Your search keyword '"Athalia Klein"' showing total 29 results

1. Oral mixture of autologous colon-extracted proteins for the Crohn’s disease: A double-blind trial

Author

Eran Goldin, Eran Israeli, Nilla Hemed, Gadi Lalazar, Yaron Ilan, Ehud Zigmond, and Athalia Klein

Subjects

Adult, Male, medicine.medical_specialty, Pathology, Time Factors, Colon, Administration, Oral, Cell Separation, Gastroenterology, Severity of Illness Index, Immune tolerance, Double blind, Remission induction, Young Adult, Crohn Disease, Double-Blind Method, T-Lymphocyte Subsets, Internal medicine, Cell separation, medicine, Immune Tolerance, Humans, Israel, Oral tolerance, Immunity, Mucosal, Crohn's disease, Crohn disease, business.industry, Remission Induction, Proteins, General Medicine, Immune modulation, Middle Aged, medicine.disease, Flow Cytometry, digestive system diseases, stomatognathic diseases, Treatment Outcome, Desensitization, Immunologic, Randomized Controlled Trial, Female, business

Abstract

To evaluate the safety and efficacy of oral administration of Alequel™, an autologous protein-containing colon extract.A total of 43 patients were enrolled in a randomized, placebo-controlled, double-blind trial. Patients were orally administered with autologous protein-containing colon extract three doses of autologous study drug per week for 15 wk, for a total of 45 doses. Patients were followed for safety parameters. Remission was defined as a Crohn's disease activity index (CDAI) score of less than or equal to 150. All patients were followed for changes in subsets of T cells by fluorescence-activated cell sorting analysis.Analysis was performed on a total number of evaluable patients of 14 in the study drug group and 15 in the placebo group. Treatment was well tolerated by all patients. No major treatment-related adverse events were reported or observed in any of the treated patients during the feeding or follow-up periods. Between weeks 6 and 9 of the study, six of the 14 (43%) evaluable subjects who received the study drug achieved a CDAI of 150 or lower. In contrast, five of the 15 (33%) evaluable subjects in the placebo group achieved remission. Between weeks 9 and 12, the remission rates were 50% and 33% for the drug group and placebo group, respectively. Among the drug-treated subjects who achieved remission, the effect of the drug was judged as stable in eight of the 14 subjects as measured by at least two CDAI scores indicating remission in the 15-wk treatment period. A decreased percentage of peripheral natural killer T regulatory cells (a decrease of 28% vs an increase of 16%) and an increased ratio of CD4(+)/CD8(+) T lymphocytes (an increase of 11% vs a decrease of 9%) were noted in subjects with a significant clinical response.Oral administration of the autologous colonic extract could be a safe and effective for the treatment of patients with moderate to severe Crohn's disease.

Published

2015

2. Glucocerebroside treatment ameliorates ConA hepatitis by inhibition of NKT lymphocytes

Author

Maya, Margalit, Samir, Abu Gazala, Samir Abu, Ghazala, Ruslana, Alper, Eran, Elinav, Athalia, Klein, Victoria, Doviner, Yoav, Sherman, Barbara, Thalenfeld, Dean, Engelhardt, Elazar, Rabbani, and Yaron, Ilan

Subjects

Male, Physiology, Liver cytology, T-Lymphocytes, Lymphocyte, Gene Expression, chemical and pharmacologic phenomena, Glucocerebroside, Biology, Glucosylceramides, Mice, Glycolipid, Physiology (medical), Concanavalin A, medicine, Animals, Liver damage, Cell Proliferation, Hepatitis, Mice, Inbred BALB C, Hepatology, Gastroenterology, Dendritic Cells, medicine.disease, Killer Cells, Natural, medicine.anatomical_structure, Liver, Immunology, biology.protein, Cytokines, Chemical and Drug Induced Liver Injury, Spleen, Transcription Factors

Abstract

Concanavalin A (ConA) induces natural killer T (NKT) cell-mediated liver damage. Glucocerebroside (GC) is a naturally occurring glycolipid. Our aims were to determine the effect of GC in a murine model of ConA-induced hepatitis. Mice in groups A and B were treated with GC 2 h before and 2 h following administration of ConA, respectively; group C mice were treated with ConA; group D mice was treated with GC; group E mice did not receive any treatment. Liver damage was evaluated by serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) levels and liver histology. The immune effect of GC was determined by fluorescence-activated cell sorter analysis of intrahepatic and intrasplenic NKT lymphocytes, measurement of cytokine levels, and Western blot analysis for STAT 1, 4, 6, and NF-κB expression. The effect of GC on NKT cell proliferation was assessed in vitro. Serum AST and ALT levels were markedly reduced in GC-treated group A mice compared with nontreated group C animals, and histological damage was markedly attenuated in group A. The beneficial effect of GC was associated with a 20% decrease of intrahepatic NKT lymphocytes, significant lowering of serum IFN-γ levels, and decreased STAT1 and STAT6 expression. In vitro administration of GC led to a 42% decrease of NKT cell proliferation in the presence of dendritic cells but not in their absence. Intraperitoneally administered radioactive GC was detected in the liver and bowel. Administration of GC led to amelioration of ConA hepatitis associated with an inhibitory effect on NKT lymphocytes. GC holds promise as a new immune-modulatory agent.

Published

2005

3. Suppression of hepatocellular carcinoma by transplantation of ex-vivo immune-modulated NKT lymphocytes

Author

Elazar Rabbani, Oren Shibolet, Ruslana Alper, Eran Elinav, Yaron Ilan, Barbara Thalenfeld, Maya Margalit, Dean Engelhardt, and Athalia Klein

Subjects

CD4-Positive T-Lymphocytes, Cytotoxicity, Immunologic, Cancer Research, Adoptive cell transfer, Carcinoma, Hepatocellular, Lymphocyte, medicine.medical_treatment, Mice, Nude, chemical and pharmacologic phenomena, CD8-Positive T-Lymphocytes, Biology, Interferon-gamma, Mice, Liver Neoplasms, Experimental, Immune system, Antigen, Weight Loss, medicine, Animals, Hepatitis B Vaccines, Lymphocytes, Immunity, Cellular, Mice, Inbred BALB C, hemic and immune systems, Dendritic Cells, Immunotherapy, T lymphocyte, STAT4 Transcription Factor, Natural killer T cell, Adoptive Transfer, Interleukin-12, DNA-Binding Proteins, Killer Cells, Natural, medicine.anatomical_structure, Oncology, Immunology, Trans-Activators, Interleukin 12, Female, Interleukin-4, Neoplasm Transplantation

