Subjects

CONJUGATED linoleic acid, HEPATOCYTE nuclear factors, HEPATOCELLULAR carcinoma, LINOLEIC acid, EPITHELIAL-mesenchymal transition, CELL differentiation

Abstract

Background. A growing number of hepatocellular carcinoma (HCC), and recurrence frequency recently have drawn researchers' attention to alternative approaches. The concept of differentiation therapies (DT) relies on inducing differentiation in HCC cells in order to inhibit recurrence and metastasis. Hepatocyte nuclear factor 4 alpha (HNF4α) is the key hepatogenesis transcription factor and its upregulation may decrease the invasiveness of cancerous cells by suppressing epithelial-mesenchymal transition (EMT). This study aimed to evaluate the effect of conjugated linoleic acid (CLA) treatment, natural ligand of HNF4α, on the proliferation, migration, and invasion capacities of HCC cells in vitro. Materials and Method. Sk-Hep-1 and Hep-3B cells were treated with different doses of CLA or BIM5078 [1-(2 ′ -chloro-5 ′ -nitrobenzenesulfonyl)−2-methylbenzimidazole], an HNF4α antagonist. The expression levels of HNF4a and EMT related genes were evaluated and associated to hepatocytic functionalities, migration, and colony formation capacities, as well as to viability and proliferation rate of HCC cells. Results. In both HCC lines, CLA treatment induced HNF4α expression in parallel to significantly decreased EMT marker levels, migration, colony formation capacity, and proliferation rate, whereas BIM5078 treatment resulted in the opposite effects. Moreover, CLA supplementation also upregulated ALB, ZO1, and HNF4α proteins as well as glycogen storage capacity in the treated HCC cells. Conclusion. CLA treatment can induce a remarkable hepatocytic differentiation in HCC cells and attenuates cancerous features. This could be as a result of HNF4a induction and EMT inhibition. [ABSTRACT FROM AUTHOR]

Published

2022

13. Mini review ATF4 and GRP78 as novel molecular targets in ER-Stress modulation for critical COVID-19 patients.

Author

Shahriari-Felordi, Mahtab, Alikhani, Hani Keshavarz, Hashemian, Seyed-Mohammad Reza, Hassan, Moustapha, and Vosough, Massoud

Abstract

Coronavirus disease 2019 (COVID-19) is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and has resulted in more than 4.4 million deaths worldwide as of August 24, 2021. Viral infections such as SARS-CoV2 are associated with endoplasmic reticulum (ER) stress and also increased the level of reactive oxygen species. Activating transcription factor 4 (ATF4) is preferentially translated under integrated stress conditions and controls the genes involved in protein homeostasis, amino acid transport and metabolism, and also protection from oxidative stress. The GRP78, regulated either directly or indirectly by ATF4, is an essential chaperone in the ER and overexpressed and appears on the surface of almost all cells during stress and function as a SARS-CoV2 receptor. In this mini-review article, we briefly discuss the effects of SARS-CoV2 infection on the ER stress, and then the stress modulator functions of ATF4 and GRP78 as novel therapeutic targets were highlighted. Finally, the effects of GRP78 inhibitory components as potential factors for targeted therapies for COVID-19 critical cases were discussed. [ABSTRACT FROM AUTHOR]

Published

2022

14. Endoplasmic reticulum stress inhibits AR expression via the PERK/eIF2α/ATF4 pathway in luminal androgen receptor triple-negative breast cancer and prostate cancer.

Author

Li, Xiaoli, Zhou, Duanfang, Cai, Yongqing, Yu, Xiaoping, Zheng, Xiangru, Chen, Bo, Li, Wenjun, Zeng, Hongfang, Hassan, Moustapha, Zhao, Ying, and Zhou, Weiying

Published

2022

15. NON-DESTRUCTIVE TESTING OF NANO-SILICA FOR ENHANCING THE DURABILITY OF LIMESTONE STRUCTURES IN THE VALLEY OF THE KINGS, LUXOR, EGYPT.

Author

Sallam, Ahmed, Khalil, Mona M. E., Hemeda, Sayed, and Hassan, Moustapha

Subjects

LIMESTONE, FLOODS

Abstract

Copyright of Conservation Science in Cultural Heritage / Quaderni di Scienza della Conservazione is the property of Salvatore Lorusso and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

16. Application of Stem Cell-Derived Extracellular Vesicles as an Innovative Theranostics in Microbial Diseases.

Author

Keshavarz Alikhani, Hani, Shokoohian, Bahare, Rezasoltani, Sama, Hossein-khannazer, Nikoo, Yadegar, Abbas, Hassan, Moustapha, and Vosough, Massoud

Subjects

EXTRACELLULAR vesicles, HIV, HEPATITIS C virus, HEPATITIS B virus, COMPANION diagnostics, PATHOGENIC microorganisms, THERAPEUTICS

Abstract

Extracellular vesicles (EVs), as nano-/micro-scale vehicles, are membranous particles containing various cargoes including peptides, proteins, different types of RNAs and other nucleic acids, and lipids. These vesicles are produced by all cell types, in which stem cells are a potent source for them. Stem cell-derived EVs could be promising platforms for treatment of infectious diseases and early diagnosis. Infectious diseases are responsible for more than 11 million deaths annually. Highly transmissible nature of some microbes, such as newly emerged severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), drives researcher's interest to set up different strategies to develop novel therapeutic strategies. Recently, EVs-based diagnostic and therapeutic approaches have been launched and gaining momentum very fast. The efficiency of stem cell-derived EVs on treatment of clinical complications of different viruses and bacteria, such as SARS-CoV-2, hepatitis B virus (HBV), hepatitis C virus (HCV), human immunodeficiency virus (HIV), Staphylococcus aureus , Escherichia coli has been demonstrated. On the other hand, microbial pathogens are able to incorporate their components into their EVs. The microbe-derived EVs have different physiological and pathological impacts on the other organisms. In this review, we briefly discussed biogenesis and the fate of EVs. Then, EV-based therapy was described and recent developments in understanding the potential application of stem cell-derived EVs on pathogenic microorganisms were recapitulated. Furthermore, the mechanisms by which EVs were exploited to fight against infectious diseases were highlighted. Finally, the deriver challenges in translation of stem cell-derived EVs into the clinical arena were explored. [ABSTRACT FROM AUTHOR]

Published

2021

17. Advanced therapeutic modalities in hepatocellular carcinoma: Novel insights.

Author

Shokoohian, Bahare, Negahdari, Babak, Aboulkheyr Es, Hamidreza, Abedi‐Valugerdi, Manuchehr, Baghaei, Kaveh, Agarwal, Tarun, Maiti, Tapas Kumar, Hassan, Moustapha, Najimi, Mustapha, and Vosough, Massoud

Subjects

HEPATOCELLULAR carcinoma, THERAPEUTICS, LIVER cancer, GENE therapy, DIAGNOSIS, AFLATOXINS

Abstract

Hepatocellular carcinoma (HCC), the most common type of liver cancer, is usually a latent and asymptomatic malignancy caused by different aetiologies, which is a result of various aberrant molecular heterogeneity and often diagnosed at advanced stages. The incidence and prevalence have significantly increased because of sedentary lifestyle, diabetes, chronic infection with hepatotropic viruses and exposure to aflatoxins. Due to advanced intra‐ or extrahepatic metastasis, recurrence is very common even after radical resection. In this paper, we highlighted novel therapeutic modalities, such as molecular‐targeted therapies, targeted radionuclide therapies and epigenetic modification‐based therapies. These topics are trending headlines and their combination with cell‐based immunotherapies, and gene therapy has provided promising prospects for the future of HCC treatment. Moreover, a comprehensive overview of current and advanced therapeutic approaches is discussed and the advantages and limitations of each strategy are described. Finally, very recent and approved novel combined therapies and their promising results in HCC treatment have been introduced. [ABSTRACT FROM AUTHOR]

