Your search keyword '"Arapshian, A."' showing total 104 results

1. Surgical management of patients with von Willebrand disease: summary of 2 systematic reviews of the literature

Author

Brignardello-Petersen, Romina, El Alayli, Abdallah, Husainat, Nedaa, Kalot, Mohamad, Shahid, Shaneela, Aljabirii, Yazan, Britt, Alec, Alturkmani, Hani, El-Khechen, Hussein, Motaghi, Shahrzad, Roller, John, Dimassi, Ahmad, Abughanimeh, Omar, Madoukh, Bader, Arapshian, Alice, Grow, Jean M., Kouides, Peter, Laffan, Michael, Leebeek, Frank W.G., O'Brien, Sarah H., Tosetto, Alberto, James, Paula D., Connell, Nathan T., Flood, Veronica, and Mustafa, Reem A.

Published

2022

2. ASH ISTH NHF WFH 2021 guidelines on the management of von Willebrand disease

Author

Connell, Nathan T., Flood, Veronica H., Brignardello-Petersen, Romina, Abdul-Kadir, Rezan, Arapshian, Alice, Couper, Susie, Grow, Jean M., Kouides, Peter, Laffan, Michael, Lavin, Michelle, Leebeek, Frank W.G., O'Brien, Sarah H., Ozelo, Margareth C., Tosetto, Alberto, Weyand, Angela C., James, Paula D., Kalot, Mohamad A., Husainat, Nedaa, and Mustafa, Reem A.

Published

2021

3. Surgical management of patients with von Willebrand disease: summary of 2 systematic reviews of the literature

Author

Bader Madoukh, Reem A. Mustafa, Omar Abughanimeh, John Roller, Paula D. James, Abdallah El Alayli, Hani Alturkmani, Mohamad A. Kalot, Alberto Tosetto, Ahmad Bilal Dimassi, Frank W.G. Leebeek, Michael Laffan, Peter A. Kouides, Veronica H. Flood, Yazan Aljabirii, Shaneela Shahid, Alec Britt, Shahrzad Motaghi, Sarah H. O'Brien, Jean M. Grow, Nedaa Husainat, Alice Arapshian, Nathan T. Connell, Romina Brignardello-Petersen, and Hussein El Khechen

Subjects

medicine.medical_specialty, MEDLINE, HEPATITIS-C, GUIDELINES, law.invention, HEMORRHAGE, Randomized controlled trial, law, Internal medicine, hemic and lymphatic diseases, von Willebrand Factor, medicine, Von Willebrand disease, Humans, Hemostasis, Science & Technology, Factor VIII, Perioperative management, HEMOPHILIA, business.industry, Hematology, medicine.disease, EFFICACY, CONCENTRATE WILATE(R), REPLACEMENT, von Willebrand Diseases, Systematic review, Minor surgery, Tranexamic Acid, SAFETY, Observational study, Systematic Review, business, Life Sciences & Biomedicine, Tranexamic acid, medicine.drug

Abstract

von Willebrand disease (VWD) is the most common inherited bleeding disorder. The management of patients with VWD who are undergoing surgeries is crucial to prevent bleeding complications. We systematically summarized the evidence on the management of patients with VWD who are undergoing major and minor surgeries to support the development of practice guidelines. We searched Medline and EMBASE from inception through October 2019 for randomized clinical trials (RCTs), comparative observational studies, and case series that compared maintaining factor VIII (FVIII) levels or von Willebrand factor (VWF) levels at >0.50 IU/mL for at least 3 days in patients undergoing major surgery, and those with options for perioperative management of patients undergoing minor surgery. Two authors screened and abstracted data and assessed the risk of bias. We conducted meta-analyses when possible. We evaluated the certainty of the evidence using the Grading of Recommendations, Assessment, Development and Evaluations (GRADE) approach. We included 7 case series for major surgeries and 2 RCTs and 12 case series for minor surgeries. Very-low-certainty evidence showed that maintaining FVIII levels or VWF levels of >0.50 IU/mL for at least 3 consecutive days showed excellent hemostatic efficacy (as labeled by the researchers) after 74% to 100% of major surgeries. Low- to very-low-certainty evidence showed that prescribing tranexamic acid and increasing VWF levels to 0.50 IU/mL resulted in fewer bleeding complications after minor procedures compared with increasing VWF levels to 0.50 IU/mL alone. Given the low-quality evidence for guiding management decisions, a shared-decision model leading to individualized therapy plans will be important in patients with VWD who are undergoing surgical and invasive procedures.

Published

2022

4. ASH ISTH NHF WFH 2021 guidelines on the management of von Willebrand disease

Author

Veronica H. Flood, Jean M. Grow, Reem A. Mustafa, Michael Laffan, Susie Couper, Frank W.G. Leebeek, Angela C. Weyand, Mohamad A. Kalot, Romina Brignardello-Petersen, Alice Arapshian, Sarah H. O'Brien, Rezan Abdul-Kadir, Peter A. Kouides, Margareth C. Ozelo, Paula D. James, Michelle Lavin, Nedaa Husainat, Nathan T. Connell, Alberto Tosetto, and Hematology

Subjects

medicine.medical_specialty, MEDLINE, Context (language use), 030204 cardiovascular system & hematology, Hemophilia A, 03 medical and health sciences, 0302 clinical medicine, Health care, medicine, Von Willebrand disease, Humans, Intensive care medicine, Desmopressin, Hemostasis, business.industry, Thrombosis, Hematology, Guideline, Venous Thromboembolism, medicine.disease, Bleeding diathesis, von Willebrand Diseases, Female, Implementation research, business, Clinical Guidelines, 030215 immunology, medicine.drug

Abstract

Background: von Willebrand disease (VWD) is a common inherited bleeding disorder. Significant variability exists in management options offered to patients. Objective: These evidence-based guidelines from the American Society of Hematology (ASH), the International Society on Thrombosis and Haemostasis (ISTH), the National Hemophilia Foundation (NHF), and the World Federation of Hemophilia (WFH) are intended to support patients, clinicians, and health care professionals in their decisions about management of VWD. Methods: ASH, ISTH, NHF, and WFH formed a multidisciplinary guideline panel. Three patient representatives were included. The panel was balanced to minimize potential bias from conflicts of interest. The University of Kansas Outcomes and Implementation Research Unit and the McMaster Grading of Recommendations Assessment, Development and Evaluation (GRADE) Centre supported the guideline development process, including performing and updating systematic evidence reviews (through November 2019). The panel prioritized clinical questions and outcomes according to their importance to clinicians and patients. The panel used the GRADE approach, including GRADE Evidence-to-Decision frameworks, to assess evidence and make recommendations, which were subject to public comment. Results: The panel agreed on 12 recommendations and outlined future research priorities. Conclusions: These guidelines make key recommendations regarding prophylaxis for frequent recurrent bleeding, desmopressin trials to determine therapy, use of antiplatelet agents and anticoagulant therapy, target VWF and factor VIII activity levels for major surgery, strategies to reduce bleeding during minor surgery or invasive procedures, management options for heavy menstrual bleeding, management of VWD in the context of neuraxial anesthesia during labor and delivery, and management in the postpartum setting.

Published

2021

5. Outcomes of long-term von Willebrand factor prophylaxis use in von Willebrand disease: A systematic literature review

Author

Abdallah El Alayli, Romina Brignardello Petersen, Nedaa M. Husainat, Mohamad A. Kalot, Yazan Aljabiri, Hani Turkmani, Alec Britt, Hussein El‐Khechen, Shaneela Shahid, John Roller, Shahrzad Motaghi, Razan Mansour, Alberto Tosetto, Rezan Abdul‐Kadir, Michael Laffan, Angela Weyand, Frank W.G. Leebeek, Alice Arapshian, Peter Kouides, Paula James, Nathan T. Connell, Veronica H. Flood, and Reem A. Mustafa

Subjects

bleeding disorder, Science & Technology, epistaxis, bleeding episodes, FACTOR CONCENTRATE, 1103 Clinical Sciences, General Medicine, Hematology, EFFICACY, Hospitalization, von Willebrand Diseases, Cardiovascular System & Hematology, QUALITY-OF-LIFE, WILATE, SAFETY, Chronic Disease, von Willebrand Factor, MODERATE, Humans, COHORT, prophylaxis, Hemophilia, Life Sciences & Biomedicine, Genetics (clinical), Von Willebrand Disease

Abstract

Background Von Willebrand Disease (VWD) is a common inherited bleeding disorder. Patients with VWD suffering from severe bleeding may benefit from the use of secondary long-term prophylaxis. Aim Systematically summarize the evidence on the clinical outcomes of secondary long-term prophylaxis in patients with VWD and severe recurrent bleedings. Methods We searched Medline and EMBASE through October 2019 for relevant randomized clinical trials (RCTs) and comparative observational studies (OS) assessing the effects of secondary long-term prophylaxis in patients with VWD. We used Cochrane Risk of Bias (RoB) tool and the RoB for Non-Randomized Studies of interventions (ROBINS-I) tool to assess the quality of the included studies. We conducted random-effects meta-analyses and assessed the certainty of the evidence using the Grading of Recommendations Assessment, Development, and Evaluation (GRADE) approach. Results We included 12 studies. Evidence from one placebo controlled RCT suggested that VWD prophylaxis as compared to no prophylaxis reduced the rate of bleeding episodes (Rate ratio [RR], .24; 95% confidence interval [CI], .17–.35; low certainty evidence), and of epistaxis (RR, .38; 95%CI, .21–.67; moderate certainty evidence), and may increase serious adverse events RR 2.73 (95%CI .12–59.57; low certainty). Evidence from four before-and-after studies in which researchers reported comparative data suggested that VWD prophylaxis reduced the rate of bleeding (RR .34; 95%CI, .25–.46; very low certainty evidence). Conclusion VWD prophylaxis treatment seems to reduce the risk of spontaneous bleeding, epistaxis, and hospitalizations. More RCTs should be conducted to increase the certainty in these benefits.