Abstract

NKT cells are a regulatory subset of T lymphocytes with immune modulatory effects and an important role in anti-tumor immunity. The feasibility of “ex-vivo education” of NKT cells has recently been demonstrated. To evaluate the anti-tumor effect of ex-vivo immune-modulated NKT lymphocytes in a murine model of hepatocellular carcinoma. Athymic Balb/C mice were sublethally irradiated and transplanted with human Hep3B HCC. NKT cells prepared from immunocompetent Balb/C mice were pulsed ex vivo with HCC-derived antigens (Group A), Hep3B cells (group B) or BSA (group C), and adoptively transferred into HCC harboring mice (1 × 06 NKT cells per mouse). Group D mice did not undergo NKT cell transplantation. Group E mice were transplanted with 1 × 106 NKT cells from HBV-immunized donors. Mice were followed for tumor size and weight. To determine the mechanism of the anti-tumor effect, intrasplenic lymphocyte populations were analyzed by FACS for NKT, CD4+ and CD8+ lymphocyte subpopulations; STAT 1, 4 and 6 expression in splenocytes was assessed by Western blot, and serum cytokine levels were measured by ELISA. Adoptive transfer of NKT cells pulsed with HCC-derived antigens (group A) and NKT cells from immunized donors (group E) resulted in complete disappearance of tumors within 4 weeks and attenuated weight loss (6.5% and 7% in groups A and E, respectively). In contrast, mice in groups B, C, and D developed large, necrotic tumors and severe weight loss (21%, 17% and 23% weight loss in groups B, C, and D, respectively). NKT/CD4 and CD8/CD4 ratios were significantly increased in groups A and E (12.3 and 17.6 in groups A and D, respectively, compared to 6.4, 4.8 and 5.6 in groups B, C and D, respectively, for the NKT/CD4 ratio; 41 and 19.8 in groups A and E, respectively, compared to 6.5, 11.8 and 3.2 in groups B, C, and D, respectively, for the CD8/CD4 ratio). Expression of the transcription factor STAT4 was evident in group A, but not in groups B-D. Serum IFNγ, IL12 and IL4 levels were increased in groups A and E. Adoptive transfer of NKT lymphocytes exposed ex vivo by HCC-derived antigens loaded on dendritic cells and NKT cells from immunized donors led to suppression of HCC in mice. NKT-mediated anti-tumor activity was associated increased NKT and CD8+ T lymphocyte numbers, increased expression of STAT4, a marker for IL-12 activity and elevated serum levels of the proinflammatory cytokines IFNγ and IL12, and of IL4. Ex-vivo modulation of NKT lymphocytes holds promise as a novel mode of immune therapy for HCC. © 2005 Wiley-Liss, Inc.

Published

2005

4. Genotype prevalence, viral load and outcome of hepatitis B virus precore mutant infection in stable patients and in patients after liver transplantation

Author

Daniel Shouval, Hemda Shmilovitz-Wiess, Jaqueline Sulkes, Athalia Klein, Ran Tur-Kaspa, Eytan Mor, Ziv Ben-Ari, Nili Daudi, Yaffa Ashur, and Marius Brown

Subjects

Adult, Male, Hepatitis B virus, Genotype, Population, Hepatitis B virus precore mutant, Virus Replication, medicine.disease_cause, Hepatitis B, Chronic, Recurrence, Seroepidemiologic Studies, medicine, Humans, Postoperative Period, education, Transplantation, education.field_of_study, business.industry, Lamivudine, Middle Aged, Viral Load, Hepatitis B, medicine.disease, Virology, Liver Transplantation, DNA, Viral, Mutation, Codon, Terminator, Reverse Transcriptase Inhibitors, Female, business, Viral load, Immunosuppressive Agents, medicine.drug

Abstract

Objective: The precore mutant is detectable in most Israeli patients with persistent hepatitis B virus (HBV) infection. The aim of this study was to determine the prevalence of HBV genotypes, viral load and outcome of precore mutant infection in stable patients and in patients after liver transplantation. Methods: The prevalence of HBV genotype and viral load were investigated in 81 patients with HBV precore mutant infection. Of these, 50 patients (40 males, 10 females; mean age 43.4 ± 11.0 yr) underwent liver transplantation and were serum HBV DNA-negative by hybridization at the time of transplantation. Patients received long-term HBV immunoprophylaxis and immunosuppression, and lamivudine in cases of graft HBV recurrence. The remaining 31 patients were stable, with serum anti-HBe-positivity. Genotypes were tested by restriction fragment length polymorphism of an S gene amplicon. Precore mutations were studied with an INNO-LiPA probe assay. Results: Follow-up was 46.6 ± 37.7 months. Most of the transplanted group was of Middle Eastern origin (53.6%); the remainder were from Eastern Europe (21.4%), Western Europe and the USA (10.8%), Africa (7.1%), and Asia (7.1%). In the transplanted group, the pre-transplant HBV genotype D was the most prevalent (96%), while genotype A was found in only 4%. Eleven patients (22%) developed recurrent HBV infection post-transplantation. There were no differences in genotype distribution between patients with graft reinfection or lamivudine resistance and patients without recurrence. Mean viral load at recurrence was 148.4 × 106 ± 60.4 × 106 copies/mL. The stable group had a similar origin and HBV genotype prevalence, but a lower mean viral load of 12.4 × 106 ± 29.4 × 106 copies/mL (p = 0.007). The prevalence of mutations at the precore region and codon 28 was similar in both groups. Conclusions: The chronic precore mutant HBV-infected patients were characterized as follows: (i) genotype D was the most frequent genotype, (ii) the HBV genotype distribution was similar in patients with stable infection and after liver transplantation, (iii) viral load at recurrence was significantly higher than in stable infection, and (iv) HBV genotype was unrelated to the development of recurrence or lamivudine resistance in the tested population.

Published

2004

5. Adoptive transfer of ex vivo immune-programmed NKT lymphocytes alleviates immune-mediated colitis

Author

Barbara Thalenfeld, Yaron Ilan, Dean Engelhardt, Elazar Rabbani, Lydia Zolotarov, Ruslana Alper, Oren Shibolet, Athalia Klein, and Yossef Kalish

Subjects

CD4-Positive T-Lymphocytes, Adoptive cell transfer, medicine.medical_treatment, Immunology, chemical and pharmacologic phenomena, Biology, Interferon-gamma, Mice, Th2 Cells, Immune system, Antigen, medicine, Animals, Immunology and Allergy, Cells, Cultured, hemic and immune systems, Dendritic Cells, Cell Biology, T helper cell, Th1 Cells, Colitis, Natural killer T cell, Adoptive Transfer, Killer Cells, Natural, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Cytokine, Trinitrobenzenesulfonic Acid, Cytokines, Female, Interleukin-4, Spleen, CD8, Ex vivo

Abstract

T lymphocyte-expressing natural killer (NK) cell markers (NKT cells) play a role in immune regulation. Our aim was to evaluate the in vivo effect of adoptive transfer of immune-programmed NKT cells. Colitis was induced in C57/B6 mice by 2,4,6-trinitrobenzenesulfonic acid. NKT, CD4, CD8 lymphocytes, and dendritic cells (DC) were prepared from spleens of naive mice, animals with colitis, and animals with colitis that were orally tolerized. Subsets of splenocytes, NKT, CD4, and CD8 and NKT+CD4, NKT+CD8, and NKT+DC lymphocytes were prepared. Assessment of the T helper cell type 1 (Th1)/Th2 cytokine secretion paradigm in vitro was performed before and following exposure to the antigen. Adoptive transfer of ex vivo immune-programmed lymphocytes from each group was performed into recipient mice, followed by colitis induction. Ex vivo exposure of NKT cells harvested from mice with colitis-to-colitis proteins [colitis-extracted proteins (CEP)] led to a Th2 cytokine shift. The interleukin (IL)-4/interferon-γ (IFN-γ) ratio increased for NKT harvested from colitis-harboring mice following exposure to CEP. Adoptive transfer of NKT lymphocytes harvested from colitis-harboring mice, which were ex vivo-educated, significantly alleviated experimental colitis in vivo. Intrahepatic NKT lymphocytes increased significantly in mice transplanted with NKT lymphocytes harvested from colitis-harboring donor mice, which were ex vivo-exposed to CEP, similar to mice transplanted with NKT lymphocytes harvested from tolerized donors. Exposure of NKT cells to the disease-target antigen induced a significant increase in the IL-4/IFN-γ cytokine ratio. Adoptive transfer of a relatively small number of immune-programmed NKT cells induced a systemic Th1 to Th2-immune shift and alleviated immune-mediated colitis.