Published

2021

18. COVID-19 and hygiene hypothesis: increment of the inflammatory bowel diseases in next generation?

Author

Shahrbaf, Mohammad Amin, Hassan, Moustapha, and Vosough, Massoud

Subjects

INFLAMMATORY bowel diseases, CORONAVIRUS diseases, HYGIENE, COVID-19, COVID-19 pandemic

Abstract

These diseases result from complex interactions between environmental factors, including cigarette smoking, low physical inactivity, and western diet, genetical predisposition, gut immune system imbalance, and gut microbiota dysbiosis [[14]]. The possible dysbiosis resulting from intensive hygiene measures, which discussed previously for the human microbiome [[23]], during the COVID-19 era can have short-term effects on the immune system, especially gut-lung axis, and long-term effect, which is related to possible dysbiosis and IBD increment in the future. Coronavirus disease 2019 (COVID-19), caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), was first detected in December 2019 in Wuhan, China, and due to the high transmission rate, caused a global pandemic [[1]]. Dysbiosis, as a consequence of immune system imbalance due to hyper hygiene status, may result in hyper-activity of Th-1 and Th-17, lower activity of T-regs, and lower expressions of IL-10 and regenerating islet-derived protein 3-gamma precursor (REG3- ), observed in IBD patients [[19]]. [Extracted from the article]

Published

2022

19. Population Pharmacokinetic, Pharmacogenetic, and Pharmacodynamic Analysis of Cyclophosphamide in Ethiopian Breast Cancer Patients.

Author

Ahmed, Jemal Hussien, Makonnen, Eyasu, Bisaso, Ronald Kuteesa, Mukonzo, Jackson Kijumba, Fotoohi, Alan, Aseffa, Abraham, Howe, Rawleigh, Hassan, Moustapha, and Aklillu, Eleni

Subjects

BREAST cancer, CANCER patients, BODY surface area, AFRICANS, PHARMACOGENOMICS, PARAMETERS (Statistics)

Abstract

Cyclophosphamide (CPA) containing chemotherapy regimen is the standard of care for breast cancer treatment in sub-Saharan Africa. Wide inter-individual variations in pharmacokinetics (PK) of cyclophosphamide (CPA) influence the efficacy and toxicity of CPA containing chemotherapy. Data on the pharmacokinetics (PK) profile of CPA and its covariates among black African patients is lacking. We investigated population pharmacokinetic/pharmacogenetic/pharmacodynamic (PK-PG-PD) of CPA in Ethiopian breast cancer patients. During the first cycle of CPA-based chemotherapy, the population PK parameters for CPA were determined in 267 breast cancer patients. Absolute neutrophil count was recorded at baseline and day 20 post-CPA administration. A population PK and covariate model analysis was performed using non-linear mixed effects modeling. Semi-mechanistic and empiric drug response models were explored to describe the relationship between the area under concentration-time curve (AUC), and neutrophil toxicity. One compartment model better described CPA PK with population clearance and apparent volume of distribution (VD) of 5.41 L/h and 46.5 L, respectively. Inter-patient variability in CPA clearance was 54.5%. Patients carrying CYP3A5*3 or *6 alleles had lower elimination rate constant and longer half-life compared to wild type carriers. CYP2C9 *2 or *3 carriers were associated with increased clearance of CPA. Patients who received 500 mg/m2 based CPA regimen were associated with a 32.3% lower than average clearance and 37.1% lower than average VD compared to patients who received 600 mg/m2. A 0.1 m2 unit increase in body surface area (BSA) was associated with a 5.6% increment in VD. The mean VD (33.5 L) in underweight group (BMI < 18.5 kg/m2) was significantly lower compared to those of overweight (48.1 L) or obese patients (51.9 L) (p < 0.001). AUC of CPA was positively correlated with neutropenic toxicity. In conclusion, we report large between-patient variability in clearance of CPA. CYP3A5 and CYP2C9 genotypes, BSA, BMI, and CPA dosage regimen influence PK of CPA. Plasma CPA exposure positively predicts chemotherapy-associated neutropenic toxicity. [ABSTRACT FROM AUTHOR]

Published

2020

20. A general covalent binding model between cytotoxic selenocompounds and albumin revealed by mass spectrometry and X-ray absorption spectroscopy.

Author

Zheng, Wenyi, He, Rui, Boada, Roberto, Subirana, Maria Angels, Ginman, Tobias, Ottosson, Håkan, Valiente, Manuel, Zhao, Ying, and Hassan, Moustapha

Subjects

ALBUMINS, SELENIUM, CELL-mediated cytotoxicity, SELENOLS, PHARMACOKINETICS

Abstract

Selenocompounds (SeCs) are promising therapeutic agents for a wide range of diseases including cancer. The treatment results are heterogeneous and dependent on both the chemical species and the concentration of SeCs. Moreover, the mechanisms of action are poorly revealed, which most probably is due to the detection methods where the quantification is based on the total selenium as an element. To understand the mechanisms underlying the heterogeneous cytotoxicity of SeCs and to determine their pharmacokinetics, we investigated selenium speciation of six SeCs representing different categories using liquid chromatography-mass spectrometry (LC-MS) and X-ray absorption spectroscopy (XAS) and the cytotoxicity using leukemic cells. SeCs cytotoxicity was correlated with albumin binding degree as revealed by LC-MS and XAS. Further analysis corroborated the covalent binding between selenol intermediates of SeCs and albumin thiols. On basis of the Se-S model, pharmacokinetic properties of four SeCs were for the first time profiled. In summary, we have shown that cytotoxic SeCs could spontaneously transform into selenol intermediates that immediately react with albumin thiols through Se-S bond. The heterogeneous albumin binding degree may predict the variability in cytotoxicity. The present knowledge will also guide further kinetic and mechanistic investigations in both experimental and clinical settings. [ABSTRACT FROM AUTHOR]

Published

2020

21. CYP2J2∗7 Genotype Predicts Risk of Chemotherapy-Induced Hematologic Toxicity and Reduced Relative Dose Intensity in Ethiopian Breast Cancer Patients.

Author

Ahmed, Jemal Hussien, Makonnen, Eyasu, Yimer, Getnet, Seifu, Daniel, Bekele, Abebe, Assefa, Mathewos, Aseffa, Abraham, Howe, Rawleigh, Fotoohi, Alan, Hassan, Moustapha, and Aklillu, Eleni