Published

2022

6. Outcomes of long‐term von Willebrand factor prophylaxis use in von Willebrand disease: A systematic literature review.

Author

El Alayli, Abdallah, Brignardello Petersen, Romina, Husainat, Nedaa M., Kalot, Mohamad A., Aljabiri, Yazan, Turkmani, Hani, Britt, Alec, El‐Khechen, Hussein, Shahid, Shaneela, Roller, John, Motaghi, Shahrzad, Mansour, Razan, Tosetto, Alberto, Abdul‐Kadir, Rezan, Laffan, Michael, Weyand, Angela, Leebeek, Frank W.G., Arapshian, Alice, Kouides, Peter, and James, Paula

Subjects

VON Willebrand disease, VON Willebrand factor, PREVENTIVE medicine, HEREDITARY hemorrhagic telangiectasia, CLINICAL trials

Abstract

Background: Von Willebrand Disease (VWD) is a common inherited bleeding disorder. Patients with VWD suffering from severe bleeding may benefit from the use of secondary long‐term prophylaxis. Aim: Systematically summarize the evidence on the clinical outcomes of secondary long‐term prophylaxis in patients with VWD and severe recurrent bleedings. Methods: We searched Medline and EMBASE through October 2019 for relevant randomized clinical trials (RCTs) and comparative observational studies (OS) assessing the effects of secondary long‐term prophylaxis in patients with VWD. We used Cochrane Risk of Bias (RoB) tool and the RoB for Non‐Randomized Studies of interventions (ROBINS‐I) tool to assess the quality of the included studies. We conducted random‐effects meta‐analyses and assessed the certainty of the evidence using the Grading of Recommendations Assessment, Development, and Evaluation (GRADE) approach. Results: We included 12 studies. Evidence from one placebo controlled RCT suggested that VWD prophylaxis as compared to no prophylaxis reduced the rate of bleeding episodes (Rate ratio [RR],.24; 95% confidence interval [CI],.17–.35; low certainty evidence), and of epistaxis (RR,.38; 95%CI,.21–.67; moderate certainty evidence), and may increase serious adverse events RR 2.73 (95%CI.12–59.57; low certainty). Evidence from four before‐and‐after studies in which researchers reported comparative data suggested that VWD prophylaxis reduced the rate of bleeding (RR.34; 95%CI,.25–.46; very low certainty evidence). Conclusion: VWD prophylaxis treatment seems to reduce the risk of spontaneous bleeding, epistaxis, and hospitalizations. More RCTs should be conducted to increase the certainty in these benefits. [ABSTRACT FROM AUTHOR]

Published

2022

7. von Willebrand disease: proposing definitions for future research

Author

Connell, Nathan T., James, Paula D., Brignardello-Petersen, Romina, Abdul-Kadir, Rezan, Ameer, Barbara, Arapshian, Alice, Couper, Susie, Di Paola, Jorge, Eikenboom, Jeroen, Giraud, Nicolas, Grow, Jean M., Haberichter, Sandra, Jacobs-Pratt, Vicki, Konkle, Barbara A., Kouides, Peter, Laffan, Michael, Lavin, Michelle, Leebeek, Frank W.G., McLintock, Claire, McRae, Simon, Montgomery, Robert, O'Brien, Sarah H., O'Donnell, James S., Ozelo, Margareth C., Scappe, Nikole, Sidonio, Robert, Jr, Tosetto, Alberto, Weyand, Angela C., Kalot, Mohamad A., Husainat, Nedaa, Mustafa, Reem A., and Flood, Veronica H.

Published

2021

8. Methylation of conserved CpG sites neighboring the beta retinoic acid response element may mediate retinoic acid receptor beta gene silencing in MCF-7 breast cancer cells

Author

Arapshian, Alice, Kuppumbatti, Yuvarani S, and Mira-y-Lopez, Rafael

Published

2000

9. An international survey to inform priorities for new guidelines on von Willebrand disease.

Author

Kalot, Mohamad A., Al‐Khatib, Mohammed, Connell, Nathan T., Flood, Veronica, Brignardello‐Petersen, Romina, James, Paula, Mustafa, Reem A., Abdul‐Kadir, Rezan, Ameer, Barbara, Arapshian, Alice, Ozelo, Margareth C., Couper, Susie, Grow, Jean, Eikenboom, Jeroen, Giraud, Nicolas, Haberichter, Sandra, Jacobs‐Pratt, Vicki, Di Paola, Jorge, Konkle, Barbara A., and Kouides, Peter

Subjects

VON Willebrand disease, MEDICAL personnel, VON Willebrand factor, DIAGNOSIS, WOMEN patients, GUIDELINES

Abstract

Introduction: von Willebrand disease (VWD) is an inherited bleeding disorder caused by a quantitative or qualitative dysfunction of von Willebrand factor. Clinicians, patients and other stakeholders have many questions about the diagnosis and management of the disease. Aim: To identify topics of highest importance to stakeholders that could be addressed by guidelines to be developed by the American Society of Hematology (ASH), the International Society on Thrombosis and Haemostasis (ISTH), the National Hemophilia Foundation (NHF) and the World Federation of Hemophilia (WFH). Methods: A survey to determine and prioritize topics to be addressed in the collaborative development of guidelines for VWD was distributed to international stakeholders including patients, caregivers and healthcare providers (HCPs). Representatives of the four organizations coordinated the distribution strategy. The survey focused on both diagnosis and management of VWD, soliciting 7‐point Likert‐scale responses and open‐ended comments, in English, French and Spanish. We conducted descriptive analysis with comparison of results by stakeholder type, gender and countries' income classification for the rating questions and qualitative conventional content data analysis for the open‐ended responses. Results: A total of 601 participants responded to the survey (49% patients/caregivers and 51% healthcare providers). The highest priority topics identified were diagnostic criteria/classification, bleeding assessment tools and treatment options for women and surgical patients. In contrast, screening for anaemia and differentiating plasma‐derived therapy versus recombinant therapies received lower ratings. Conclusion: This survey highlighted areas of importance to a diverse representation of stakeholders in the diagnosis and management of VWD, providing a framework for future guideline development and implementation. [ABSTRACT FROM AUTHOR]

Published

2020

10. Epigenetic CRBP downregulation appears to be an evolutionarily conserved (human and mouse) and oncogene-specific phenomenon in breast cancer

Author

Arapshian Alice, Bertran Silvina, Kuppumbatti Yuvarani S, Nakajo Shigeo, and Mira-y-Lopez Rafael

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background The cellular retinol binding protein I gene (CRBP) is downregulated in a subset of human breast cancers and in MMTV-Myc induced mouse mammary tumors. Functional studies suggest that CRBP downregulation contributes to breast tumor progression. What is the mechanism underlying CRBP downregulation in cancer? Here we investigated the hypothesis that CRBP is epigenetically silenced through DNA hypermethylation in human and mouse breast cancer. Results Bisulfite sequencing of CRBP in a panel of 6 human breast cancer cell lines demonstrated that, as a rule, CRBP hypermethylation is closely and inversely related to CRBP expression and identified one exception to this rule. Treatment with 5-azacytidine, a DNA methyltransferase inhibitor, led to CRBP reexpression, supporting the hypothesis that CRBP hypermethylation is a proximal cause of CRBP silencing. In some cells CRBP reexpression was potentiated by co-treatment with retinoic acid, an inducer of CRBP, and trichostatin A, a histone deacetylase inhibitor. Southern blot analysis of a small panel of human breast cancer specimens identified one case characterized by extensive CRBP hypermethylation, in association with undetectable CRBP mRNA and protein. Bisulfite sequencing of CRBP in MMTV-Myc and MMTV-Neu/NT mammary tumor cell lines extended the rule of CRBP hypermethylation and silencing (both seen in MMTV-Myc but not MMTV-Neu/NT cells) from human to mouse breast cancer and suggested that CRBP hypermethylation is an oncogene-specific event. Conclusion CRBP hypermethylation appears to be an evolutionarily conserved and principal mechanism of CRBP silencing in breast cancer. Based on the analysis of transgenic mouse mammary tumor cells, we hypothesize that CRBP silencing in human breast cancer may be associated with a specific oncogenic signature.

Published

2004

11. Improved prevention of bleeding episodes with emicizumab in 3 patients with concomitant hemophilia A and von Willebrand disease.

Author

Ansteatt, Kristin T., Roberts, Jonathan C., Helms, Jackie M., and Tarantino, Michael D.