Published

2003

6. Early expression of interferon gamma following oral antigen administration is associated with peripheral tolerance induction

Author

Yoram Menachem, Roslana Alper, Athalia Klein, Olga Kolker, Yaron Ilan, Oren Shibolet, Elazar Rabbani, and Dean Engelhardt

Subjects

Male, Time Factors, medicine.medical_treatment, Lymphocyte, Immunology, Administration, Oral, Gene Expression, Microbiology, Interferon-gamma, Mice, Immune system, Antigen, Oral administration, Immune Tolerance, medicine, Animals, Interferon gamma, Antigens, Colitis, Peripheral tolerance induction, Mice, Inbred BALB C, business.industry, Body Weight, medicine.disease, Interleukin-10, Infectious Diseases, Cytokine, medicine.anatomical_structure, Trinitrobenzenesulfonic Acid, business, medicine.drug

Abstract

Oral tolerance is the induction of immune hyporesponsiveness to orally administered antigens. It was described in association with a decrease in interferon gamma (IFNgamma) production by activated T cells. To determine the role of IFNgamma and IL10 in immunemodulation via oral tolerization. Colitis was induced by intracolonic instillation of trinitrobenzene sulfonic acid. Treated mice received five oral doses of colitis-extracted proteins (CEPs) every other day, starting immediately after colitis induction. Control mice received similar doses of bovine serum albumin. Colitis was assessed in both groups by standard clinical, micro- and macroscopic scores. IFNgamma and IL10 expression in splenic lymphocytes from both groups was tested by RT-PCR immediately after oral feeding, 1, 4, 8, 12, and 24 h thereafter and then every 24 h for 2 weeks. Feeding of CEPs markedly ameliorated experimental colitis. These mice gained weight and showed markedly improved macro- and microscopic parameters of colitis. Tolerized mice exhibited IFNgamma expression in splenic lymphocytes starting immediately following oral CEP immunization and up to 14 d thereafter. IL10 was expressed starting 1 h after CEP feeding and during the first 48 h thereafter. In contrast, non-tolerized control mice manifested IFNgamma expression starting on day 6 and had no IL10 expression. Early induction of IFNgamma expression by oral antigen may be associated with systemic tolerance in the experimental colitis setting. In contrast, late expression of IFNgamma is associated with a pro-inflammatory response in non-tolerized controls.

Published

2003

7. Quality Assurance,Quality Control and Accreditation

Author

Eric P. Bennett, Marcela Contreras, K. Whitby, Antonio Seoane, V. Mayaudon, Fátima Carneiro, R. Slinger, C. Hind, Rifaat Safadi, Noga Manny, Eithan Galun, Elisabeth Ledent, Gösta Berlin, M.-H. Hsieh, A. Bailey, T.-F. Ho, J. Vermeij, Alison Rusnak, Nunzio Cutuli, Kirk J. McManus, Y.-T. Huang, S.J. Stanworth, Natalie M. Cowley, Teresa Zelinski, Lena Edelman, Hazel Cockburn, Daniel Shouval, John W. Semple, D.J. van Rhenen, E.J. Fransen, L. Corash, D. Howell, J.A.J. Barbara, M. Ferguson, Sue Knowles, L. Lin, C.V. Prowse, S.-C. Yang, Naotaka Hamasaki, Gabriella Milana, J.A. Garson, Masaaki Yamamoto, Andrew Lang-Stevenson, Harsha Boralessa, Koray Ergünay, G. Kessler, Manuel Giralt, M. Tepper, J.A. Barbara, G. Sher, V. Scalia, Catherine A. Hyland, A. Giulivi, Gail Coghlan, Salvatore Musumeci, José Antonio García-Erce, R.M. Warwick, Guillaume Dighiero, R.B. Ferns, Henrik Clausen, Hari Boralessa, Nissim Harush, Margarida Amado, P. Gill, Yaron Ilan, R.S. Tedder, Víctor Manuel Solano, Athalia Klein, Allan Saul, Martine Lévy, and M. Bailey

Subjects

Engineering management, business.industry, media_common.quotation_subject, Control (management), Quality (business), Hematology, General Medicine, business, Quality assurance, Accreditation, media_common

Published

2000

8. Tracing hepatitis B virus to the 16th century in a Korean mummy

Author

Chang Seok Oh, Paul R. Grant, Dong Hoon Shin, Gila Kahila Bar-Gal, Myeung Ju Kim, Orit Pappo, Mark Spigelman, Seok Bae Kim, Athalia Klein, Daniel Shouval, Jong-Wan Kim, and Tae Hyun Kim

Subjects

Most recent common ancestor, Hepatitis B virus, Sequence analysis, Population, Genome, Viral, Biology, medicine.disease_cause, Genome, DNA sequencing, Complete sequence, Hepatitis B, Chronic, Asian People, medicine, Humans, education, Child, Phylogeny, education.field_of_study, Korea, Hepatology, Genetic Variation, Mummies, Sequence Analysis, DNA, Hepatitis B, medicine.disease, Virology, Phylogeography, History, 16th Century, DNA, Viral

Abstract

A rare find of a mummified child from the 16th century AD, in Korea, with relatively preserved organs, enabled a search for ancient hepatitis B virus (aHBV) DNA sequences from laparoscopic-derived liver biopsies. Analysis of the complete aHBV genome (3,215 base pairs) revealed a unique HBV genotype C2 (HBV/C2) sequence commonly spread in Southeast Asia, which probably represents an HBV that infected the Joseon Dynasty population in Korea. Comparison of the aHBV sequences with contemporary HBV/C2 DNA sequences revealed distinctive differences along four open reading frames. Genetic diversity between contemporary and recovered aHBV/C2 DNA may be the result of immunologic, environmental, and/or pharmacologic pressures. The calculated time of most recent common ancestor suggests that the Korean HBV sequence origin dates back at least 3,000 years and possibly as long as 100,000 years. This isolate most likely represents the earliest human HBV sequence that colonized Southeast Asia by human migration. Conclusion: This study describes the complete sequence of the oldest HBV isolate and the most ancient full viral genome known so far. (HEPATOLOGY 2012;56:1671–1680)

Published

2012

9. Hepatitis B virus precore mutants are identical in carriers from various ethnic origins and are associated with a range of liver disease severity

Author

Shlomit Aharonson, Athalia Klein, and Ran Tur-Kaspa

Subjects

Adult, Male, Hepatitis B virus, Hepatitis B virus DNA polymerase, viruses, Molecular Sequence Data, medicine.disease_cause, Polymerase Chain Reaction, Virus, Liver disease, Ethnicity, medicine, Humans, Hepatitis B e Antigens, Aged, Hepatitis, Mutation, Base Sequence, Hepatology, biology, Liver Diseases, Middle Aged, Hepatitis B, medicine.disease, biology.organism_classification, Virology, Stop codon, Oligodeoxyribonucleotides, Hepadnaviridae, Carrier State, DNA, Viral, Female