Subjects

BREAST cancer patients, GENOTYPES, LOGISTIC regression analysis, ODDS ratio

Abstract

Chemotherapy-induced hematologic toxicity is the primary reasons of dose reductions and/or delays, low relative dose intensity (RDI), and predicts anticancer response. We investigated the incidence and predictors of chemotherapy-induced hematologic toxicities and reduced RDI in Ethiopian breast cancer patients, and implication of pharmacogenetics variations. Breast cancer patients (n = 249) were enrolled prospectively to receive cyclophosphamide based chemotherapy. Hematological toxicity (neutropenia, anemia, and thrombocytopenia) were monitored throughout chemotherapy cycle. The primary and secondary outcomes were incidence of grade 3 or 4 toxicity and reduced RDI, respectively. CYP2B6∗6, CYP3A5∗3, CYP2C9 (∗2,∗3), CYP2C19 (∗2,∗3), CYP2J2∗7, POR∗28 , and ABCB1 (rs3842) genotyping were done. Cox proportional hazard and logistic regression were used to estimate risk predictors of toxicity and reduced RDI, respectively. Majority (73.5%) of the patients were < 45 years of age. The incidence of grade 3 or 4 hematological toxicity was 51.0% (95% CI = 44.54–57.46%). Multivariate Cox proportional hazard regression indicated CYP2J2∗7 genotype [Hazard ratio (HR) = 1.82; 95% CI = 1.14–2.90], pretreatment grade 1 leukopenia (HR = 2.75; 95% CI = 1.47–5.15) or grade 1 or 2 neutropenia (HR = 2.75; 95% CI = 1.73–4.35) as significant predictors of hematologic toxicities. The odds of having hematologic toxicities was lower in CYP2C9∗2 or ∗3 carriers (p = 0.024). The prevalence of reduced RDI was 56.6% (95% CI = 50.3–62.9%). Higher risk of reduced RDI was associated with CYP2J2∗7 allele [Adjusted odds ratio (AOR) = 2.79; 95% CI = 1.21–6.46], BMI ≤ 18.4 kg/m2 (AOR = 5.98; 95% CI = 1.36–26.23), baseline grade 1 leukopenia (AOR = 6.09; 95% CI = 1.24–29.98), and baseline neutropenia (AOR = 3.37; 95% CI = 1.41–8.05). The odds of receiving reduced RDI was lower in patients with CYP2B6 ∗6/∗6 genotype (AOR = 0.19; 95% CI = 0.06–0.77). We report high incidence of chemotherapy-induced hematological toxicities causing larger proportion of patients to receive reduced RDI in Ethiopian breast cancer patients. Patients carrying CYP2J2∗7 allele and low baseline blood counts are at a higher risk for chemotherapy-induced hematologic toxicities and receiving reduced RDI, and may require prior support and close follow up during chemotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

22. Downregulation of miR-1266-5P, miR-185-5P and miR-30c-2 in prostatic cancer tissue and cell lines.

Author

Ostadrahimi, Shiva, Fayaz, Shima, Parvizhamidi, Monireh, Abedi-Valugerdi, Manuchehr, Hassan, Moustapha, Kadivar, Mehdi, Teimoori-Toolabi, Ladan, Asgari, Mojgan, Shahrokh, Hossein, Abolhasani, Maryam, Mahdian, Reza, and Fard-Esfahani, Pezhman

Subjects

MICRORNA, TUMOR suppressor genes, DIAGNOSIS, PROSTATE cancer, PROSTATE cancer treatment, CANCER cells, THERAPEUTICS, CANCER treatment

Abstract

Over the latest decade, the role of microRNAs (miRNAs/miRs) has received more attention. miRNAs are small non-coding RNAs that may serve a role as oncogenes or tumor suppressor genes. Certain miRNAs regulate the apoptosis pathway by influencing pro- or anti-apoptotic genes. We hypothesized that increases in the expression of B cell lymphoma 2 (BCL2) and BCL2-like 1 (BCL2L1) genes, which have been reported in various types of cancer tissues, may be due to the downregulation of certain miRNAs. The present study aimed to identify miRNAs that target BCL2 and BCL2L1 anti-apoptotic genes in prostate cancer (PCa) clinical tissue samples. Certain candidate miRNAs were selected bioinformatically and their expression in PCa samples was analyzed and compared with that in benign prostatic hyperplasia (BPH) tissue samples. The candidate miRNAs that targeted BCL2 and BCL2L1 genes were searched in online databases (miRWalk, microRNA.org, miRDB and TargetScan). A total of 12 miRNAs that target the 3'-untranslated region of the aforementioned genes and/or for which downregulation of their expression has previously been reported in cancer tissues. A total of 30 tumor tissue samples from patients with PCa and 30 samples tissues from patients with BPH were obtained and were subjected to reverse transcription-quantitative polymerase chain reaction for expression analysis of 12 candidate miRNAs, and the BCL2 and BCL2L1 genes. Additionally, expression of 3 finally selected miRNAs and genes was evaluated in prostate cancer PC3 and DU145 cell lines and human umbilical vein endothelial cells. Among 12 miRNA candidates, the expression of miR-1266, miR-185 and miR-30c-2 was markedly downregulated in PCa tumor tissues and cell lines. Furthermore, downregulation of these miRNAs was associated with upregulation of the BCL2 and BCL2L1 genes. An inverse association between three miRNAs (miR-1266, miR-185 and miR-30c-2) and two anti-apoptotic genes (BCL2 and BCL2L1) may be considered for interventional miRNA therapy of PCa. [ABSTRACT FROM AUTHOR]

Published

2018

23. G-CSF mobilized peripheral blood stem cell collection for allogeneic transplantation in healthy donors: Analysis of factors affecting yield.

Author

Machaczka, Maciej, Hägglund, Hans, Staver, Emma, Joks, Monika, Hassan, Moustapha, Wahlin, Björn Engelbrekt, and Axdorph Nygell, Ulla

Abstract

Mobilized PBSC are the main source for allogeneic HSCT. We aimed to evaluate factors that affect CD34+ cell yield including the donor's age, gender, BSA, processed blood volume and the method of G-CSF dose calculation. Data from 170 healthy donors were analyzed. The concentration of CD34+ cells in the peripheral blood (PB) and the processed volume of blood were significantly correlated to CD34+ cells yield ( P < .00005 and P < .001, respectively). The G-CSF dose per m2 was significantly correlated to the concentration of CD34+ cells in the PB ( P = .0003) and in the product ( P = .01). Smaller BSA and less processed volume were found among female donors, who were given lesser G-CSF dose per m2, and showed lower yield compared to men. However, multivariate analysis of the yield showed that only the concentration of CD34+ cells in the PB and the processed volume remained independent significant. [ABSTRACT FROM AUTHOR]

Published

2017

24. Flavin-containing monooxygenase 3 (FMO3) role in busulphan metabolic pathway.

Author

El-Serafi, Ibrahim, Terelius, Ylva, Abedi-Valugerdi, Manuchehr, Naughton, Seán, Saghafian, Maryam, Moshfegh, Ali, Mattsson, Jonas, Potácová, Zuzana, and Hassan, Moustapha

Subjects

BUSULFAN, HEMATOPOIETIC stem cell transplantation, FLAVINS, MONOOXYGENASES, DRUG metabolism

Abstract

Busulphan (Bu) is an alkylating agent used in the conditioning regimen prior to hematopoietic stem cell transplantation (HSCT). Bu is extensively metabolized in the liver via conjugations with glutathione to form the intermediate metabolite (sulfonium ion) which subsequently is degraded to tetrahydrothiophene (THT). THT was reported to be oxidized forming THT-1-oxide that is further oxidized to sulfolane and finally 3-hydroxysulfolane. However, the underlying mechanisms for the formation of these metabolites remain poorly understood. In the present study, we performed in vitro and in vivo investigations to elucidate the involvement of flavin-containing monooxygenase-3 (FMO3) and cytochrome P450 enzymes (CYPs) in Bu metabolic pathway. Rapid clearance of THT was observed when incubated with human liver microsomes. Furthermore, among different recombinant microsomal enzymes, the highest intrinsic clearance for THT was obtained via FMO3 followed by several CYPs including 2B6, 2C8, 2C9, 2C19, 2E1 and 3A4. In Bu- or THT-treated mice, inhibition of FMO3 by phenylthiourea significantly suppressed the clearance of both Bu and THT. Moreover, the simultaneous administration of a high dose of THT (200μmol/kg) to Bu-treated mice reduced the clearance of Bu. Consistently, in patients undergoing HSCT, repeated administration of Bu resulted in a significant up-regulation of FMO3 and glutathione-S-transfrase -1 (GSTA1) genes. Finally, in a Bu-treated patient, additional treatment with voriconazole (an antimycotic drug known as an FMO3-substrate) significantly altered the Bu clearance. In conclusion, we demonstrate for the first time that FMO3 along with CYPs contribute a major part in busulphan metabolic pathway and certainly can affect its kinetics. The present results have high clinical impact. Furthermore, these findings might be important for reducing the treatment-related toxicity of Bu, through avoiding interaction with other concomitant used drugs during conditioning and hence improving the clinical outcomes of HSCT. [ABSTRACT FROM AUTHOR]