Published

2024

12. Retinoic acid receptor alpha2 is a growth suppressor epigenetically silenced in MCF-7 human breast cancer cells.

Author

Farias EF, Arapshian A, Bleiweiss IJ, Waxman S, Zelent A, and Mira-Y-Lopez R

Subjects

Breast Neoplasms metabolism, Carcinoma metabolism, Cell Division drug effects, Cell Division genetics, DNA Methylation drug effects, Enzyme Inhibitors pharmacology, Epithelial Cells drug effects, Epithelial Cells metabolism, Female, Gene Expression Regulation, Neoplastic drug effects, Gene Silencing drug effects, Genes, Tumor Suppressor drug effects, Humans, Promoter Regions, Genetic drug effects, Promoter Regions, Genetic genetics, Receptors, Retinoic Acid drug effects, Receptors, Retinoic Acid metabolism, Retinoic Acid Receptor alpha, Tretinoin pharmacology, Tumor Cells, Cultured, Breast Neoplasms genetics, Carcinoma genetics, Gene Expression Regulation, Neoplastic genetics, Gene Silencing physiology, Genes, Tumor Suppressor physiology, Receptors, Retinoic Acid genetics

Abstract

Retinoic acid (RA) receptor (RAR) beta2 has been shown to be underexpressed in human breast cancer cells, including MCF-7 cells, and recent reports have suggested that hypermethylation of the RAR beta2 promoter and 5'-UTR is the underlying cause. Here we show that RAR alpha2 is also underexpressed in MCF-7 breast cancer cells, at both the message and the protein level, relative to normal or nontumorigenic breast epithelial cells. Bisulfite sequencing of the CpG island in the RAR alpha2 promoter revealed highly penetrant and uniform cytosine methylation in MCF-7 cells. Pretreatment with the DNA methyltransferase inhibitor, azacytidine, followed by treatment with RA and a histone deacetylase inhibitor, trichostatin A, resulted in partial promoter demethylation and RAR alpha2 induction, which strongly suggested that promoter hypermethylation is responsible for RAR alpha2 underexpression. We compared the outcome of ectopic expression in MCF-7 cells of matched levels of RAR alpha2 and RAR beta2. On the basis of a clonogenic assay, RAR alpha2 displayed ligand-dependent growth-suppressive activity similar to that of RARb eta2; thus, 10 and 20 nM RA inhibited clonogenic growth by 52 and 80%, respectively, in RAR alpha2-transfected cells compared with 75 and 77%, respectively, in RAR beta2-transfected cells. We conclude that the silencing of the RAR alpha2 promoter by hypermethylation may play a contributory role in the dysregulation of RA signaling in mammary tumorigenesis.

Published

2002

13. Emicizumab for Severe Von Willebrand Disease (VWD) and VWD/Hemophilia A (BCDI-XII)

Author

Genentech, Inc. and Jonathan Roberts, Assistance Medical Director

Published

2023

14. RBP7 functions as a tumor suppressor in HR + breast cancer by inhibiting the AKT/SREBP1 pathway and reducing fatty acid.

Author

Yu, Yue, Xu, Zhihua, Zhou, Hao, Xu, Ruyan, Xu, Jia, Liu, Wenjun, Wu, Yuxin, Qiu, Yue, Zhang, Guangbo, Huang, Xue, and Chen, Yan

Subjects

FATTY acids, BREAST cancer, STAINS & staining (Microscopy), OLEIC acid, CELL proliferation

Abstract

Background: Increasing evidence proves that RBP7 plays a significant role in breast cancer (BC). The present study was aimed to investigate the mechanism of RBP7. Methods: Western Blotting and qRT-PCR were performed for evaluating the expression levels. CCK8, colony forming, xenograft mouse model, wound healing and transwell assays were conducted to examine cell ability of proliferation, invasion and migration. Nile red staining and Oil red O staining were used for testing the lipid. Results: RBP7 was related to overall survival (OS) in patients with HR + BC. RBP7 protein was significantly decreased in HR + BC tissues and cells. RBP7 suppressed HR + BC cell proliferation in vitro and in vivo, and inhibited migration and invasion. RBP7 reduced fatty acid in HR + BC cells by inhibiting the AKT/SREBP1 pathway. Conclusions: RBP7 may function as a tumor suppressor in HR + BC by inhibiting the AKT/SREBP1 pathway and reducing fatty acid. [ABSTRACT FROM AUTHOR]

Published

2024

15. Perioperative hemostasis management in patients with von Willebrand disease: an institutional experience.

Author

Toenges, Rosa, Miesbach, Wolfgang, Ludwig, Kaja, and Krammer-Steiner, Beate

Published

2024

16. Comprehensive comparison of global coagulation assays to differentiate lupus anticoagulant from acquired hemophilia A in patients with prolonged APTT.

Author

Chikasawa, Yushi, Amano, Kagehiro, Shinozawa, Keiko, Bingo, Masato, Miyashita, Ryui, Yamaguchi, Tomoko, Mitsuhashi, Ayano, Inaba, Hiroshi, Hagiwara, Takeshi, and Kinai, Ei

Abstract

There is no established method for differentiating acquired hemophilia A (AHA) from lupus anticoagulant (LA) positivity because both present with prolonged activated partial thromboplastin time. We compared various parameters of rotational thromboelastometry (ROTEM), thrombin generation assay (TGA), and clot waveform analysis (CWA) in patients with AHA (n = 10) and LA (n = 44). Compared with AHA, possible (n = 12) and definite (n = 32) LA showed significantly shorter clotting time (CT) in NATEM mode of ROTEM (> 3600 vs. 501/533). In TGA, peak height was significantly lower in AHA (16 vs. 242/174 nM). In CWA, CT was significantly longer (81 vs. 36/41 s) and Ad|min1| was lower (2.1 vs. 8.7/6.7) in AHA. Notably, CT by NATEM and peak height in TGA completely discriminated between AHA and LA, whereas Ad|min1| did not discriminate between them in 4 cases of AHA and 1 of LA. Comparison of 3 patients with both AHA and LA against a patient with only LA and markedly low FVIII activity (3.5%) showed that both CT by NATEM and peak height of TGA precisely classified the former 3 cases as AHA and the latter 1 case as LA, whereas Ad|min1| classified all 4 cases as AHA. ROTEM and TGA can comparably distinguish between AHA and LA. [ABSTRACT FROM AUTHOR]

Published

2023

17. Neurological Complications Associated with Hereditary Bleeding Disorders.

Author

Bhatti, Muhammad Qasim, Gonzalez-Fernandez, Ezekiel, Bhatia, Kunal, Divani, Afshin A., Di Napoli, Mario, Hinduja, Archana, and Datta, Yvonne H.

Abstract

Purpose of Review: Hereditary bleeding disorders may have a wide variety of clinical presentations ranging from mild mucosal and joint bleeding to severe central nervous system (CNS) bleeding, of which intracranial hemorrhage (ICH) is the most dreaded complication. In this review, we will discuss the pathophysiology of specific hereditary bleeding disorders, namely, hemophilia A, hemophilia B, and von Willebrand disease (vWD); their clinical manifestations with a particular emphasis on neurological complications; a brief overview of management strategies pertaining to neurological complications; and a review of literature guiding treatment strategies. Recent Findings: ICH is the most significant cause of morbidity and mortality in patients with hemophilia. Adequate control of bleeding with the administration of specific factors or blood products, identification of risk factors for bleeding, and maintaining optimal coagulant activity are essential for appropriately managing CNS bleeding complications in these patients. The administration of specific recombinant factors is tailored to a patient's pharmacokinetics and steady-state levels. During acute bleeding episodes, initial factor activity should be maintained between 80 and 100%. Availability of monoclonal antibody Emicizumab has revolutionized prophylactic therapies in patients with hemophilia. Management of ICH in patients with vWD involves using plasma-derived factor concentrates, recombinant von Willebrand factor, and supportive antifibrinolytic agents individualized to the type and severity of vWD. Summary: Hemophilia and vWD are the most common hereditary bleeding disorders that can predispose patients to life-threatening CNS complications—intracranial bleeds, intraspinal bleeding, and peripheral nerve syndromes. Early care coordination with a hematologist can help develop an effective prophylactic regimen to avoid life-threatening bleeding complications in these patients. Further research is needed to evaluate using emicizumab as an on-demand treatment option for acute bleeding episodes in patients with hemophilia. [ABSTRACT FROM AUTHOR]

Published

2023

18. The Contribution of Hippocampal All-Trans Retinoic Acid (ATRA) Deficiency to Alzheimer's Disease: A Narrative Overview of ATRA-Dependent Gene Expression in Post-Mortem Hippocampal Tissue.

Author

Almaguer, Joey, Hindle, Ashly, and Lawrence, J. Josh

Subjects

ALZHEIMER'S disease, GENE expression, TRETINOIN, RETINOIC acid receptors, HIPPOCAMPUS (Brain)

Abstract

There is accumulating evidence that vitamin A (VA) deficiency contributes to the pathogenesis and progression of Alzheimer's disease (AD). All-trans retinoic acid (ATRA), a metabolite of VA in the brain, serves distinct roles in the human hippocampus. Agonists of retinoic acid receptors (RAR), including ATRA, promote activation of the non-amyloidogenic pathway by enhancing expression of α-secretases, providing a mechanistic basis for delaying/preventing amyloid beta (Aβ) toxicity. However, whether ATRA is actually deficient in the hippocampi of patients with AD is not clear. Here, using a publicly available human transcriptomic dataset, we evaluated the extent to which ATRA-sensitive genes are dysregulated in hippocampal tissue from post-mortem AD brains, relative to age-matched controls. Consistent with ATRA deficiency, we found significant dysregulation of many ATRA-sensitive genes and significant upregulation of RAR co-repressors, supporting the idea of transcriptional repression of ATRA-mediated signaling. Consistent with oxidative stress and neuroinflammation, Nrf2 and NfkB transcripts were upregulated, respectively. Interestingly, transcriptional targets of Nrf2 were not upregulated, accompanied by upregulation of several histone deacetylases. Overall, our investigation of ATRA-sensitive genes in the human hippocampus bolsters the scientific premise of ATRA depletion in AD and that epigenetic factors should be considered and addressed as part of VA supplementation. [ABSTRACT FROM AUTHOR]

Published

2023

19. Von Willebrand Disease, Hemophilia, and Other Inherited Bleeding Disorders in Pregnancy.

Author

Pacheco, Luis D., Saade, George R., and James, Andra H.