Abstract

Hepatitis B virus carriers in Israel are mostly HBeAg negative, of whom 5% to 10% have circulating hepatitis B virus. Recently, a hepatitis B virus variant with a stop codon in the precore region was identified, and it was suggested that specific mutations are associated with fulminant or severe chronic active hepatitis. We have analyzed serum samples from HBeAg-positive and HBeAg-negative patients by polymerase chain reaction, using primers spanning the precore/core region. Nucleotide sequence analysis (by direct sequencing) from amplified hepatitis B virus DNA demonstrated that viral genomes from all HBeAg-negative patients contain G to A mutation (nucleotide 1896), leading to the formation of a stop codon. An additional G to A mutation was identified three nucleotides downstream (nucleotide 1899). These patients are of various ethnic origins, with no unique clinical characteristics and with normal liver histology, chronic hepatitis or cirrhosis. No mutation at the precore/core region was observed in the HBeAg-positive patients. In conclusion, the precore mutations identified in hepatitis B virus carriers in Israel are identical regardless of the carrier's ethnic origin and are associated with mild-to-severe liver disease.

Published

1992

10. Oral Administration of OKT3 Monoclonal Antibody to Human Subjects Induces a Dose-Dependent Immunologic Effect in T Cells and Dendritic Cells

Author

Ehud Zigmond, Francisco J. Quintana, Mauricio F. Farez, Gopal Murugaiyan, Ibrahim Kasis, Athalia Klein, Ami Ben Ya'acov, Claire Baecher-Allan, Elizabeth Axelrod, Howard L. Weiner, Madi El Haj, Gadi Lalazar, Henry Wu, Lidya Zolotarov, Adi Dembinsky, Nila Hemed, Pia Kivisäkk, Roopali Gandhi, Yaron Ilan, and Samia J. Khoury

Subjects

Graft Rejection, Male, Regulatory T cell, medicine.drug_class, medicine.medical_treatment, T-Lymphocytes, Immunology, Dose-Response Relationship, Immunologic, Administration, Oral, medicine.disease_cause, Monoclonal antibody, Glucosylceramides, Article, Muromonab-CD3, Autoimmunity, Autoimmune Diseases, Oral administration, medicine, Immunology and Allergy, Humans, Cells, Cultured, Adjuvants, Pharmaceutic, Cell Proliferation, Immunosuppression Therapy, business.industry, Antibodies, Monoclonal, Immunotherapy, Dendritic Cells, medicine.disease, Transplant rejection, medicine.anatomical_structure, Immunoglobulin G, Cytokines, Drug Therapy, Combination, Interleukin 17, business, medicine.drug, Follow-Up Studies

Abstract

Parenteral OKT3 is used to treat transplant rejection and a humanized anti-CD3 Mab has shown positive clinical effects in new onset diabetes. Oral administration of anti-CD3 has not been tested in humans, but suppresses autoimmunity in animal models. Beta-glucosylceramide enhances NKT cell and regulatory T cell activity and enhances the effects of oral anti-CD3 in animals.Fifteen healthy volunteers (three per group) received orally administered OKT3 over a dose range of 0.2 to 5.0 mg daily with or without beta-glucosylceramide 7.5 mg for 5 days. Safety and immune parameters were measured on days 5, 10, and 30.Oral OKT3 enhanced T cell proliferation, suppressed Th1 and Th17 responses by 43% and 41%, respectively, increased TGF-beta/IL-10 expression and decreased IL-23/IL-6 expression by dendritic cells, and affected the IgG repertoire as measured by antigen arrays. Co-administration of oral beta-glucosylceramide induced similar effects. No side effects were observed and no subjects developed human anti-mouse antibodies.These findings demonstrate that oral anti-CD3 monoclonal antibody is safe and biologically active in humans and presents a new avenue for the treatment of autoimmune diseases.

Published

2009

11. The mouse ribosomal protein L7 gene. Its primary structure and functional analysis of the promoter region

Author

Oded Meyuhas and Athalia Klein

Subjects

Ribosomal Proteins, Molecular Sequence Data, Restriction Mapping, Pair-rule gene, Biology, Transfection, Biochemistry, Cell Line, Gene product, Mice, Sequence Homology, Nucleic Acid, Gene cluster, Animals, Coding region, Amino Acid Sequence, RNA, Messenger, Promoter Regions, Genetic, Molecular Biology, Gene, Regulator gene, Genetics, Base Sequence, Structural gene, Exons, Cell Biology, Rats, Nested gene, Genes, Oligonucleotide Probes

Abstract

The expressed gene coding for mouse ribosomal protein L7 (rpL7) was structurally and functionally characterized. It consists of seven exons, spans 3107 base pairs, and its coding sequence initiates within exon 1. The primary structure of mouse rpL7 (270 amino acids), as inferred from the nucleotide sequence of the exons of the gene, and from the cDNA, is 12 residues longer than the rat counterpart. The rpL7 gene shares common structural features with most other mammalian ribosomal protein genes analyzed thus far. These include the lack of a canonical TATA box and a major transcription initiation site at a cytidine residue embedded in a stretch of 14 pyrimidines, flanked by C + G-rich regions. Transient expression assays revealed that the promoter region of rpL7 gene bears several regulatory elements, both upstream to the capsite and within the transcribed portion of the gene. One internal regulatory element was assigned to the first intron and a second one to a 20-base pair region spanning the first exon-intron junction. The activity of a deletion mutant of rpL32 gene, lacking its internal elements can be rescued by insertion, in the sense orientation, of the corresponding elements from the rpL7 gene. The unique spatial organization of the regulatory elements in rpL7 gene, as well as in other murine ribosomal protein genes examined thus far, might indicate that this common architecture is involved in the mechanism coordinating their expression.

Published

1990

12. A double-blind clinical trial for treatment of Crohn's disease by oral administration of Alequel, a mixture of autologous colon-extracted proteins: a patient-tailored approach

Author

Ehud Zigmond, Yaron Ilan, Eran Goldin, Oren Shibolet, Nilla Hemed, Eran Israeli, James J. Donegan, Maya Margalit, Athalia Klein, and Elazar Rabbani

Subjects

Adult, Male, medicine.medical_specialty, Tailored approach, Adolescent, Colon, CD8 Antigens, CD4-CD8 Ratio, Colonoscopy, Administration, Oral, Disease, Gastroenterology, Autoantigens, law.invention, Double blind, Cohort Studies, Epitopes, Randomized controlled trial, Crohn Disease, Double-Blind Method, law, Oral administration, Internal medicine, Sickness Impact Profile, Medicine, Humans, Intestinal Mucosa, Crohn's disease, Hepatology, medicine.diagnostic_test, business.industry, Middle Aged, medicine.disease, digestive system diseases, Surgery, Clinical trial, Killer Cells, Natural, Treatment Outcome, CD4 Antigens, Quality of Life, Prednisone, Female, business, Immunosuppressive Agents, Follow-Up Studies