Published

2017

25. Toxicological effects of fludarabine and treosulfan conditioning before allogeneic stem-cell transplantation.

Author

Remberger, Mats, Törlen, Johan, Serafi, Ibrahim, Garming-Legert, Karin, Björklund, Andreas, Ljungman, Per, Sundin, Mikael, Hassan, Moustapha, Mattsson, Jonas, Törlen, Johan, Serafi, Ibrahim El, and Björklund, Andreas

Subjects

ANTIMETABOLITES, ANTIVIRAL agents, VASCULAR diseases, CYSTITIS, HEMATOPOIETIC stem cell transplantation, HEMORRHAGE, HOMOGRAFTS, IMMUNOSUPPRESSION, RESEARCH funding, BUSULFAN

Abstract

We studied early potential treosulfan-related toxicity in 118 patients treated with treosulfan-based conditioning before allogeneic hematopoietic stem-cell transplantation. Most patients (n = 93) had a hematological malignancy. In 80 cases, a HLA-A, -B and -DR matched unrelated donor was used, while 33 patients had a HLA-identical sibling donor, and five received an HLA-A, -B or -DR allele mismatched, unrelated donor. Levels of AST, ALT, and bilirubin were significantly increased 1 week after HSCT compared to before HSCT. However, only a few patients had transaminase levels >2 to 3 × the upper normal level. All patients became neutropenic; 61% were already so at the time of graft infusion. Nearly all patients engrafted, except for three who died very early. Non-relapse mortality was 7.5% at 100 days and 11.9% at 1 year after HSCT. Veno-occlusive disease of the liver occurred in one patient and hemorrhagic cystitis in two patients. This study shows that early regimen-related toxicity after HSCT was low despite similar marrow toxicities compared to myeloablative regimens. [ABSTRACT FROM AUTHOR]

Published

2017

26. Switch of Steady-State to an Accelerated Granulopoiesis in Response to Androctonus australis hector Venom.

Author

Kaddache, Asma, Hassan, Moustapha, Laraba-Djebari, Fatima, and Hammoudi-Triki, Djelila

Subjects

ANDROCTONUS australis, VENOM, BONE marrow, BUTHIDAE, TOXINS

Abstract

Although several studies have shown that scorpion venoms cause a systemic inflammatory response syndrome, little is known about the contribution of the hematopoietic organs. The aim of this study was to investigate the effect of Androctonus australis hector venom on the bone marrow and on local inflammatory mediators, in concordance with the systemic inflammatory reaction elicited in mice. The consequences of a direct interaction of venom with murine bone marrow cells were also assessed by in vitro study. Obtained results showed that the early systemic neutrophilia correlated with a rapid granulocyte mobilization. This response was followed by an accelerated granulopoiesis that was supported by TNF-α and IL-6 signals . In vitro data revealed that the venom exerted a proliferative effect on murine hematopoietic cells and stimulated their differentiation towards granulocyte lineage mainly through cytokine secretion. In conclusion, this study indicated that the bone marrow rapidly exerts its activity in response to the experimental envenomation via the granulopoiesis process and inflammatory mediators in concert with the development of a systemic response. The ability of venom to directly switch steady-state granulopoiesis to an accelerated state in vitro could aggravate the disturbance caused by the venom. Better understanding of the mechanisms involved may lead to the emergence of new targets to avoid cell spreading and accumulation by acting on the very early stage of the systemic inflammatory response. [ABSTRACT FROM AUTHOR]

Published

2017

27. From Roscovitine to CYC202 to Seliciclib -- from bench to bedside: discovery and development.

Author

Zhelev, Nikolai, Trifonov, Dimitar, Shudong Wang, Hassan, Moustapha, El Serafi, Ibrahim, and Mitev, Vanio

Subjects

CYCLIN-dependent kinase inhibitors, DRUG development, DRUG efficacy, CARDIAC hypertrophy, SYSTEMS biology

Abstract

This monograph reviews the discovery and development of the cyclin-dependent kinase inhibitor roscovitine (R-roscovitine, CYC202, Seliciclib). The authors summarise the in vitro and in vivo data that have formed the basis for clinical investigation of Seliciclib as an anti-cancer drug. Kinase selectivity, cellular effects and the pharmacological properties of the drug are discussed in addition to the clinical results of Seliciclib being reviewed. Novel results on the effect of the drug in cardiac hypertrophy are summarized and potential applications of Seliciclib in other therapeutic areas, including, inflammation, virology, glomerulonephritis and polycystic kidney disease, are discussed. Finally the authors argue that optimisation of the therapeutic effect of kinase inhibitors such as Seliciclib can be enhanced using a systems biology approach involving mathematical modelling of the molecular pathways regulating cell growth and division. [ABSTRACT FROM AUTHOR]

Published

2017

28. Biodistribution of biodegradable polymeric nano-carriers loaded with busulphan and designed for multimodal imaging.

Author

Asem, Heba, Ying Zhao, Fei Ye, Barrefelt, Åsa, Abedi-Valugerdi, Manuchehr, El-Sayed, Ramy, El-Serafi, Ibrahim, Abu-Salah, Khalid M., Hamm, Jörg, Muhammed, Mamoun, and Hassan, Moustapha

Subjects

POLYMERIC composites, BUSULFAN, NANOCARRIERS, DRUG delivery devices, BIODEGRADABLE nanoparticles, MAGNETIC resonance imaging, CANCER treatment

Abstract

Background: Multifunctional nanocarriers for controlled drug delivery, imaging of disease development and followup of treatment efficacy are promising novel tools for disease diagnosis and treatment. In the current investigation, we present a multifunctional theranostic nanocarrier system for anticancer drug delivery and molecular imaging. Superparamagnetic iron oxide nanoparticles (SPIONs) as an MRI contrast agent and busulphan as a model for lipophilic antineoplastic drugs were encapsulated into poly (ethylene glycol)-co-poly (caprolactone) (PEG-PCL) micelles via the emulsion-evaporation method, and PEG-PCL was labelled with VivoTag 680XL fluorochrome for in vivo fluorescence imaging. Results: Busulphan entrapment efficiency was 83% while the drug release showed a sustained pattern over 10 h. SPION loaded-PEG-PCL micelles showed contrast enhancement in T2*-weighted MRI with high r2* relaxivity. In vitro cellular uptake of PEG-PCL micelles labeled with fluorescein in J774A cells was found to be time-dependent. The maximum uptake was observed after 24 h of incubation. The biodistribution of PEG-PCL micelles functionalized with VivoTag 680XL was investigated in Balb/c mice over 48 h using in vivo fluorescence imaging. The results of real-time live imaging were then confirmed by ex vivo organ imaging and histological examination. Generally, PEG-PCL micelles were highly distributed into the lungs during the first 4 h post intravenous administration, then redistributed and accumulated in liver and spleen until 48 h post administration. No pathological impairment was found in the major organs studied. Conclusions: Thus, with loaded contrast agent and conjugated fluorochrome, PEG-PCL micelles as biodegradable and biocompatible nanocarriers are efficient multimodal imaging agents, offering high drug loading capacity, and sustained drug release. These might offer high treatment efficacy and real-time tracking of the drug delivery system in vivo, which is crucial for designing of an efficient drug delivery system. [ABSTRACT FROM AUTHOR]

Published

2016

29. Real generation of power quality disturbances.

Author

Nahoum, Pamela, Yammine, Emile, Karam, Elie, Najjar, Maged B., and Hassan, Moustapha El

Published

2015

30. Survey on electrical modeling methods applied on different battery types.

Author

Ghossein, Nagham El, Salameh, Jack P., Karami, Nabil, Hassan, Moustapha El, and Najjar, Maged B.