Published

2023

20. The Vascular Endothelium and Coagulation: Homeostasis, Disease, and Treatment, with a Focus on the Von Willebrand Factor and Factors VIII and V.

Author

Pablo-Moreno, Juan A. De, Serrano, Luis Javier, Revuelta, Luis, Sánchez, María José, and Liras, Antonio

Subjects

VON Willebrand factor, VASCULAR endothelium, BLOOD coagulation factor VIII, DISSEMINATED intravascular coagulation, BLOOD coagulation factors, MONOCLONAL antibodies

Abstract

The vascular endothelium has several important functions, including hemostasis. The homeostasis of hemostasis is based on a fine balance between procoagulant and anticoagulant proteins and between fibrinolytic and antifibrinolytic ones. Coagulopathies are characterized by a mutation-induced alteration of the function of certain coagulation factors or by a disturbed balance between the mechanisms responsible for regulating coagulation. Homeostatic therapies consist in replacement and nonreplacement treatments or in the administration of antifibrinolytic agents. Rebalancing products reestablish hemostasis by inhibiting natural anticoagulant pathways. These agents include monoclonal antibodies, such as concizumab and marstacimab, which target the tissue factor pathway inhibitor; interfering RNA therapies, such as fitusiran, which targets antithrombin III; and protease inhibitors, such as serpinPC, which targets active protein C. In cases of thrombophilia (deficiency of protein C, protein S, or factor V Leiden), treatment may consist in direct oral anticoagulants, replacement therapy (plasma or recombinant ADAMTS13) in cases of a congenital deficiency of ADAMTS13, or immunomodulators (prednisone) if the thrombophilia is autoimmune. Monoclonal-antibody-based anti-vWF immunotherapy (caplacizumab) is used in the context of severe thrombophilia, regardless of the cause of the disorder. In cases of disseminated intravascular coagulation, the treatment of choice consists in administration of antifibrinolytics, all-trans-retinoic acid, and recombinant soluble human thrombomodulin. [ABSTRACT FROM AUTHOR]

Published

2022

21. Big picture initiatives in bleeding disorders.

Author

Rauch, Antoine, Valentino, Leonard A., Mills, Kevin, Witkop, Michelle L., Santaella, Maria E., DiMichele, Donna, Recht, Michael, and Susen, Sophie

Subjects

MEDICAL personnel, TRANSITION to adulthood, HEMORRHAGE, MENORRHAGIA

Abstract

Introduction: The inherited bleeding disorders (IBD) community has witnessed significant therapeutic advances recently, yet important gaps persist, particularly for those with rare disorders and historically underserved populations. Aims: ‐To create a national research blueprint agenda, led by the National Hemophilia Foundation (NHF), enhancing patient‐centric principles, accelerate research progress and address important gaps in care.‐To review critical gaps that remain to be addressed in women with IBDs, who face specific bleeding challenges. Methods: The NHF research blueprint research agenda was defined by input from across the community, including caregivers and patients who are considered subject matter experts of their IBD, research leaders, allied health professionals and specialists, and representatives of the biopharmaceutical industry. In addition, two medical experts in the field of IBDs performed a comprehensive review to address the knowledge gaps in women with IBDs. Results: Two foundational principles of the NHF blueprint are: (1) it must deliver on key issues that significantly impact the lives of those affected by IBDs, and (2) the priorities defined are relevant and actionable aimed to achieve health equity among all those affected by IBDs. A multidisciplinary approach is necessary for an optimal management of puberty, transition to adulthood and pregnancy. Even if strict guidelines are followed, recent studies show that women with IBDs are still facing a high burden. Conclusion: NHF blueprint will be issued in 2022. A specific research agenda is needed in women with IBDs to further improve their management and quality of life. [ABSTRACT FROM AUTHOR]

Published

2022

22. Management of a patient with acute myeloid leukaemia with a diagnosis of type 2 von Willebrand disease and a novel variant within the von Willebrand factor (VWF) gene.

Author

Dillon, James, Mykytiv, Vitaliy, Keenan, Catriona, Mullaney, Brendan, Orfali, Nina, Ryan, Kevin, Duggan, Cleona, and Crowley, Maeve P.

Subjects

VON Hippel-Lindau disease, VON Willebrand disease, ACUTE myeloid leukemia, VON Willebrand factor, DIAGNOSIS, MEDICAL societies

Abstract

International clinical practice guidelines for the treatment and prophylaxis of thrombosis associated with central venous catheters in patients with cancer. Von Willebrand disease (VWD) is the most frequently inherited bleeding disorder worldwide (prevalence: one in 10 000) with a bleeding phenotype ranging from minor mucosal bleeds to life-threatening haemorrhage.1 Treatment includes antifibrinolytic agents such as tranexamic acid and therapies that directly increase Von Willebrand factor (VWF) levels, such as desmopressin (DDAVP SP ® sp ) and VWF-containing concentrates.2 Acute myeloid leukaemia (AML) is a heterogenous haematological malignancy (annual incidence: five per 100 000). As this was a novel I VWF i variant, the patient's phenotype and VWF levels were used to estimate her bleeding risk and the treatment required. [Extracted from the article]

Published

2022

23. Successful Kidney Transplant for Nephropathic Cystinosis in a Patient with Von Willebrand Disease Type III: The First Case Report.

Author

Alsultan, Mohammad Khaled, Bdeir, Zeina Nizar, Hassan, Qussai, and Ali, Tahani

Subjects

VON Willebrand disease, KIDNEY transplantation, VON Willebrand factor, CHRONIC kidney failure, BLOOD coagulation factor VIII, BLOOD products

Abstract

Nephropathic cystinosis (NC) is a rare autosomal recessive disease, which causes cysteine-crystals accumulation with progression to end-stage renal disease (ESRD). Von willebrand disease (VWD) type III is a rare subtype of von willebrand factor (VWF) abnormality, which is characterized by severe reduction of VWF and factor VIII activity. A 16-year-old patient with NC and VWD type III presented with uremic symptoms due to ESRD. Dialysis access was inserted and followed by hemodialysis (HD) for 4 months with a proper infusion of blood products. While renal transplant remains the treatment of choice of NC and superior to chronic HD, bleeding complications were a major concern in this case with coexisting VWD type III. However, with the meticulous implementation of the Hematology team's daily recommendations, renal transplantation was successfully performed. This is the first case that mentions a new association between two inherited rare disorders, NC and VWD type III, and this entity has not been reported before. Moreover, successful kidney transplantation in our patient supports the possibility of these procedures in hereditary clotting disorders. [ABSTRACT FROM AUTHOR]

Published

2021

24. Untargeted metabolomics reveals multiple metabolites influencing smoking-related DNA methylation.

Author

Yunfeng Huang, Qin Hui, Walker, Douglas I., Uppal, Karan, Goldberg, Jack, Jones, Dean P., Vaccarino, Viola, and Sun, Yan V.

Published

2018

25. Commentary: surviving sexism in bleeding disorders affecting women.

Author

Sholzberg M and James PD

Subjects

Female, Humans, Sexism, Blood Coagulation Disorders, Hemorrhagic Disorders, Menorrhagia

Published

2022

26. Enhanced in Vitro Anti-Tumor Activity of 5-Azacytidine by Entrapment into Solid Lipid Nanoparticles.

Author

Jahanfar, Farhad, Hasani, Akbar, Shanebandi, Dariush, Rahmati, Mohammad, and Hamishehkar, Hamed

Subjects

NANOSTRUCTURED materials, NANOFABRICS, NANOPARTICLES manufacturing, AZACITIDINE, GENE expression

Abstract

Purpose: In this study the effectiveness of encapsulating of 5-azacytidine into the lipid nanoparticles was investigated and in vitro effect of encapsulated 5-azacytidine studied on MCF-7 cell lines Methods: 5-azacytidine-loaded solid lipid nanoparticles were produced by double emulsification (w/o/w) method by using stearic acid as lipid matrix, soy lecithin and poloxamer 407 as surfactant and co-surfactant respectively. Particle size, zeta potential, surface morphology, entrapment efficiency and kinetic of drug release were studied. In vitro effect of 5-azacytidine on MCF-7 cell line studied by MTT assay, DAPI staining, Rhodamine B relative uptake, and also Real time RT-PCR was performed for studying difference effect of free and encapsulated drug on expression of RARß2 gene. Results: The formulation F5 with 55.84±0.46 % of entrapment efficiency shows zero order kinetic of drug release and selected for in vitro studies; the cytotoxicity of free drug and encapsulated drug in 48 h of incubation have significant difference. DAPI staining shows morphology of apoptotic nucleus in both free and encapsulated drug, Rhodamine B labeled SLNs show time dependency and accumulation of SLNs in cytoplasm. Real time qRT-PCR doesn't show any significant difference (p>0.05) in expression of RARß2 gene in both cells treated with free or encapsulated drug. Conclusion: The results of the present study indicated that the entrapment of 5-azacytidine into SLNs enhanced its cytotoxicity performance and may pave a way for the future design of a desired dosage form for 5-azacytidine. [ABSTRACT FROM AUTHOR]

Published

2016

27. Altered RBP1 Gene Expression Impacts Epithelial Cell Retinoic Acid, Proliferation, and Microenvironment.

Author

Yu, Jianshi, Perri, Mariarita, Jones, Jace W., Pierzchalski, Keely, Ceaicovscaia, Natalia, Cione, Erika, and Kane, Maureen A.