Abstract

In this study, we evaluated the safety and efficacy of a personalized mode of treatment for Crohn's disease (CD) by oral administration of Alequel an extract of autologous colonic proteins.Thirty-one patients with moderate to severe CD were enrolled in a 27-wk randomized, double-blind, placebo-controlled trial. Patients were randomized to receive either a placebo or the study drug prepared from autologous colonic extract.Oral administration of autologous colonic proteins resulted in clinical remission (58% vs 29%; 46.6% vs 26.6%, using an intention to treat analysis, p= NS), clinical response (67% vs 43%; 53.3% vs 40%, using an intention to treat analysis, p= NS) and improved quality of life (Inflammatory Bowel Disease Questionnaire score improvement 43%vs 12%) in the drug study group, compared to placebo group. No treatment-related adverse events were noted. Only in the study-drug-treated cohort who achieved clinical remission (DR), there was a decreased number of subject-specific, antigen-directed, IFNgamma spot-forming colonies. DR subjects had a lower initial C-reactive protein level than DNOR or placebo subjects, an increased percentage of peripheral blood nature killer T cells, and an increased CD4+/CD8+ T-cell ratio throughout the period of drug administration.Oral administration of Alequel is a safe method for treatment of patients with moderate to severe CD, and its efficacy needs to be proven. Several markers may be applicable as surrogate markers for the clinical effect.

Published

2006

13. Suppression of hepatocellular carcinoma growth in mice via leptin, is associated with inhibition of tumor cell growth and natural killer cell activation

Author

Yaron Ilan, Elazar Rabbani, Orit Pappo, Eran Elinav, Athalia Klein, Asad Abd-Elnabi, Dean Engelhardt, and Itamar Bernstein

Subjects

Leptin, Male, medicine.medical_specialty, Carcinoma, Hepatocellular, Ratón, Mice, Nude, Suppressor of Cytokine Signaling Proteins, Mice, SCID, Biology, In Vitro Techniques, Lymphocyte Activation, Natural killer cell, Mice, Immune system, Suppressor of Cytokine Signaling 1 Protein, Internal medicine, Cell Line, Tumor, medicine, Animals, Humans, RNA, Neoplasm, Cell Proliferation, Hepatology, Cell growth, digestive, oral, and skin physiology, Liver Neoplasms, Intracellular Signaling Peptides and Proteins, STAT2 Transcription Factor, Flow Cytometry, Lymphocyte Subsets, Natural killer cell proliferation, Killer Cells, Natural, Repressor Proteins, Endocrinology, medicine.anatomical_structure, Cell culture, Natural killer cell activation, hormones, hormone substitutes, and hormone antagonists, Neoplasm Transplantation

Abstract

Background/Aims Leptin exerts potent immune modulatory properties. The aim of this study was to determine leptin's anti-tumor effect in a murine model of hepatocellular carcinoma (HCC). Methods In vivo, athymic nude mice were transplanted with Hep3B cells, followed by daily leptin administration for 6 weeks. Results Leptin administration induced a significant reduction in tumor size, improved survival rate, and was associated with a significant increase in peripheral natural killer (NK) cell number. Splenocytes from leptin-treated mice featured decreased expression of CIS mRNA. SCID mice featured a similar leptin-associated tumor suppression. In contrast, NK-deficient SCID-beige mice developed larger tumors which were unresponsive to leptin. NK cells incubated in vitro with increasing doses of leptin demonstrated increased cytotoxicity and proliferation. Incubation of leptin with hepatoma cells induced a dose-dependent reduction in proliferation, suggesting a direct anti-tumor effect. Leptin induced increased mRNA expression of STAT2 and SOCS1 on HCC cell lines. Conclusions Leptin administration induces a significant suppression of human HCC. This effect is mediated by induction of natural killer cell proliferation and activation, along with direct inhibition of tumor growth. Decreased NK expression of inhibitory CIS and over-expression of the antiproliferative STAT2 and SOCS1 proteins in HCC lines may underline the anti-cancerous effects of leptin.

Published

2005

14. Induction of oral immune regulation towards liver-extracted proteins for treatment of chronic HBV and HCV hepatitis: results of a phase I clinical trial

Author

Athalia Klein, Barbara Thalenfeld, Oren Shibolet, Eran Israeli, Elazar Rabbani, Yaron Ilan, Alaa Melhem, Nilla Hemed, Orit Pappo, Rifaat Safadi, and Dean Engelhardt

Subjects

Adult, Male, Adolescent, Hepatitis C virus, Administration, Oral, medicine.disease_cause, Interferon-gamma, Viral Proteins, Immune system, Hepatitis B, Chronic, Antigen, medicine, Humans, Hepatitis B e Antigens, Prospective Studies, Hepatitis B virus, Hepatology, medicine.diagnostic_test, business.industry, virus diseases, Hepatitis C, Hepatitis B, Hepatitis C, Chronic, Middle Aged, Viral Load, medicine.disease, digestive system diseases, Chromium Radioisotopes, Interleukin-10, Treatment Outcome, Liver, Liver biopsy, Immunology, Female, business, Viral load, Cell Division, T-Lymphocytes, Cytotoxic

Abstract

Background: Anti-viral immunity can be modulated via oral feeding of viral proteins. Hepatitis B and C viral (HBV, HCV)-associated hepatocellular injury is mediated by a defective host anti-viral immune response. Aims: To determine the effect of oral administration of a mixture of liver-extracted proteins with HBV/HCV proteins, on viral load, liver injury, and the anti-viral T-cell response of chronic HBV/HCV patients. Methods: Fourteen patients with chronic HBV and 15 patients with chronic HCV were treated orally with hepatocyte-extracted proteins and HBV or HCV viral proteins for 24 weeks, and followed for an additional 26 weeks. Patients were monitored for HBV-DNA or HCV-RNA levels, liver enzymes and liver histology. Viral-directed T-cell immunity was assessed by IFNγ and IL10 ELISPOT, viral-specific T-cell proliferation, cytotoxicity, and cytokines assays, and followed for peripheral natural killer T-cell (NKT) number. Results: In both chronic HBV and HCV patients, oral administration of a mixture of selected liver-extracted proteins and viral proteins induced a favorable increase in viral-specific T-cell proliferation, and IFNγ-secreting clones, along with a significant decrease in the anti-viral IL10-secreting T-cell clones. However, the effects of modulation of the anti-viral immunity differed between the HBV and HCV patients. In both groups, no major adverse events were noted. In chronic HBV patients, a significant decrease in viral load was observed in 5/14 (35.7%) of patients. HB surface antigen/HB nucleocapsid antigen scores on liver biopsy improved in 46.1% and 50%, respectively, and the histological necroinflammatory score improved in 4/13 (30.7%). Forty percent of the patients with elevated liver enzymes showed a favorable biochemical response. In contrast, an improvement in the histological necroinflammatory score was observed in only 2/12 (17%) of the chronic HCV patients. No significant decrease in HCV RNA was noted in any of these patients. Conclusions: Immune regulation of the anti-HBV/HCV immune response via oral administration of a mixture of liver-extracted and viral proteins significantly altered the viral-specific immunity. This effect was associated with clinical and virological improvements in chronic HBV patients.