Published

2015

31. STUDIES ON THE DETERIORATION OF COPTIC MURAL PAINTINGS IN THE MONASTERY OF MARTYRS AND THE LUXOR TEMPLE.

Author

SALLAM, Ahmed, Ying ZHAO, HASSAN, Moustapha, TOPRAK, Muhammet, MUHAMMED, Mamoun, and UHEIDA, Abdusalam

Subjects

PRESERVATION of mural painting & decoration, ART deterioration, MARTYRS

Abstract

In this study the surfaces and cross sections of deteriorated Coptic mural paintings were investigated using Computer Tomography (CT) scan images and video, and points (voids) on the surface were analyzed. To our knowledge, it is the first report on the application of CT scan for the investigation of deteriorated Coptic mural painting surfaces in Upper Egypt. The samples tested were collected from two sites: the Monastery of Martyrs (Deir alShuhada-Esna) and the Luxor temple. The selection of these monasteries was due to their historical importance, which is directly related to Egyptian Coptic heritage. The deteriorated surfaces of the selected mural paintings were characterized using new avenues of computed X-ray tomography (CT scan) in order to gather sufficient information about their composition and structure. The obtained results show that CT scan images provided us with detailed information about the sample porosity and structure. In the case of the Martyrs monastery, it was found that the mural paintings consist of one layer which contains clay minerals (kaolinite, montmorillonite, and illite) in the form of coarse plaster. On the other hand, the Martyrs Monastery showed higher porosity than the Roman Fresco in the Luxor Temple. [ABSTRACT FROM AUTHOR]

Published

2016

32. The use of watermarking to multiplex stereo images.

Author

Kerek, Bilal El, Baba, Hani El, Hassan, Moustapha El, and Hassan, Bachar El

Published

2014

33. Cytochrome P450 Oxidoreductase Influences CYP2B6 Activity in Cyclophosphamide Bioactivation.

Author

El-Serafi, Ibrahim, Afsharian, Parvaneh, Moshfegh, Ali, Hassan, Moustapha, and Terelius, Ylva

Subjects

CYTOCHROME P-450, OXIDOREDUCTASES, CYCLOPHOSPHAMIDE, BIOTRANSFORMATION (Metabolism), HEALTH outcome assessment

Abstract

Introduction: Cyclophosphamide is commonly used as an important component in conditioning prior to hematopoietic stem cell transplantation, a curative treatment for several hematological diseases. Cyclophosphamide is a prodrug activated mainly by cytochrome P450 2B6 (CYP2B6) in the liver. A high degree of inter- and intra-individual variation in cyclophosphamide kinetics has been reported in several studies. Materials and Methods: Hydroxylation of cyclophosphamide was investigated in vitro using three microsomal batches of CYP2B6*1 with different ratios of POR/CYP expression levels. Twenty patients undergoing hematopoietic stem cell transplantation were also included in the study. All patients received an i.v. infusion of cyclophosphamide (60 mg/kg/day, for two days) as a part of their conditioning. Blood samples were collected from each patient before cyclophosphamide infusion, 6 h after the first dose and before and 6 h after the second dose. POR gene expression was measured by mRNA analysis and the pharmacokinetics of cyclophosphamide and its active metabolite were determined. Results: A strong correlation between the in vitro intrinsic clearance of cyclophosphamide and the POR/CYP ratio was found. The apparent Km for CYP2B6.1 was almost constant (3-4 mM), while the CLint values were proportional to the POR/CYP ratio (3-34 μL/min/nmol CYP). In patients, the average expression of the POR gene in blood was significantly (P <0.001) up-regulated after cyclophosphamide infusion, with high inter-individual variations and significant correlation with the concentration ratio of the active metabolite 4-hydroxy-cyclophosphamide/cyclophosphamide. Nine patients were carriers for POR*28; four patients had relatively high POR expression. Conclusions: This investigation shows for the first time that POR besides CYP2B6 can influence cyclophosphamide metabolism. Our results indicate that not only CYPs are important, but also POR expression and/or activity may influence cyclophosphamide bioactivation, affecting therapeutic efficacy and treatment related toxicity and hence on clinical outcome. Thus, both POR and CYP genotype and expression levels may have to be taken into account when personalizing treatment schedules to achieve optimal therapeutic drug plasma concentrations of cyclophosphamide. [ABSTRACT FROM AUTHOR]

Published

2015

34. The effect of circadian rhythm on pharmacokinetics and metabolism of the Cdk inhibitor, roscovitine, in tumor mice model.

Author

Sallam, Hatem, El-Serafi, Ahmed T., Filipski, Elisabeth, Terelius, Ylva, Lévi, Francis, and Hassan, Moustapha

Subjects

CIRCADIAN rhythms, PHARMACOKINETICS, CYCLIN-dependent kinase inhibitors, CLINICAL trials, CANCER chemotherapy, TUMOR growth, DRUG administration, LABORATORY mice

Abstract

Roscovitine is a selective Cdk-inhibitor that is under investigation in phase II clinical trials under several conditions, including chemotherapy. Tumor growth inhibition has been previously shown to be affected by the dosing time of roscovitine in a Glasgow osteosarcoma xenograft mouse model. In the current study, we examined the effect of dose timing on the pharmacokinetics, biodistribution and metabolism of this drug in different organs in B6D2F1 mice. The drug was orally administered at resting (ZT3) or activity time of the mice (ZT19) at a dose of 300 mg/kg. Plasma and organs were removed at serial time points (10, 20 and 30 min; 1, 2, 4, 6, 8, 12 and 24 h) after the administration. Roscovitine and its carboxylic metabolite concentrations were analyzed using HPLC-UV, and pharmacokinetic parameters were calculated in different organs. We found that systemic exposure to roscovitine was 38% higher when dosing at ZT3, and elimination half-life was double compared to when dosing at ZT19. Higher organ concentrations expressed as (organ/plasma) ratio were observed when dosing at ZT3 in the kidney (180%), adipose tissue (188%), testis (132%) and lungs (112%), while the liver exposure to roscovitine was 120% higher after dosing at ZT19. The metabolic ratio was approximately 23% higher at ZT19, while the intrinsic clearance (CLint) was approximately 67% higher at ZT19, indicating faster and more efficient metabolism. These differences may be caused by circadian differences in the absorption, distribution, metabolism and excretion processes governing roscovitine disposition in the mice. In this article, we describe for the first time the chronobiodistribution of roscovitine in the mouse and the contribution of the dosing time to the variability of its metabolism. Our results may help in designing better dosing schedules of roscovitine in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2015

35. A New Technique to Multiplex Stereo Images: LSB Watermarking and Hamming Code.

Author

Kerek, Bilal El, Baba, Hani El, Hassan, Moustapha El, and Hassan, Bachar El

Published

2013

36. Implementation of wireless network using location fingerprinting technique for indoor positioning.

Author

Hassan, Moustapha El, Hassan, Bachar El, and Nachabe, Lina

Abstract

The goal of this paper is to implement a wireless positioning system based on the RF wave, which can be used in an internal environment. First, localization in a wireless sensor network is simulated using Matlab. Then, a ZigBee network has been implemented using a technique known as location fingerprinting, which is based on signal strength to estimate the position of a moving object. Finally, the results are analyzed to conclude on the performance of the method used. [ABSTRACT FROM PUBLISHER]

Published

2012

37. DYNAMIC MR IMAGING, BIODISTRIBUTION AND PHARMACOKINETICS OF POLYMER SHELLED MICROBUBBLES CONTAINING SPION.

Author

BARREFELT, ÅSA, PARADOSSI, GAIO, ASEM, HEBA, MARGHERITELLI, SILVIA, SAGHAFIAN, MARYAM, ODDO, LETIZIA, MUHAMMED, MAMOUN, ASPELIN, PETER, HASSAN, MOUSTAPHA, and BRISMAR, TORKEL B.