Subjects

EPITHELIAL cells, TRETINOIN, GENE expression, STAINS & staining (Microscopy), EPITHELIUM, RETINOL-binding proteins

Abstract

Vitamin A is an essential diet-derived nutrient that has biological activity affected through an active metabolite, all-trans retinoic acid (atRA). Retinol-binding protein type 1 (RBP1) is an intracellular chaperone that binds retinol and retinal with high affinity, protects retinoids from non-specific oxidation, and delivers retinoids to specific enzymes to facilitate biosynthesis of RA. RBP1 expression is reduced in many of the most prevalent cancers, including breast cancer. Here, we sought to understand the relationship between RBP1 expression and atRA biosynthesis in mammary epithelial cells, as well as RBP1 expression and atRA levels in human mammary tissue. We additionally aimed to investigate the impact of RBP1 expression and atRA on the microenvironment as well as the potential for therapeutic restoration of RBP1 expression and endogenous atRA production. Using human mammary ductal carcinoma samples and a series of mammary epithelial cell lines representing different stages of tumorigenesis, we investigated the relationship between RBP1 expression as determined by QPCR and atRA via direct liquid chromatography-multistage-tandem mass spectrometry-based quantification. The functional effect of RBP1 expression and atRA in epithelial cells was investigated via the expression of direct atRA targets using QPCR, proliferation using Ki-67 staining, and collagen deposition via picrosirius red staining. We also investigated the atRA content of stromal cells co-cultured with normal and tumorigenic epithelial cells. Results show that RBP1 and atRA are reduced in mammary tumor tissue and tumorigenic epithelial cell lines. Knock down of RBP1 expression using shRNA or overexpression of RBP1 supported a direct relationship between RBP1 expression with atRA. Increases in cellular atRA were able to activate atRA direct targets, inhibit proliferation and inhibit collagen deposition in epithelial cell lines. Conditions encountered in tumor microenvironments, including low glucose and hypoxia, were able to reduce RBP1 expression and atRA. Treatment with either RARα agonist AM580 or demethylating agent Decitabine were able to increase RBP1 expression and atRA. Cellular content of neighboring fibroblasts correlated with the RA producing capacity of epithelial cells in co-culture. This work establishes a direct relationship between RBP1 expression and atRA, which is maintained when RBP1 expression is restored therapeutically. The results demonstrate diseases with reduced RBP1 could potentially benefit from therapeutics that restore RBP1 expression and endogenous atRA. [ABSTRACT FROM AUTHOR]

Published

2022

28. A clinically relevant bi-cellular murine mammary tumor model as a useful tool for evaluating the effect of retinoic acid signaling on tumor progression.

Author

Todaro, Laura, Veloso, María, Campodónico, Paola, Puricelli, Lydia, Farías, Eduardo, and Bal de Kier Joffé, Elisa

Abstract

Background: The effect of retinoic acid (RA) on breast cancer progression is controversial. Our objective was to obtain information about breast cancer progression, taking advantage of the ER-negative murine mammary adenocarcinoma model LM38 (LM38-LP constituted by luminal (LEP) and myoepithelial-like cells (MEP), LM38-HP mainly composed of spindle-shaped epithelial cells, and LM38-D2 containing only large myoepithelial cells), and to validate the role of the retinoic acid receptors (RARs) in each cell-type compartment. Materials and methods: We studied the expression and functionality of the RARs in LM38 cell lines. We analyzed cell growth and cell cycle distribution, apoptosis, the activity of proteases, motility properties, and expression of the molecules involved in these pathways. We also evaluated tumor growth and dissemination in vivo under retinoid treatment. Results: LM38 cell lines expressed most retinoic receptor isotypes that were functional. However, only the bi-cellular LM38-LP cells responded to retinoids by increasing RARβ2 and CRBP1 expression. The growth of LM38 cell sublines was inhibited by retinoids, first by inducing arrest in MEP cells, then apoptosis in LEP cells. Retinoids induced inhibitory effects on motility, invasiveness, and activity of proteolytic enzymes, mainly in the LM38-LP cell line. In in-vivo assays with the LM38-LP cell line, RA treatment impaired both primary tumor growth and lung metastases dissemination. Conclusion: These in-vivo and in-vitro results show that to achieve maximum effects of RA on tumor progression both the LEP and MEP cell compartments have to be present, suggesting that the interaction between the LEP and MEP cells is crucial to full activation of the RARs. [ABSTRACT FROM AUTHOR]

Published

2013

29. CrbpI regulates mammary retinoic acid homeostasis and the mammary microenvironment.

Author

Pierzchalski, Keely, Jianshi Yu, Norman, Victoria, and Kane, Maureen A.

Subjects

VITAMIN A, BREAST cancer, TRETINOIN, HOMEOSTASIS, RETINOIDS

Abstract

Cellular retinol-binding protein, type I (CrbpI), encoded by retinol-binding protein, type 1 (Rbp1), is a chaperone of vitamin A (retinol) that is epigenetically silenced in ~25% of human breast cancers. CrbpI delivers vitamin A to enzymes for metabolism into an active metabolite, all-trans retinoic acid (atRA), where atRA is essential to cell proliferation, apoptosis, differentiation, and migration. Here, we show the effect of CrbpI loss on mammary atRA homeostasis using the Rbp1-/- mouse model. Rbp1-/- mouse mammary tissue has disrupted retinoid homeostasis that results in 40% depleted endogenous atRA. CrbpI loss and atRA depletion precede defects in atRA biosynthesis enzyme expression. Compensation by CrbpIII as a retinoid chaperone does not functionally replace CrbpI. Mammary subcellular fractions isolated from Rbp1-/- mice have altered retinol dehydro- genase/reductase (Rdh) enzyme activity that results in 24-42% less atRA production. Rbp1-/- mammary tissue has epithelial hyperplasia, stromal hypercellularity, increased collagen, and increased oxidative stress characteristic of atRA deficiency and early tissue dysfunction that precedes tumor formation. Consistent with the findings from the Rbp1-/- mouse, tumorigenic epithelial cells lacking CrbpI expression produce 51% less atRA. Together, these data show that CrbpI loss disrupts atRA homeostasis in mammary tissue, resulting in microenvironmental defects similar to those observed at the early stages of tumorigenesis. [ABSTRACT FROM AUTHOR]

Published

2013

30. Exposures in early life: associations with DNA promoter methylation in breast tumors.

Author

Tao, M.-H., Marian, C., Shields, P. G., Potischman, N., Nie, J., Krishnan, S. S., Berry, D. L., Kallakury, B. V., Ambrosone, C., Edge, S. B., Trevisan, M., Winston, J., and Freudenheim, J. L.

Abstract

There is evidence that epigenetic changes occur early in breast carcinogenesis. We hypothesized that early-life exposures associated with breast cancer would be associated with epigenetic alterations in breast tumors. In particular, we examined DNA methylation patterns in breast tumors in association with several early-life exposures in a population-based case–control study. Promoter methylation of E-cadherin, p16 and RAR-β2 genes was assessed in archived tumor blocks from 803 cases with real-time methylation-specific PCR. Unconditional logistic regression was used for case–case comparisons of those with and without promoter methylation. We found no differences in the prevalence of DNA methylation of the individual genes by age at menarche, age at first live birth and weight at age 20. In case–case comparisons of premenopausal breast cancer, lower birth weight was associated with increased likelihood of E-cadherin promoter methylation (OR = 2.79, 95% CI, 1.15–6.82, for ⩽2.5 v. 2.6–2.9 kg); higher adult height with RAR-β2 methylation (OR = 3.34, 95% CI, 1.19–9.39, for ⩾1.65 v. <1.60 m); and not having been breastfed with p16 methylation (OR = 2.75, 95% CI, 1.14–6.62). Among postmenopausal breast cancers, birth order was associated with increased likelihood of p16 promoter methylation. Being other than first in the birth order was inversely associated with likelihood of ⩾1 of the three genes being methylated for premenopausal breast cancers, but positively associated with methylation in postmenopausal women. These results suggest that there may be alterations in methylation associated with early-life exposures that persist into adulthood and affect breast cancer risk. [ABSTRACT FROM PUBLISHER]

Published

2013

31. Efficacy of the dietary histone deacetylase inhibitor butyrate alone or in combination with vitamin A against proliferation of MCF-7 human breast cancer cells.

Author

Andrade, F. O., Nagamine, M. K., De Conti, A., Chaible, L. M., Fontelles, C. C., Jordão Junior, A. A., Vannucchi, H., Dagli, M. L. Z., Bassoli, B. K., Moreno, F. S., and Ong, T. P.

Published

2012

32. Hypermethylation of apoptotic genes as independent prognostic factor in neuroblastoma disease.

Author

Grau, Elena, Martinez, Francisco, Orellana, Carmen, Canete, Adela, Yañez, Yania, Oltra, Silvestre, Noguera, Rosa, Hernandez, Miguel, Bermúdez, Jose D., and Castel, Victoria

Published

2011

33. During hormone depletion or tamoxifen treatment of breast cancer cells the estrogen receptor apoprotein supports cell cycling through the retinoic acid receptor α1 apoprotein.