Published

2004

15. Treatment of chronic hepatitis B virus infection via oral immune regulation toward hepatitis B virus proteins

Author

Yaron Ilan, Orit Papo, Elazar Rabbani, Barbara Thalenfeld, Aharon Bloch, Nilla Hemed, Oren Shibolet, Athalia Klein, Mina Rowe, Eran Israeli, Rifaat Safadi, Dean Engelhardt, Alaa Melhem, Ruslana Alper, and Ori Segol

Subjects

Adult, Male, Hepatitis B virus, Adolescent, viruses, Administration, Oral, medicine.disease_cause, Risk Assessment, Virus, Drug Administration Schedule, Statistics, Nonparametric, Hepatitis B, Chronic, Chronic hepatitis, Oral administration, Immune Tolerance, Medicine, Humans, Prospective Studies, Aged, Probability, Hepatitis B Surface Antigens, Hepatology, Dose-Response Relationship, Drug, business.industry, Viral Core Proteins, Gastroenterology, Immune regulation, Viral hepatitis b, biochemical phenomena, metabolism, and nutrition, Middle Aged, Virology, Reverse transcription polymerase chain reaction, Treatment Outcome, Immunology, Female, Viral disease, Immunotherapy, business, Follow-Up Studies

Abstract

Hepatitis B virus (HBV) is a noncytopathic virus, and hepatocellular injury is mediated by a defective host antiviral immune response. We have previously shown that antiviral immunity can be modulated through oral feeding of viral proteins. The aims of this study were to determine the safety and efficacy of treatment of patients with chronic HBV by means of p.o. administration of HBV envelope proteins.A total of 42 chronic HBV patients were treated p.o. with HBV envelope proteins (HBsAg+preS1+preS2), three times/wk for 20-30 wk, and followed for an additional 20 wk. Patients were monitored for HBV-DNA levels, liver enzymes, and liver histology. HBV-directed T cell immune modulation was assessed in vitro by HBV specific T cell-proliferation, cytotoxicity, IFN gamma, and IL10 ELISPOT assays, and reverse transcription-polymerase chain reaction cytokines assay.Favorable response in one of the primary endpoints was achieved in 28/42 patients (66.6%) by means of p.o. immune regulation. A significant decrease in viral load was observed in 15 patients (35.7%). HBsAg/HBcAg biopsy scores improved in 41% and 57.1% of patients, respectively. Histological improvement in liver necroinflammatory score was noted in 12/40 patients (30%). In all, 80% showed biochemical response. Five of 19 HBeAg positive patients (26.3%) became negative for HBeAg. A favorable augmentation in anti-HBV specific T cell response, with increased HbsAg specific T cell proliferation (78%), cytotoxicity (75%), and IFN gamma positive T cell clones (62.9%) was noted. In addition, a decrease in the IL10 gamma positive T cell clones was achieved (48.1%). Natural killer T (NKT) lymphocytes increased significantly in all treated patients.Immune regulation of the anti-HBV immune response via p.o. administration of HBV envelope proteins alleviated the immune-mediated liver injury while augmenting the effective antiviral immunity.

Published

2003

16. Genotypic and phenotypic resistance: longitudinal and sequential analysis of hepatitis B virus polymerase mutations in patients with lamivudine resistance after liver transplantation

Author

Ran Tur-Kaspa, Nili Daudi, Eytan Mor, Athalia Klein, Orit Papo, Ziv Ben-Ari, Daniel Shouval, Rachamim Gadba, Jaqueline Sulkes, and Zmira Samra

Subjects

Adult, Male, Hepatitis B virus, Genotype, medicine.medical_treatment, Population, Drug Resistance, DNA-Directed DNA Polymerase, Biology, Liver transplantation, medicine.disease_cause, law.invention, law, medicine, Humans, Longitudinal Studies, education, Child, Polymerase chain reaction, education.field_of_study, Hepatology, Gastroenterology, Wild type, Lamivudine, Middle Aged, Virology, Liver Transplantation, Transplantation, Phenotype, Mutation, Reverse Transcriptase Inhibitors, Female, medicine.drug

Abstract

Objective Lamivudine-resistant strains appear in 27–62.5% of liver transplant recipients treated with lamivudine for hepatitis B virus (HBV) recurrence, and may lead to failure of antiviral therapy. In an extension of our previous study, we investigated the molecular events associated with the emergence of lamivudine-resistant mutants in this population. Methods Sequential serum samples from 10 consecutive patients with lamivudine resistance after liver transplantation were analyzed for viral genotype, precore mutants, and viral polymerase gene mutants (L528M, M552V, M552I) using restriction fragment length polymorphism. Quantitative analysis of HBV DNA was performed using hybridization assay and polymerase chain reaction. Results Eight patients (80%) were infected with genotype D and two (20%) with genotype C. Polymerase mutants (genotypic resistance) were identified in all the patients. Phenotypic resistance (rise in serum HBV DNA titers above the detection limit of the hybridization assay) developed in five patients (50%); of the remainder, three (30%) did not have phenotypic resistance, and two were primary nonresponders. Genotypic resistance was detected earlier than phenotypic resistance (median 285 days [range 42–510] vs median 387 days [range 320–420], p = 0.055). In five patients (50%), the emergence of the YMDD mutants took over the wild type; in three (30%), the YMDD mutant took over the wild type, but the wild type re-emerged during lamivudine therapy; and in two (20%), the YMDD mutants were detected in a mixture with the wild type (in different percentages). The mean pretreatment serum ALT level was significantly lower in the patients who did not develop phenotypic resistance ( p = 0.0002). The M552I pure viral population was found mainly in these patients, and all retained stable graft function (median follow-up 33 months). A high pretreatment HBV DNA level (>50 × 10 6 copies/ml) was highly statistically significantly correlated with the rapid occurrence of phenotypic resistance ( r = −0.90, p = 0.04). Conclusions We reached the following conclusions: 1) In our area, liver transplant recipients who develop resistance to lamivudine given for recurrent HBV infection seem to be mainly infected with genotype D. 2) Re-emergence of the wild type can occur during lamivudine therapy. 3) Genotypic resistance precedes phenotypic resistance, although phenotypic resistance does not always follow genotypic resistance. 4) Quantitative determination of viremia and analysis of polymerase gene mutants are recommended for monitoring antiviral therapy of liver transplant patients with HBV reinfection in the graft.

Published

2003

17. Resistance of Hepatitis Delta Virus Replication to Interferon- Treatment in Transfected Human Cells

Author

Ran Tur-Kaspa, Yaron Ilan, Athalia Klein, and Jonathan Taylor

Subjects

Carcinoma, Hepatocellular, viruses, Genome, Viral, Interferon alpha-2, Biology, Transfection, Virus Replication, medicine.disease_cause, Virus, chemistry.chemical_compound, Plasmid, 2',5'-Oligoadenylate Synthetase, Tumor Cells, Cultured, medicine, Humans, Immunology and Allergy, Interferon alfa, Hepatitis B virus, Liver Neoplasms, Interferon-alpha, virus diseases, RNA, biochemical phenomena, metabolism, and nutrition, Blotting, Northern, Virology, Recombinant Proteins, Infectious Diseases, Viral replication, chemistry, RNA, Viral, Hepatitis Delta Virus, DNA, medicine.drug

Abstract

Interferon-alpha (IFN-alpha) is known to inhibit both DNA and RNA viruses, including hepatitis B virus (HBV). In humans the antiviral effect, if any, of IFN-alpha on hepatitis delta virus (HDV) is complicated by the fact that HDV is spread only to patients already infected with HBV. An in vitro model system was used to assay for an antiviral effect of IFN-alpha on HDV genome replication. Hep G2 cells were transfected with a plasmid containing a trimer of HDV and treated with IFN (20 or 100 units/mL) starting 1-7 days after transfection. RNA extracted from treated and nontreated cells was assayed by both slot blot and Northern analyses. The IFN-alpha treatment as expected increased the 2'-5' oligo A synthetase RNA activity, but it did not affect HDV genome replication. Thus, in the absence of HBV, it appears that HDV is resistant to IFN-alpha.