Subjects

MAGNETIC resonance imaging, DRUG analysis, MEDICAL polymers, MICROBUBBLES, NONINVASIVE diagnostic tests, IRON oxide nanoparticles

Abstract

Magnetic Resonance Imaging (MRI) is a noninvasive diagnostic method that provides information on morphological and physiological changes of the internal organs over time. Imaging and measurements can be repeated on the same subject, thereby reducing inter-individual variability effects and hence the number of subjects required. A potential MRI contrast agent consisting of microbubbles embedded with superparamagnetic iron oxide nanoparticles (SPION) in the shell (SPION MBs) was injected intravenously into rats to determine their biodistribution and pharmacokinetics using MR imaging. Agarose phantoms containing SPION MBs were scanned using 3 T MRI to construct a standard curve. Rats were injected with SPION MBs, free SPION or plain MBs and scanned dynamically at 3 T using a clinical MR scanner. The relaxation rate (R2*) was studied over time as a measure of the iron oxide concentrations to enable calculation of the pharmacokinetic parameters. The kinetics of SPION MBs in the liver was fitted to a one-compartment model. Furthermore, the biological fate of SPION MBs was examined via a histological survey of tissue samples using Perls' Prussian blue staining and immunohistochemistry (IHC). 1.2 h after injection of SPION MBs, T2* of the liver had decreased to its minimum. The elimination half-life of SPION MBs was 598.2 ± 97.3 h, while the half-life for SPION was 222.6 ± 26.4 h. Moreover, our study showed that SPION MBs were taken up by the macrophages in the lungs, spleen and liver. MBs labeled with SPION can be used for MR imaging. Moreover, MRI is a reliable and noninvasive tool that can be utilized in pharmacokinetic investigations of future contrast agents using SPION MBs and SPION in the rat. Biodistribution and pharmacokinetics of polymer shelled microbubbles (MBs), embedded with superparamagnetic iron oxide nanoparticles (SPION) in the shell, were determined in rats using dynamic Magnetic Resonance (MR) imaging. The histological survey of tissue samples showed that SPION MBs were taken up by macrophages in the lungs, spleen and liver. The elimination half-life of SPION MBs was longer than that of SPION. This study shows that MRI is a reliable and non-invasive method for pharmacokinetic calculations. [ABSTRACT FROM AUTHOR]

Published

2014

38. Rat islets are not rejected by anti-islet antibodies in mice treated with costimulation blockade.

Author

Diab, Randa A. H., Hassan, Moustapha, Tibell, Annika, Holgersson, Jan, and Kumagai‐Braesch, Makiko

Subjects

XENOGRAFTS, ISLET cell tumor, ISLANDS of Langerhans, IMMUNOGLOBULINS, ALLOXAN, GLUCOSE tolerance tests, TRANSPLANTATION of organs, tissues, etc.

Abstract

Background Costimulation blockade can prevent rejection of islet xenografts in naïve but not sensitized recipients. Donor-specific antibodies ( DSA) may partly explain this observation. The effect of DSA on rat islet xenograft survival in mice receiving costimulation blockade was investigated. Methods Naïve C57 BL/6 mice with alloxan-induced diabetes were transplanted under the left kidney capsule with 100 Lewis rat islets. Recipients were divided into three groups receiving: (i) isotype control antibodies (Abs); (ii) anti- CD154 and CTLA4Ig; or (iii) anti- CD154, CTLA4Ig, and anti- LFA-1 every second day, day 0-8. At the time of transplantation (Tx), half of the animals in each group received naïve mouse serum and half xenoimmune serum derived from mice previously transplanted with rat islets. Non-fasting blood glucose levels and body weight were followed daily. Cured mice were examined by intraperitoneal glucose tolerance ( IPGT) tests at 1 and 4 months after transplantation. Results Donor-specific antibodies were detected in immune serum-injected recipients up to at least 96 h post-Tx. Short term (≤96 h), there was no significant difference with regard to graft mass, infiltrating and apoptotic cells between groups of mice receiving naïve and immune sera. A moderate infiltration of polymorphonuclear and mononuclear cells was seen 96 h post-Tx in mice given control Abs, whether or not they received immune or naïve mouse serum. Mice given costimulation blockade had well-maintained endocrine tissue and very little cell infiltration. There was no significant difference in islet xenograft function and survival long term between groups receiving naïve and immune sera in combination with costimulation blockade. About half of the mice receiving costimulation blockade lost graft function within 110 days. Conclusion The presence at Tx of DSA does not appear to negatively influence early and late islet xenograft survival in mice receiving costimulation blockade. [ABSTRACT FROM AUTHOR]

Published

2014

39. The nanoparticulate Quillaja saponin KGI exerts anti-proliferative effects by down-regulation of cell cycle molecules in U937 and HL-60 human leukemia cells.

Author

Berenjian, Saideh, Hu, Kefei, Abedi-Valugerdi, Manuchehr, Hassan, Moustapha, Bashir Hassan, Sadia, and Morein, Bror

Subjects

PHYSIOLOGICAL effects of nanoparticles, QUILLAJA, CELL cycle regulation, CYCLIN-dependent kinases regulation, CYCLIN genetics, LEUKEMIA treatment, MYELOID leukemia, BIOCHEMICAL mechanism of action, CANCER cell proliferation, PREVENTION

Abstract

Cancer cells are characterized by uncontrolled replication involving loss of control of cyclin dependent kinases (CDKs) and cyclins, and by abolished differentiation. In this study we introduce KGI, which is a nanoparticle with a Quillaja saponin as an active molecule. By the use of RNA array analysis and confirmation at the protein level, we show that KGI affects myeloid leukemia cells (in particular, the U937 monoblast cancer cell) by the following mechanisms: (A) ceasing cell replication via proteasome degradation, (B) down-regulation of key molecules at check points between G1/S and G2/M phases, (C) reduction of thymidine kinase activity, followed by (D) exit to differentiation and production of interleukin-8 (IL-8), eventually leading to apoptosis. Leukemia cell lines (U937 and HL-60 cells) were exposed to KGI for 8 h, after which the drug was removed. The cancer cells did not revert to replication over the following 10 days. Thus our findings suggest that the nanoparticle KGI inhibits proliferation and promotes differentiation in leukemic cells by interfering with the cell cycle process. [ABSTRACT FROM AUTHOR]

Published

2014

40. Cyclophosphamide Alters the Gene Expression Profile in Patients Treated with High Doses Prior to Stem Cell Transplantation.