Author

Salazar, Marcela D, Ratnam, Maya, Patki, Mugdha, Kisovic, Ivana, Trumbly, Robert, Iman, Mohamed, and Ratnam, Manohar

Subjects

RETINOIC acid receptors, CELL receptors, ESTROGEN receptors, CELL cycle, CANCER cells, ESTROGEN antagonists, TRETINOIN, HORMONE receptor positive breast cancer

Abstract

Introduction: Current hormonal adjuvant therapies for breast cancer including tamoxifen treatment and estrogen depletion are overall tumoristatic and are severely limited by the frequent recurrence of the tumors. Regardless of the resistance mechanism, development and progression of the resistant tumors requires the persistence of a basal level of cycling cells during the treatment for which the underlying causes are unclear. Methods: In estrogen-sensitive breast cancer cells the effects of hormone depletion and treatment with estrogen, tamoxifen, all-trans retinoic acid (ATRA), fulvestrant, estrogen receptor α (ER) siRNA or retinoic acid receptor α (RARα) siRNA were studied by examining cell growth and cycling, apoptosis, various mRNA and protein expression levels, mRNA profiles and known chromatin associations of RAR. RARα subtype expression was also examined in breast cancer cell lines and tumors by competitive PCR. Results: Basal proliferation persisted in estrogen-sensitive breast cancer cells grown in hormone depleted conditioned media without or with 4-hydroxytamoxifen (OH-Tam). Downregulating ER using either siRNA or fulvestrant inhibited basal proliferation by promoting cell cycle arrest, without enrichment for ErbB2/3+ overexpressing cells. The basal expression of RARα1, the only RARα isoform that was expressed in breast cancer cell lines and in most breast tumors, was supported by apo-ER but was unaffected by OH-Tam; RAR-β and -γ were not regulated by apo-ER. Depleting basal RARα1 reproduced the antiproliferative effect of depleting ER whereas its restoration in the ER depleted cells partially rescued the basal cycling. The overlapping tamoxifen-insensitive gene regulation by apo-ER and apo-RARα1 comprised activation of mainly genes promoting cell cycle and mitosis and suppression of genes involved in growth inhibition; these target genes were generally insensitive to ATRA but were enriched in RAR binding sites in associated chromatin regions. Conclusions: In hormone-sensitive breast cancer, ER can support a basal fraction of S-phase cells (i) without obvious association with ErbB2/3 expression, (ii) by mechanisms unaffected by hormone depletion or OH-Tam and (iii) through maintenance of the basal expression of apo-RARα1 to regulate a set of ATRA-insensitive genes. Since isoform 1 of RARα is genetically redundant, its targeted inactivation or downregulation should be further investigated as a potential means of enhancing hormonal adjuvant therapy. [ABSTRACT FROM AUTHOR]

Published

2011

34. Retinoids regulate stem cell differentiation.

Author

Gudas, Lorraine J. and Wagner, John A.

Subjects

RETINOIDS, MOLECULAR cell differentiation, STEM cells, CELL communication, TRANSCRIPTION factors, GENE expression, TRETINOIN, VITAMIN A

Abstract

Retinoids are ubiquitous signaling molecules that influence nearly every cell type, exert profound effects on development, and complement cancer chemotherapeutic regimens. All-trans retinoic acid (RA) and other active retinoids are generated from vitamin A (retinol), but key aspects of the signaling pathways required to produce active retinoids remain unclear. Retinoids generated by one cell type can affect nearby cells, so retinoids also function in intercellular communication. RA induces differentiation primarily by binding to RARs, transcription factors that associate with RXRs and bind RAREs in the nucleus. Binding of RA: (1) initiates changes in interactions of RAR/RXRs with co-repressor and co-activator proteins, activating transcription of primary target genes; (2) alters interactions with proteins that induce epigenetic changes; (3) induces transcription of genes encoding transcription factors and signaling proteins that further modify gene expression (e.g., FOX03A, Hoxa1, Sox9, TRAIL, UBE2D3); and (4) results in alterations in estrogen receptor α signaling. Proteins that bind at or near RAREs include Sin3a, N-CoR1, PRAME, Trim24, NRIP1, Ajuba, Zfp423, and MN1/TEL. Interactions among retinoids, RARs/RXRs, and these proteins explain in part the powerful effects of retinoids on stem cell differentiation. Studies of this retinol signaling cascade enhance our ability to understand and regulate stem cell differentiation for therapeutic and scientific purposes. In cancer chemotherapeutic regimens retinoids can promote tumor cell differentiation and/or induce proteins that sensitize tumors to drug combinations. Mechanistic studies of retinoid signaling continue to suggest novel drug targets and will improve therapeutic strategies for cancer and other diseases, such as immune-mediated inflammatory diseases. J. Cell. Physiol. 226: 322-330, 2011. © 2010 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2011

35. Quantitative analysis of promoter methylation in exfoliated epithelial cells isolated from breast milk of healthy women.

Published

2010

36. Epigenetic alterations in disseminated neuroblastoma tumour cells: influence of TMS1 gene hypermethylation in relapse risk in NB patients.

Author

Grau, E., Martinez, F., Orellana, C., Canete, A., Yañez, Y., Oltra, S., Noguera, R., Hernandez, M., Bermúdez, J. D., and Castel, V.

Subjects

NEUROBLASTOMA, NERVOUS system tumors, CANCER cells, CANCER relapse, BONE marrow

Abstract

Most neuroblastoma patients over 18 months of age at diagnosis present disseminated disease. The presence of neuroblastoma cells in bone marrow can be used to evaluate the response to treatment. It is possible that alterations in certain tumour cells might confer a selective advantage over tumour dissemination process, and probably be helpful in the clonal selection of tumour-specific cells that could originate metastasis. We performed real-time quantitative PCR to identify the presence of disseminated tumour cells in bone marrow samples, and we used MSP to analyse the methylation profile of 20 genes putatively implied in dissemination. We described epigenetic alterations in the methylated status of certain genes in disseminated tumour cells from bone marrow. Those cases with high rate of hypermethylation showed an increased probability of relapse during or after treatment. We found significantly poor prognosis in event-free survival in cases with hypermethylation of TMS1, MGMT and RARβ2 genes. We could not confirm the presence of a specific methylation profile in disseminated neuroblastoma tumour cells, but a high accumulation of epigenetic events in those cells is associated with a high risk of relapse, independently of MYCN amplification. [ABSTRACT FROM AUTHOR]

Published

2010

37. Familial and racial determinants of tumour suppressor genes promoter hypermethylation in breast tissues from healthy women.

Author

Dumitrescu, R.G., Marian, C., Krishnan, S. S., Spear, S. L., Kallakury, B. V.S ., Perry, D. J., Convit, J. R., Seillier-Moiseiwitsch, F., Yang, Y., Freudenheim, J. L., and Shields, P. G.

Subjects

CANCER in women, BREAST cancer, MAMMAPLASTY, METHYLATION, AFRICAN Americans, EUROPEAN Americans

Abstract

To determine the hypermethylation status of the promoter regions of tumour suppressor genes in breast tissues from healthy women and identify the determinants of these epigenetic changes. Questionnaires and breast tissues were collected from healthy women without a history of cancer and undergoing reduction mammoplasty ( N= 141). Methylation for p16INK4, BRCA1, ERα and RAR-β promoter regions from breast tissues were determined by methylation specific PCR. Associations were examined with chi-square and Fisher’s exact test as well as logistic regression. All statistical tests were two-sided. p16INK4, BRCA1, ERα and RAR-β hypermethylation were identified in 31%, 17%, 9% and 0% of the women, respectively. Women with BRCA1 hypermethylation had an eight-fold increase in the risk of ERα hypermethylation ( P= 0.007). p16INK4 hypermethylation was present in 28% of African-Americans, but 65% in European-Americans ( P= 0.02). There was an increased likelihood of p16INK4 or BRCA1 hypermethylation for women with family history of cancer (OR 2.3; 95%CI: 1.05–4.85 and OR 5.0; 95%CI: 1.55–15.81, respectively). ERα hypermethylation was associated with family history of breast cancer (OR 6.6; 95%CI: 1.58–27.71). After stratification by race, p16INK4 in European-Americans and BRCA1 hypermethylation in African-Americans were associated with family history of cancer (OR 3.8; 95%CI: 1.21–12.03 and OR 6.5; 95%CI: 1.33–31.32, respectively). Gene promoter hypermethylation was commonly found in healthy breast tissues from women without cancer, indicating that these events are frequent and early lesions. Race and family history of cancer increase the likelihood of these early events. [ABSTRACT FROM AUTHOR]

Published

2010

38. Hypermethylation of HLA class I gene is associated with HLA class I down-regulation in human gastric cancer.

Author

Ye, Q., Shen, Y., Wang, X., Yang, J., Miao, F., Shen, C., and Zhang, J.

Subjects

CANCER patients, POLYMERASE chain reaction, HLA histocompatibility antigens, CANCER cells, METHYLATION

Abstract

Abstract Down-regulated expression of human leukocyte antigen (HLA) class I molecules in many human cancers facilitate tumor cells to escape from immune attack. Promoter hypermethylation, one of the major epigenetic changes responsible for gene inactivation, plays an important role in gastric carcinogenesis. This study evaluated the expression and alteration of HLA class I molecules in a panel of 47 pairs of gastric cancer specimens with their noncancerous parts from Chinese patients by using immunohistochemistry (IHC), reverse transcription polymerase chain reaction (RT-PCR) and methylation-specific PCR (MSP) analysis. The expression of HLA-A, HLA-B/C and HLA class I complex was lost or down-regulated in human gastric cancer. The percentage of promoter methylation was 59.57% for HLA-A gene, 55.32% for HLA-B gene and 48.94% for HLA-C gene in gastric cancer, while it was decreased to 19.15%, 12.77% and 6.38% in the adjacent nontumor tissues, respectively. Seven of 10 (70%), 4 of 6 (66.7%) and 3 of 4 (75%) gastric cancer specimens with promoter hypermethylation at HLA-A, -B and -C loci showed transcriptional inactivation of HLA-A,- B and - C genes, suggesting an association between promoter hypermethylation and down-regulated expression of HLA class I molecules. Human gastric cancer cell line BGC-823 showed HLA-A down-regulation with promoter methylation of HLA-A locus. Treatment with DNA methyltransferase inhibitor restored the expression of HLA-A mRNA and surface HLA-A complex. Thus, our results showed that promoter hypermethylation might be one of the mechanisms that lead to HLA class I antigen down-regulation in gastric cancer. [ABSTRACT FROM AUTHOR]

Published

2010

39. Epigenetic modulation of the retinoid X receptor α by green tea in the azoxymethane- Apc Min/+ mouse model of intestinal cancer.