Published

1992

18. The TATA-less promoter of hepatitis B virus S gene contains a TBP binding site and an active initiator

Author

Athalia Klein, V. Bogomolski-Yahalom, Y Haviv, I Greenblat, and Ran Tur-Kaspa

Subjects

Chloramphenicol O-Acetyltransferase, Cancer Research, Hepatitis B virus, Carcinoma, Hepatocellular, TATA box, Recombinant Fusion Proteins, Mutant, Response element, Molecular Sequence Data, CAAT box, Biology, Transfection, Initiator element, Virology, Tumor Cells, Cultured, Humans, Cloning, Molecular, Promoter Regions, Genetic, Gene, Genetics, Binding Sites, Hepatitis B Surface Antigens, Base Sequence, TATA-Box Binding Protein, Liver Neoplasms, Genetic Variation, Promoter, Molecular biology, TATA Box, Recombinant Proteins, DNA-Binding Proteins, Infectious Diseases, DNA, Viral, Transcription Factors

Abstract

The surface antigen (S) gene promoter, one of the major hepatitis B virus (HBV) promoters, directs the synthesis of a 2.1 kb mRNA which encodes the preS2 and S polypeptides. The preS2/S promoter does not contain a classical TATA box, and transcription regulation of the preS2/S gene has not been fully elucidated. We analysed two regions involved in preS2/S gene transcription of the HBV adw subtype: the diverged TATA box and a putative initiator element. We demonstrated sequence specific promoter activity of the putative TATA-like sequences in the preS2/S gene promoter (-25 to -32 bp). Using end labeled synthetic oligonucleotides we observed specific binding of nuclear extracts to the diverged TATA sequence, that was significantly reduced using a mutated oligonucleotide. Specific binding of yeast TBP to the diverged TATA sequence was shown which was increased in the mutant containing a classical TATA box. We analysed the proposed initiator (Inr) sequence of the preS2/S promoter region (-13 to -16 bp). Deletion of the inr element markedly reduced promoter activity as assessed by CAT expression. Gel shift assays showed specific binding of nuclear extracts to wild type but not to mutant Inr. Expression studies with double mutants of the diverged TATA and the Inr element established that both elements are active in transcription regulation.

Published

1997

19. Estrogen suppresses hepatitis B virus expression in male athymic mice transplanted with HBV transfected Hep G-2 cells

Author

Yaniv Almog, Athalia Klein, Ran Tur-Kaspa, Ruth Adler, and Orgad Laub

Subjects

Gene Expression Regulation, Viral, Male, HBsAg, Hepatitis B virus, medicine.drug_class, Mice, Nude, Biology, medicine.disease_cause, Transfection, Virus, Mice, Virology, Gene expression, medicine, Tumor Cells, Cultured, Animals, Humans, Hepatitis B e Antigens, RNA, Messenger, Pharmacology, Regulation of gene expression, Mice, Inbred BALB C, Sex Characteristics, Estradiol, virus diseases, Neoplasms, Experimental, biology.organism_classification, Molecular biology, digestive system diseases, Hepadnaviridae, HBeAg, Estrogen, DNA, Viral, RNA, Viral, Female

Abstract

Hormones are known to regulate both viral and cellular genes. It has been shown previously that estrogen has an effect on liver gene transcription and mRNA stability. Sex hormones might have a role in the chronic persistence of hepatitis B virus (HBV) infection. In fact, there is a male preponderance in the incidence of chronic HBV infection, and HBsAg expression was reported to be much higher in male transgenic mice than in the females. We investigated the effect of estrogen on HBV gene expression and regulation in athymic mice bearing 2.2.15 cells, a human hepatoblastoma cell line derived from Hep G-2 transfected with HBV sequences. Both male and female mice were treated with estradiol after tumors could be observed. Episomal DNA was extracted from the tumors and hybridized with 32P-labelled HBV DNA. Southern blot and slot blot analyses demonstrated that male mice had higher expression of HBV DNA. Estrogen treatment suppressed HBV DNA expression in males, but had only a minor effect on females. HBeAg production in male mice was also inhibited by estrogen treatment. HBV RNA extracted from 2.2.15 cells showed 2-3-fold reduction following beta-estradiol treatment. Moreover, inhibition of HBV transcription by estrogen was demonstrated by an RNA pulse-labelling experiment. These data indicate that estrogen inhibits HBV expression in the in vivo model presented in this study. These results might contribute to a better understanding of the effect of sex hormones on the pathogenesis of HBV-induced liver disease.

Published

1992

20. Subject Index Vol. 79, 2000

Author

Noga Manny, R.S. Tedder, Lena Edelman, T.-F. Ho, Víctor Manuel Solano, Y.-T. Huang, J. Vermeij, Elisabeth Ledent, Yaron Ilan, G. Kessler, Fátima Carneiro, C.V. Prowse, Marcela Contreras, L. Lin, M. Ferguson, Hazel Cockburn, Sue Knowles, S.-C. Yang, M. Tepper, Masaaki Yamamoto, J.A. Garson, Eric P. Bennett, Gabriella Milana, Kirk J. McManus, Naotaka Hamasaki, Koray Ergünay, José Antonio García-Erce, M.-H. Hsieh, V. Scalia, Salvatore Musumeci, Eithan Galun, K. Whitby, Gösta Berlin, R.B. Ferns, J.A.J. Barbara, Alison Rusnak, E.J. Fransen, L. Corash, Andrew Lang-Stevenson, Catherine A. Hyland, Antonio Seoane, V. Mayaudon, Natalie M. Cowley, Henrik Clausen, D. Howell, R. Slinger, Rifaat Safadi, Harsha Boralessa, Teresa Zelinski, R.M. Warwick, A. Bailey, Nissim Harush, Manuel Giralt, Hari Boralessa, C. Hind, Daniel Shouval, S.J. Stanworth, John W. Semple, J.A. Barbara, G. Sher, Margarida Amado, P. Gill, Guillaume Dighiero, A. Giulivi, Gail Coghlan, Nunzio Cutuli, D.J. van Rhenen, Athalia Klein, Allan Saul, Martine Lévy, and M. Bailey

Subjects

Index (economics), Statistics, Subject (documents), Hematology, General Medicine, Mathematics