Author

El-Serafi, Ibrahim, Abedi-Valugerdi, Manuchehr, Potácová, Zuzana, Afsharian, Parvaneh, Mattsson, Jonas, Moshfegh, Ali, and Hassan, Moustapha

Subjects

HEMATOPOIETIC stem cell transplantation, CYCLOPHOSPHAMIDE, GENE expression, CANCER chemotherapy, BONE marrow transplantation, IMMUNE response

Abstract

Background: Hematopoietic stem cell transplantation is a curative treatment for several haematological malignancies. However, treatment related morbidity and mortality still is a limiting factor. Cyclophosphamide is widely used in condition regimens either in combination with other chemotherapy or with total body irradiation. Methods: We present the gene expression profile during cyclophosphamide treatment in 11 patients conditioned with cyclophosphamide for 2 days followed by total body irradiation prior to hematopoietic stem cell transplantation. 299 genes were identified as specific for cyclophosphamide treatment and were arranged into 4 clusters highly down-regulated genes, highly up-regulated genes, early up-regulated but later normalized genes and moderately up-regulated genes. Results: Cyclophosphamide treatment down-regulated expression of several genes mapped to immune/autoimmune activation and graft rejection including CD3, CD28, CTLA4, MHC II, PRF1, GZMB and IL-2R, and up-regulated immune-related receptor genes, e.g. IL1R2, IL18R1, and FLT3. Moreover, a high and significant expression of ANGPTL1 and c-JUN genes was observed independent of cyclophosphamide treatment. Conclusion: This is the first investigation to provide significant information about alterations in gene expression following cyclophosphamide treatment that may increase our understanding of the cyclophosphamide mechanism of action and hence, in part, avoid its toxicity. Furthermore, ANGPTL1 remained highly expressed throughout the treatment and, in contrast to several other alkylating agents, cyclophosphamide did not influence c-JUN expression. [ABSTRACT FROM AUTHOR]

Published

2014

41. Comparison of Algorithms for Oral Busulphan Area Under the Concentration-Time Curve Limited Sampling Estimate.

Author

Sjöö, Fredrik, El-Serafi, Ibrahim, Enestig, Jon, Mattsson, Jonas, Liwing, Johan, and Hassan, Moustapha

Subjects

STEM cell transplantation, ORAL medication, PHARMACOKINETICS, HEALTH outcome assessment, ESTIMATES, PEDIATRICS

Abstract

Background and Objectives: Therapeutic drug monitoring (TDM) of the first dose of busulphan during conditioning prior to allogeneic stem cell transplantation provides the possibility of improving the clinical outcome via dose adjustment of subsequent doses. The plasma area under the concentration-time curve (AUC) for busulphan is generally accepted as the parameter that gives the best exposure estimate; however, the sampling frequency needed for reliable AUC calculation remains controversial. The aim of the present investigation was to develop and evaluate a limited sampling model for oral busulphan. Methods: We have compared models using three to four samples with standard WinNonlin adaptive compartment modeling based on eight samples as reference. The evaluated study population included both adult and pediatric patients, but the linear model was devised using analysis of only pediatric patient plasma concentrations. The present model was developed using data from 23 patients with a mean age of 38 years (range 13-59 years) and was evaluated in 20 pediatric patients with a mean age of 6 years (range 0.1-13 years) as well as 23 adult patients (mean age 43 years; range 18-67 years). Results: In 23 patients, the mean AUC from a curve fitting model (Purves method) and a single compartment model had an intraclass correlation coefficient (ICC) of 0.947. From a log-log plot of AUC values it was evident that using this estimate of the AUC would affect dose adjustment decisions for very few of the patients. Applying the linear model using three samples resulted in an ICC of 0.932, mostly due to worse performance in the adult population. Conclusions: The present results support the use of limited sampling in clinical TDM for oral busulphan provided adequate algorithms and sampling times are used. Moreover, they also demonstrate the caution that is needed when transferring a pharmacokinetic model from a pediatric population to an adult population. [ABSTRACT FROM AUTHOR]

Published

2014

42. Pharmacokinetics and biodistribution of the cyclin-dependent kinase inhibitor -CR8- in mice.

Author

Sallam, Hatem, El-Serafi, Ibrahim, Meijer, Laurent, and Hassan, Moustapha

Subjects

PHARMACOKINETICS, BIOAVAILABILITY, CYCLIN-dependent kinase inhibitors, LABORATORY mice, APOPTOSIS, LIQUID chromatography

Abstract

Background: CR8 is a second generation inhibitor of cyclin-dependent kinases derived from roscovitine. CR8 was shown to be 50-100 fold more potent than roscovitine in inducing apoptosis in different tumor cell lines. In the present investigation, we have established an analytical method for the quantification of CR8 in biological samples and evaluated its bioavailability, biodistribution and pharmacokinetics in mice. Methods: A liquid chromatography method utilizing UV-detection was used for the determination of CR8. CR8 was administered either orally (100 mg/kg) or i.v. (50 mg/kg) and the animals were sacrificed at different time points. Blood samples and organs were collected, after which the pharmacokinetic parameters were calculated for plasma and organs. Results: CR8 was eluted at 5 minutes in the high performance liquid chromatography system used. The LLOQ detection was 0.10 µg/ml and linearity was observed within the 0.10-10 µg/ml range (r² > 0.998). The accuracy and precision were >86%, while the recovery from plasma was >95%. CR8 was stable for 2 months at room temperature in both solution and plasma. CR8 pharmacokinetics was fitted to a two-compartment open model after oral administration and to a one compartment model after i.v. injection. The elimination half-life was about 3 hours. Organ exposure to CR8 (expressed as % AUC organ vs. AUC plasma) was highest in liver (205%), adipose tissue (188%) and kidney (150%) and low in bone marrow (30%) and brain (15%) as compared to plasma. The oral bioavailability of CR8 was found to be essentially 100%. Conclusions: We have developed a rapid and simple method for the analysis of CR8. CR8 pharmacokinetics pattern showed 100% bioavailability, long half-life and limited distribution to brain and bone marrow, which may allow systemic exposure higher than the IC50 reported for cell death in tumor cell lines. CR8 displays favorable pharmacological properties and is therefore a good candidate for future clinical studies. [ABSTRACT FROM AUTHOR]

Published

2013

43. Biodistribution, kinetics, and biological fate of SPION microbubbles in the rat.

Author

Barrefelt, Åsa, Saghafian, Maryam, Kuiper, Raoul, Fei Ye, Egri, Gabriella, Klickermann, Moritz, Brismar, Torkel B., Aspelin, Peter, Muhammed, Mamoun, Dähne, Lars, and Hassan, Moustapha

Published

2013

44. Activation of Wnt/β-Catenin Pathway in Monocytes Derived from Chronic Kidney Disease Patients.

Author

Al-Chaqmaqchi, Heevy Abdulkareem Musa, Moshfegh, Ali, Dadfar, Elham, Paulsson, Josefin, Hassan, Moustapha, Jacobson, Stefan H., and Lundahl, Joachim

Subjects

WNT genes, CATENIN genetics, MONOCYTES, KIDNEY diseases, CARDIOVASCULAR disease related mortality, PATHOLOGICAL physiology, GENE expression, ATHEROSCLEROSIS, DISEASE susceptibility, PATIENTS

Abstract

Patients with chronic kidney disease (CKD) have significantly increased morbidity and mortality resulting from infections and cardiovascular diseases. Since monocytes play an essential role in host immunity, this study was directed to explore the gene expression profile in order to identify differences in activated pathways in monocytes relevant to the pathophysiology of atherosclerosis and increased susceptibility to infections. Monocytes from CKD patients (stages 4 and 5, estimated GFR <20 ml/min/1.73 m2) and healthy donors were collected from peripheral blood. Microarray gene expression profile was performed and data were interpreted by GeneSpring software and by PANTHER tool. Western blot was done to validate the pathway members. The results demonstrated that 600 and 272 genes were differentially up- and down regulated respectively in the patient group. Pathways involved in the inflammatory response were highly expressed and the Wnt/β-catenin signaling pathway was the most significant pathway expressed in the patient group. Since this pathway has been attributed to a variety of inflammatory manifestations, the current findings may contribute to dysfunctional monocytes in CKD patients. Strategies to interfere with this pathway may improve host immunity and prevent cardiovascular complications in CKD patients. [ABSTRACT FROM AUTHOR]