Author

Volate, Suresh R., Muga, Stephanie J., Issa, Ala Y., Nitcheva, Daniela, Smith, Theresa, and Wargovich, Michael J.

Published

2009

40. Metabolism and regulation of gene expression by 4-oxoretinol versus all-trans retinoic acid in normal human mammary epithelial cells.

Author

LIU, LIMIN, DERGUINI, FADILA, and GUDAS, LORRAINE J.

Subjects

TRETINOIN, RETINOIDS, GENE expression, CELL metabolism, PHARMACOLOGY, ADRENERGIC receptors, CYTOLOGY

Abstract

We previously demonstrated that 4-oxoretinol (4-oxo-ROL) activated retinoic acid receptors (RARs) in F9 stem cells. We showed that 4-oxo-ROL inhibited the proliferation of normal human mammary epithelial cells (HMECs). To understand the mechanisms by which 4-oxo-ROL regulates HMEC growth we examined gene expression profiles following 4-oxo-ROL or all-trans retinoic acid (tRA). We also compared growth inhibition by tRA, 4-oxo-ROL, or 4-oxo-RA. All three retinoids inhibited HMEC proliferation. Gene expression analyses indicated that 4-oxo-ROL and tRA modulated gene expression in closely related pathways. The expression of many genes, e.g. ATP-binding cassette G1 (ABCG1); adrenergic receptorβ2 (ADRB2); ras-related C3 botulinum toxin substrate (RAC2); and short-chain dehydrogenase/reductase 1 gene (SDR1) was changed after 4-oxo-ROL or tRA. Metabolism of these retinoids was analyzed by high-performance liquid chromatography (HPLC). In 1 µM tRA treated HMECs all of the tRA was found intracellularly, and tRA was the predominant intracellular retinoid. In 1 µM 4-oxo-ROL treated HMECs most 4-oxo-ROL was esterified to 4-oxoretinyl esters, no tRA was detected, and 4-oxo-ROL and 4-oxo-RA were observed intracellularly. In 1 µM 4-oxoretinoic acid (4-oxo-RA) treated HMECs little intracellular 4-oxo-RA was detected; most 4-oxo-RA was in the medium. Our results indicate that: (a) 4-oxo-ROL regulates gene expression and inhibits proliferation of HMECs; (b) 4-oxo-ROL and tRA regulate some of the same genes; (c) more tRA is found in cells, as compared to 4-oxoretinoic acid, when each drug is added at the same concentration in the medium; and (d) the mechanism by which 4-oxo-ROL exerts its biological activity does not involve intracellular tRA production. J. Cell. Physiol. 220: 771–779, 2009. © 2009 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

41. Signalling with retinoids in the human lung: validation of new toolsfor the expression study of retinoid receptors.

Published

2009

42. Chmp 1A is a mediator of the anti-proliferative effects of All-trans Retinoic Acid in human pancreatic cancer cells.

Author

Jing Li, Orr, Brandon, White, Kayla, Belogortseva, Natalia, Niles, Richard, Boskovic, Goran, Nguyen, Hanh, Dykes, Ava, and Park, Maiyon

Subjects

PROTEINS, CHROMATIN, CANCER cells, PANCREATIC diseases, GENE silencing

Abstract

Background: We recently have shown that Charged multivesicular protein/Chromatin modifying protein1A (Chmp1A) functions as a tumor suppressor in human pancreatic tumor cells. Pancreatic cancer has the worst prognosis of all cancers with a dismal 5-year survival rate. Preclinical studies using ATRA for treating human pancreatic cancer suggest this compound might be useful for treatment of pancreatic cancer patients. However, the molecular mechanism by which ATRA inhibits growth of pancreatic cancer cells is not clear. The objective of our study was to investigate whether Chmp1A is involved in ATRA-mediated growth inhibition of human pancreatic tumor cells. Results: We performed microarray studies using HEK 293T cells and discovered that Chmp1A positively regulated Cellular retinol-binding protein 1 (CRBP-1). CRBP-1 is a key regulator of All-trans retinoic acid (ATRA) through ATRA metabolism and nuclear localization. Since our microarray data indicates a potential involvement of Chmp1A in ATRA signaling, we tested this hypothesis by treating pancreatic tumor cells with ATRA in vitro. In the ATRA-responsive cell lines, ATRA significantly increased the protein expression of Chmp1A, CRBP-1, P53 and phospho-P53 at serine 15 and 37 position. We found that knockdown of Chmp1A via shRNA abolished the ATRA-mediated growth inhibition of PanC-1 cells. Also, Chmp1A silencing diminished the increase of Chmp1A, P53 and phospho-P53 protein expression induced by ATRA. In the ATRA non-responsive cells, ATRA did not have any effect on the protein level of Chmp1A and P53. Chmp1A over-expression, however, induced growth inhibition of ATRA non-responsive cells, which was accompanied by an increase of Chmp1A, P53 and phospho-P53. Interestingly, in ATRA responsive cells Chmp1A is localized to the nucleus, which became robust upon ATRA treatment. In the ATRA-non-responsive cells, Chmp1A was mainly translocated to the plasma membrane upon ATRA treatment. Conclusion: Collectively our data provides evidence that Chmp1A mediates the growth inhibitory activity of ATRA in human pancreatic cancer cells via regulation of CRBP-1. Our results also suggest that nuclear localization of Chmp1A is important in mediating ATRA signaling. [ABSTRACT FROM AUTHOR]

Published

2009

43. Allelic methylation bias of the RARB2 tumor suppressor gene promoter in cancer.

Author

Pappas, Jane J., Toulouse, André, Hébert, Josée, Fetni, Raouf, and Bradley, W. E. C.

Published

2008

44. Biomarker and animal models for assessment of retinoid efficacy in cancer chemoprevention.

Author

Niles, Richard M.

Subjects

VITAMIN A, CANCER, CHEMOPREVENTION, CANCER prevention, LUNG cancer, DNA

Abstract

Vitamin A is essential for normal growth and development. Epidemiology and laboratory studies suggest that decreased vitamin A levels and defective metabolism/action may contribute to the genesis of certain cancers. Based on this information, natural and synthetic derivatives of vitamin A (retinoids) have been used for chemoprevention of cancer. Retinoids have had some success in the chemoprevention of leukoplakia and in the decreased incidence of second primaries in head and neck cancer. There is little information on biomarkers that can be used to assess the efficacy of the chemopreventive activity of retinoids. The ability of retinoids to induce RARb has been consistently shown to correlate with the response of cells and tissues to retinoic acid, but few other biomarkers have been certified as indicators of retinoid activity. In light of the failure of the ATBC and CARET clinical intervention trials for chemoprevention of lung cancer, greater use of animal models for chemoprevention studies is necessary. The potential combination of phytochemicals that inhibit DNA methyltransferase activity with retinoids holds promise for more effective chemoprevention of retinoid-unresponsive premalignant lesions. [ABSTRACT FROM AUTHOR]

Published

2007

45. The Ki67+ proliferation index correlates with increased cellular retinol-binding protein-1 and the coordinated loss of plakophilin-1 and desmoplakin during progression of cervical squamous lesions.

Author

Schmitt-Graeff, A, Koeninger, A, Olschewski, M, Haxelmans, S, Nitschke, R, Bochaton-Piallat, M-L, Lifschitz-Mercer, B, Gabbiani, G, Langbein, L, and Czernobilsky, B

Subjects

CARRIER proteins, VITAMIN A, SQUAMOUS cell carcinoma, PAPILLOMAVIRUSES, DESMOSOMES, MEDICAL research

Abstract

Aims: To investigate the modulation of cellular retinol-binding protein (CRBP)-1 and the desmosomal plaque proteins plakophilin (PKP)-1 and desmoplakin (DP) in correlation with the Ki67+ proliferation index (PI) during the progression of cervical squamous intraepithelial lesions (SIL) to squamous cell carcinoma (SCC). Methods: Using in situ imaging by brightfield and confocal laser scanning microscopy, the expression of CRBP-1 protein and transcripts, PKP-1, DP and the Ki67 PI were analysed in 38 low-grade (L) SIL, 56 high-grade (H) SIL, 49 SCC, 30 control cervices and 10 human papillomavirus-positive condylomatous lesions. Results: CRBP-1+ cells increased from 11.4% in the normal cervix to 80.3% in LSILs, 92.3% in HSILs and slightly decreased to 78.3% in invasive SCCs ( P = 0.0001) in close association with the Ki67 PI ( r =0.41; P < 0.0001). PKP-1+ and DP+ cells were correlated (0.32; P < 0.0001) and decreased from normal (81% versus 92.3%) to LSIL (53.1% versus 85.3%), to HSIL (46.4% versus 67.5%) and SCC (35.1% versus 35.9%). The Ki67+ PI was inversely correlated with DP (−0.20, P = 0.0014) and PKP-1 (−0.19, P = 0.015). Condylomata retained low CRBP-1 and high expression of PKP-1 and DP. Conclusions: The gain of CRBP-1 and the loss of desmosomal proteins occur early in cervical carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2007

46. Novel retinoic acid metabolism blocking agents have potent inhibitory activities on human breast cancer cells and tumour growth.

Author

Patel, J. B., Mehta, J., Belosay, A., Sabnis, G., Khandelwal, A., Brodie, A. M. H., Soprano, D. R., and Njar, V. C. O.

Subjects

TRETINOIN, NEOVASCULARIZATION, CELL proliferation, APOPTOSIS, ESTROGEN, XENOGRAFTS, PROTEIN analysis, PROTEIN metabolism, ANIMAL experimentation, ANTINEOPLASTIC agents, BREAST tumors, CELL cycle, CELL physiology, CELL receptors, COMPARATIVE studies, IMIDAZOLES, RESEARCH methodology, MEDICAL cooperation, MICE, RESEARCH, RETINOIDS, EVALUATION research, PHARMACODYNAMICS

Abstract

Antitumour effects of retinoids are attributed to their influence on cell proliferation, differentiation, apoptosis and angiogenesis. In our effort to develop useful agents for breast cancer therapy, we evaluated the effects of four representative retinoic acid metabolism blocking agents (RAMBAs, VN/14-1, VN/50-1, VN/66-1 and VN/69-1) on growth inhibition of oestrogen receptor positive (ER +ve, MCF-7 and T-47D) and oestrogen receptor negative (ER −ve, MDA-MB-231) human breast cancer cells. Additionally, we investigated the biological effects/molecular mechanism(s) underlying their growth inhibitory properties as well as their antitumour efficacies against MCF-7 and MCF-7Ca tumour xenografts in nude mice. We also assessed the effect of combining VN/14-1 and all-trans-retinoic acid (ATRA) on MCF-7 tumuor xenografts. The ER +ve cell lines were more sensitive (IC50 values between 3.0 and 609 nM) to the RAMBAs than the ER −ve MDA-MB-231 cell line (IC50=5.6–24.0 μM). Retinoic acid metabolism blocking agents induced cell differentiation as determined by increased expression of cytokeratin 8/18 and oestrogen receptor-α (ER-α). Similar to ATRA, they also induced apoptosis via activation of caspase 9. Cell cycle analysis indicated that RAMBAs arrested cells in the G1 and G2/M phases and caused significant downregulation (>80%) of cyclin D1 protein. In vivo, the growth of MCF-7 mammary tumours was dose-dependently and significantly inhibited (92.6%, P<0.0005) by VN/14-1. The combination of VN/14-1 and ATRA also inhibited MCF-7 breast tumour growth in vivo (up to 120%) as compared with single agents (P<0.025). VN/14-1 was also very effective in preventing the formation of MCF-7Ca tumours and it significantly inhibited the growth of established MCF-7Ca tumours, being as effective as the clinically used aromatase inhibitors, anastrozole and letrozole. Decrease in cyclin D1 and upregulation of cytokeratins, Bad and Bax with VN/14-1 may be responsible for the efficacy of this compound in inhibiting breast cancer cell growth in vitro and in vivo. Our results suggest that our RAMBAs, especially VN/14-1 may be useful novel therapy for breast cancer.British Journal of Cancer (2007) 96, 1204–1215. doi:10.1038/sj.bjc.6603705 www.bjcancer.com Published online 27 March 2007 [ABSTRACT FROM AUTHOR]

Published

2007

47. The effect of body weight on altered expression of nuclear receptors and cyclooxygenase-2 in human colorectal cancers.

Author

Delage, Barbara, Rullier, Anne, Capdepont, Maylis, Rullier, Eric, and Cassand, Pierrette

Subjects

BODY weight, NUCLEAR receptors (Biochemistry), CYCLOOXYGENASE 2, COLON cancer, OBESITY, EPIDEMIOLOGY

Abstract

Background: Epidemiological studies on risk factors for colorectal cancer (CRC) have mainly focused on diet, and being overweight is now recognized to contribute significantly to CRC risk. Overweight and obesity are defined as an excess of adipose tissue mass and are associated with disorders in lipid metabolism. Peroxisome proliferator-activated receptors (PPARs) and retinoid-activated receptors (RARs and RXRs) are important modulators of lipid metabolism and cellular homeostasis. Alterations in expression and activity of these ligand-activated transcription factors might be involved in obesity-associated diseases, which include CRC. Cyclooxygenase-2 (COX-2) also plays a critical role in lipid metabolism and alterations in COX-2 expression have already been associated with unfavourable clinical outcomes in epithelial tumors. The objective of this study is to examine the hypothesis questioning the relationship between alterations in the expression of nuclear receptors and COX-2 and the weight status among male subjects with CRC. Method: The mRNA expression of the different nuclear receptor subtypes and of COX-2 was measured in 20 resected samples of CRC and paired non-tumor tissues. The association between expression patterns and weight status defined as a body mass index (BMI) was statistically analyzed. Results: No changes were observed in PPARγ mRNA expression while the expression of PPARδ, retinoid-activated receptors and COX-2 were significantly increased in cancer tissues compared to normal colon mucosa (P ≤ 0.001). The weight status appeared to be an independent factor, although we detected an increased level of COX-2 expression in the normal mucosa from overweight patients (BMI ≥ 25) compared to subjects with healthy BMI (P = 0.002). Conclusion: Our findings show that alterations in the pattern of nuclear receptor expression observed in CRC do not appear to be correlated with patient weight status. However, the analysis of COX-2 expression in normal colon mucosa from subjects with a high BMI suggests that COX-2 deregulation might be driven by excess weight during the colon carcinogenesis process. [ABSTRACT FROM AUTHOR]

Published

2007

48. Cellular retinol binding protein-1 expression in endometrial hyperplasia and carcinoma: diagnostic and possible therapeutic implications.

Author

Orlandi, Augusto, Ferlosio, Amedeo, Ciucci, Alessandro, Francesconi, Arianna, Lifschitz-Mercer, Beatriz, Gabbiani, Giulio, Spagnoli, Luigi G, and Czernobilsky, Bernard

Published

2006

49. Promoter methylation reduces C/EBPδ (CEBPD) gene expression in the SUM-52PE human breast cancer cell line and in primary breast tumors.

Author

D. Tang, G.S. Sivko, and J.W. DeWille

Abstract

CCAAT/Enhancer Binding Proteins (C/EBPs) are a highly conserved family of leucine zipper proteins that regulate cell growth and differentiation. C/EBPδ functions in the initiation and maintenance of mammary epithelial cell G0 growth arrest and ‘loss of function’ alterations in C/EBPδ gene expression have been reported in human breast cancer and in rodent carcinogen-induced mammary tumors. The molecular mechanism underlying reduced C/EBPδ gene expression in mammary tumorigenesis, however, is unknown. In this report we demonstrate that C/EBPδ gene expression is undetectable in the SUM-52PE human breast cancer cell line and that silencing of SUM-52PE C/EBPδ gene expression is due to epigenetic promoter hypermethylation (26/27 CpGs methylated). The hypermethylated SUM-52PE C/EBPδ gene promoter is associated with reduced levels of acetylated Histone H4, consistent with a closed, transcriptionally inactive chromatin conformation. Treatment with 5′-aza-cytidine and trichostatin A (TSA) re-activates cytokine-induced SUM-52PE C/EBPδ gene expression. C/EBPδ gene expression is reduced to virtually undetectable levels in 32% (18/57) of primary human breast tumors. Site-specific CpG methylation was observed in 33% (6/18) of the low C/EBPδ expressing primary breast tumors. CpG methylation adjacent to the C/EBPδ proximal promoter Sp1 site was associated with reduced C/EBPδ expression in a primary breast cancer sample. Electromobility shift assays (EMSA) demonstrated a significant reduction in binding to oligos containing the CpG methylation 5′ to the Sp1 binding site. These results demonstrate a direct link between C/EBPδ gene promoter hyper- and site specific-methylation and reduced C/EBPδ gene expression in breast cancer cell lines and primary breast tumors. [ABSTRACT FROM AUTHOR]

Published

2006

50. Dominant negative retinoic acid receptor initiates tumor formation in mice.

Author

Kupumbati, Tara S., Cattoretti, Giorgio, Marzan, Christine, Farias, Eduardo F., Taneja, Reshma, and Mira-y-Lopez, Rafael

Subjects

TRETINOIN, TUMOR growth, ONCOGENIC viruses, LYMPHOMAS, MICE, CANCER research

Abstract

Background: Retinoic acid suppresses cell growth and promotes cell differentiation, and pharmacological retinoic acid receptor (RAR) activation is anti-tumorigenic. This begs the question of whether chronic physiological RAR activation by endogenous retinoids is likewise antitumorigenic. Results: To address this question, we generated transgenic mice in which expression of a ligand binding defective dominant negative RARá (RARáG303E) was under the control of the mouse mammary tumor virus (MMTV) promoter. The transgene was expressed in the lymphoid compartment and in the mammary epithelium. Observation of aging mice revealed that transgenic mice, unlike their wild type littermates, developed B cell lymphomas at high penetrance, with a median latency of 40 weeks. MMTV-RARáG303E lymphomas were high grade Pax-5+, surface H+L Ig negative, CD69+ and BCL6- and cytologically and phenotypically resembled human adult high grade (Burkitt's or lymphoblastic) lymphomas. We postulated that mammary tumors might arise after a long latency period as seen in other transgenic models of breast cancer. We tested this idea by transplanting transgenic epithelium into the cleared fat pads of wild type hosts, thus bypassing lymphomagenesis. At 17 months post-transplantation, a metastatic mammary adenocarcinoma developed in one of four transplanted glands whereas no tumors developed in sixteen of sixteen endogenous glands with wild type epithelium. Conclusion: These findings suggest that physiological RAR activity may normally suppress B lymphocyte and mammary epithelial cell growth and that global RAR inactivation is sufficient to initiate a stochastic process of tumor development requiring multiple transforming events. Our work makes available to the research community a new animal resource that should prove useful as an experimental model of aggressive sporadic lymphoma in immunologically uncompromised hosts. We anticipate that it may also prove useful as a model of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2006