Published

2013

45. The Role of Programmed Cell Death Ligand-1 (PD-L1/CD274) in the Development of Graft versus Host Disease.

Author

Al-Chaqmaqchi, Heevy, Sadeghi, Behnam, Abedi-Valugerdi, Manuchehr, Al-Hashmi, Sulaiman, Fares, Mona, Kuiper, Raoul, Lundahl, Joachim, Hassan, Moustapha, and Moshfegh, Ali

Subjects

GRAFT versus host disease, MOLECULAR genetics, COMPUTATIONAL biology, GENE expression, CELL death, DEVELOPMENTAL biology, HEMATOPOIETIC stem cells

Abstract

Programmed cell death ligand-1 (PD-L1/CD274) is an immunomodulatory molecule involved in cancer and complications of bone marrow transplantation, such as graft rejection and graft-versus-host disease. The present study was designed to assess the dynamic expression of this molecule after hematopoietic stem cell transplantation in relation to acute graft-versus-host disease. Female BALB/c mice were conditioned with busulfan and cyclophosphamide and transplanted with either syngeneic or allogeneic (male C57BL/6 mice) bone marrow and splenic cells. The expression of PD-L1 was evaluated at different time points employing qPCR, western blot and immunohistochemistry. Allogeneic- but not syngeneic-transplanted animals exhibited a marked up-regulation of PD-L1 expression in the muscle and kidney, but not the liver, at days 5 and 7 post transplantation. In mice transplanted with allogeneic bone marrow cells, the enhanced expression of PD-L1 was associated with high serum levels of IFNγ and TNFα at corresponding intervals. Our findings demonstrate that PD-L1 is differently induced and expressed after allogeneic transplantation than it is after syngeneic transplantation, and that it is in favor of target rather than non-target organs at the early stages of acute graft-versus-host disease. This is the first study to correlate the dynamics of PD-L1 at the gene-, protein- and activity levels with the early development of acute graft-versus-host disease. Our results suggest that the higher expression of PD-L1 in the muscle and kidney (non-target tissues) plays a protective role in skeletal muscle during acute graft-versus-host disease. [ABSTRACT FROM AUTHOR]

Published

2013

46. Role of pharmacogenetics in busulfan/cyclophosphamide conditioning therapy prior to hematopoietic stem cell transplantation.

Author

Hassan, Moustapha and Andersson, Borje S.

Published

2013

47. Busulphan-Cyclophosphamide Cause Endothelial Injury, Remodeling of Resistance Arteries and Enhanced Expression of Endothelial Nitric Oxide Synthase.

Author

Al-Hashmi, Sulaiman, Boels, Piet J. M., Zadjali, Fahad, Sadeghi, Behnam, Sällström, Johan, Hultenby, Kjell, Hassan, Zuzana, Arner, Anders, and Hassan, Moustapha

Subjects

STEM cell transplantation, CYCLOPHOSPHAMIDE, CARDIOVASCULAR diseases, MESENTERIC artery, NITRIC oxide, LABORATORY mice

Abstract

Stem cell transplantation (SCT) is a curative treatment for malignant and non malignant diseases. However, transplantationrelated complications including cardiovascular disease deteriorate the clinical outcome and quality of life. We have investigated the acute effects of conditioning regimen on the pharmacology, physiology and structure of large elastic arteries and small resistance-sized arteries in a SCT mouse model. Mesenteric resistance arteries and aorta were dissected from Balb/c mice conditioned with busulphan (Bu) and cyclophosphamide (Cy). In vitro isometric force development and pharmacology, in combination with RT-PCR, Western blotting and electron microscopy were used to study vascular properties. Compared with controls, mesenteric resistance arteries from the Bu-Cy group had larger internal circumference, showed enhanced endothelium mediated relaxation and increased expression of endothelial nitric oxide synthase (eNOS). Bu-Cy treated animals had lower mean blood pressure and signs of endothelial injury. Aortas of treated animals had a higher reactivity to noradrenaline. We conclude that short-term consequences of Bu-Cy treatment divergently affect large and small arteries of the cardiovascular system. The increased noradrenaline reactivity of large elastic arteries was not associated with increased blood pressure at rest. Instead, Bu-Cy treatment lowered blood pressure via augmented microvascular endothelial dependent relaxation, increased expression of vascular eNOS and remodeling toward a larger lumen. The changes in the properties of resistance arteries can be associated with direct effects of the compounds on vascular wall or possibly indirectly induced via altered translational activity associated with the reduced hematocrit and shear stress. This study contributes to understanding the mechanisms that underlie the early effects of conditioning regimen on resistance arteries and may help in designing further investigations to understand the late effects on vascular system. [ABSTRACT FROM AUTHOR]

Published

2012

48. Inhibition of proteasome deubiquitinating activity as a new cancer therapy.

Author

D'Arcy, Pádraig, Brnjic, Slavica, Olofsson, Maria Hägg, Fryknäs, Mårten, Lindsten, Kristina, De Cesare, Michelandrea, Perego, Paola, Sadeghi, Behnam, Hassan, Moustapha, Larsson, Rolf, and Linder, Stig

Subjects

CANCER treatment, TARGETED drug delivery, UBIQUITIN, B cell lymphoma, MULTIPLE myeloma, CANCER invasiveness

Abstract

Ubiquitin-tagged substrates are degraded by the 26S proteasome, which is a multisubunit complex comprising a proteolytic 20S core particle capped by 19S regulatory particles. The approval of bortezomib for the treatment of multiple myeloma validated the 20S core particle as an anticancer drug target. Here we describe the small molecule b-AP15 as a previously unidentified class of proteasome inhibitor that abrogates the deubiquitinating activity of the 19S regulatory particle. b-AP15 inhibited the activity of two 19S regulatory-particle-associated deubiquitinases, ubiquitin C-terminal hydrolase 5 (UCHL5) and ubiquitin-specific peptidase 14 (USP14), resulting in accumulation of polyubiquitin. b-AP15 induced tumor cell apoptosis that was insensitive to TP53 status and overexpression of the apoptosis inhibitor BCL2. We show that treatment with b-AP15 inhibited tumor progression in four different in vivo solid tumor models and inhibited organ infiltration in an acute myeloid leukemia model. Our results show that the deubiquitinating activity of the 19S regulatory particle is a new anticancer drug target. [ABSTRACT FROM AUTHOR]

Published

2011

49. Therapeutic drug monitoring is essential for intravenous busulfan therapy in pediatric hematopoietic stem cell recipients.

Author

Malär, Reta, Sjöö, Fredrik, Rentsch, Katharina, Hassan, Moustapha, and Güngör, Tayfun

Subjects

DRUG monitoring, HEMATOPOIETIC stem cells, STEM cells, OPERATIVE surgery, THERAPEUTICS

Abstract

Malär R, Sjöö F, Rentsch K, Hassan M, Güngör T. Therapeutic drug monitoring is essential for intravenous busulfan therapy in pediatric hematopoietic stem cell recipients. Pediatr Transplantation 2011: 15: 580-588. © 2011 John Wiley & Sons A/S. Abstract: Busulfan is widely used for myeloablative conditioning in HSCT. Intravenous busulfan has been introduced to reduce interindividual variability in plasma levels especially in pediatric patients. TDM of intravenous busulfan was performed in 34 pediatric HSCT patients with malignant (n = 9) and non-malignant (n = 25) diseases (50% of patients

Published

2011

50. N-acetyl-.

Author

Karlsson, Helen, Nava, Silvia, Remberger, Mats, Hassan, Zuzana, Hassan, Moustapha, and Ringdén, Olle

Published

2011