Published

2000

21. Contents Vol. 79, 2000

Author

Antonio Seoane, Teresa Zelinski, V. Mayaudon, E.J. Fransen, R. Slinger, L. Corash, A. Bailey, Yaron Ilan, Catherine A. Hyland, Elisabeth Ledent, Lena Edelman, Noga Manny, Eric P. Bennett, A. Giulivi, Kirk J. McManus, Manuel Giralt, J.A.J. Barbara, Naotaka Hamasaki, Athalia Klein, K. Whitby, Allan Saul, Hazel Cockburn, R.B. Ferns, V. Scalia, Andrew Lang-Stevenson, Rifaat Safadi, J.A. Barbara, G. Sher, Martine Lévy, Eithan Galun, R.M. Warwick, C. Hind, Marcela Contreras, R.S. Tedder, L. Lin, Gail Coghlan, Víctor Manuel Solano, M. Ferguson, Salvatore Musumeci, Masaaki Yamamoto, C.V. Prowse, Fátima Carneiro, J. Vermeij, Sue Knowles, M. Bailey, S.-C. Yang, S.J. Stanworth, Gabriella Milana, José Antonio García-Erce, M.-H. Hsieh, Koray Ergünay, John W. Semple, Alison Rusnak, D. Howell, Henrik Clausen, Natalie M. Cowley, Hari Boralessa, Guillaume Dighiero, Nunzio Cutuli, D.J. van Rhenen, T.-F. Ho, Y.-T. Huang, J.A. Garson, Daniel Shouval, Nissim Harush, Harsha Boralessa, Gösta Berlin, Margarida Amado, P. Gill, G. Kessler, and M. Tepper

Subjects

Hematology, General Medicine

Published

2000

22. T1198 Oral Administration of Alequel™, a Mixture of Autologous Colon-Extracted Proteins for Treatment of Crohn's Disease: Results of a Double-Blind Clinical Trial

Author

Yaron Ilan, Gadi Lalazar, Eran Israeli, Ehud Zigmond, Nilla Hemed, Athalia Klein, and Eran Goldin

Subjects

medicine.medical_specialty, Crohn's disease, Pathology, Hepatology, business.industry, Gastroenterology, medicine.disease, Double blind, Clinical trial, Oral administration, Internal medicine, medicine, business

Published

2009

23. Oral immune regulation using colitis extracted proteins for treatment of Crohn’s disease: Results of a phase I clinical trial

Author

Elazar Rabbani, Yaron Ilan, Nilla Hemed, Eran Goldin, Dean Engelhardt, Oren Shibolet, Eran Israeli, and Athalia Klein

Subjects

Adult, Male, Colon, Lymphocyte, Administration, Oral, Phases of clinical research, Immune system, Crohn Disease, Intestinal mucosa, Clinical Research, Oral administration, medicine, Humans, Prospective Studies, Intestinal Mucosa, Colitis, Crohn's disease, business.industry, ELISPOT, Gastroenterology, Proteins, General Medicine, Middle Aged, medicine.disease, medicine.anatomical_structure, Immunology, Female, business

Abstract

AIM: To evaluate safety and possible efficacy of induction of oral immune regulation using colitis extracted proteins (CEP) in Crohn’s disease (CD) subjects. METHODS: Ten CDs were treated orally with autologous CEP thrice weekly for 16 wk. Subjects were monitored for CDAI and IBDQ. Immune modulatory effect was assessed by T-lymphocyte FACS analysis, CEP-specific IFNγ ELISPOT assay and cytokine levels. RESULTS: Induction of oral immune regulation significantly ameliorated disease activity. All (10/10) subjects had clinical response (CDAI ≤ 70) and 7/10 achieved clinical remission (CDAI ≤ 150). Significant increase in mean IBDQ score was noted (134±9 vs 164±12). No treatment-related adverse events were noted. High levels of CEP-specific IFNγ spot forming colonies were detected in five subjects prior to treatment and in all five, a marked decrease was observed. The CD4+/CD8+ lymphocyte ratio and peripheral NKT cell numbers increased significantly, in 7/10 and in 5/10 subjects, respectively. Significant increase in serum IL-10 and IL-4 levels was observed in 7/10 subjects during treatment period. CONCLUSION: Immune regulation via oral administration of CEP is a safe and possibly effective treatment for subjects with moderate CD and may provide means of antigen-specific immune modulation.

Published

2005

24. 54 Suppression of hepatocellular carcinoma by transplantation of immune-modulated NKT lymphocytes is associated with STAT4 expression and a TH1 immune response

Author

Oren Shibolet, Dean Engelhardt, Ruslana Alper, Elazar Rabbani, Barbara Thalenfeld, Maya Margalit, Athalia Klein, and Yaron Ilan

Subjects

Transplantation, Th1 immune response, Immune system, Hepatology, business.industry, Hepatocellular carcinoma, Immunology, medicine, medicine.disease, business, STAT4

Published

2003

25. A plastic anemia—associated hepatitis successfully treated by bone marrow transplantation

Author

E. Galun, Yaron Ilan, Reuven Or, Rifaat Safadi, Daniel Shouval, and Athalia Klein

Subjects

Hepatitis, medicine.medical_specialty, Hepatology, Bone marrow transplantation, business.industry, Anemia, Internal medicine, medicine, medicine.disease, business, Gastroenterology

Published

1998

26. Resistance of delta virus replication to interferon alpha treatment in transfected human cells

Author

Jonathan Taylor, Yaron Ilan, Athalia Klein, and Ran Tur-Kaspa

Subjects

Delta, Hepatology, Viral replication, Alpha interferon, Transfection, Biology, Virology

Published

1991

27. The effect of alpha interferon on HBV replication and protein expression in nude mice transplanted with transfected Hep G2 cells

Author

Y. Kravis, Ran Tur-Kaspa, Ruth Adler, Athalia Klein, and Orgad Laub

Subjects

Hep G2, Hepatology, In vivo, Alpha interferon, Transfection, Biology, Hbv replication, Virology, Molecular biology, Protein expression

Published

1990

28. SEROTONIN BINDING PROTEIN: ENHANCEMENT OF BINDING BY Fe2+AND INHIBITION OF BINDING BY DRUGS2

Author

Hadassah Tamir, Athalia Klein, and Maurice M. Rapport

Subjects

inorganic chemicals, chemistry.chemical_classification, GTP', Plasma protein binding, Serotonergic, Biochemistry, Cellular and Molecular Neuroscience, Serotonin binding, chemistry, Adenine nucleotide, Biogenic amine, Serotonin, Binding site

Abstract

— The binding of serotonin to a soluble, high affinity binding protein, present in synaptosomes and associated with serotonergic tracts, has now been studied for the effects of metallic ions and various drugs. At optimal concentration (10-4 M) of Fe2+ the enhancement of binding was close to 20-fold. A much smaller effect was noted with Cu2+. With other ions (Fe3+, Mn2+, Co2+, Ni2+, Cr3+, Mg2+, Ca2+) little or no effect was seen. For the effect with Fe2+. preincubation was required (10 min, 25°C) and concentrations higher than 10-4M were inhibitory. Studies based on equilibrium dialysis show that the effect of Fe2+ was on the affinity of the binding of serotonin to the protein, rather than on the binding capacity. In polydcrylamide gels at pH 8.6 the migratory properties of thc serotonin-protein complex formed in the presence of Fe2+ differ from those of the complex formed without Fe2+. Nucleotides (ATP, GTP, ADP, AMP) inhibited thc binding. The effects of several classes of drugs (inhibitors of biogenic amine storage and uptake, psychotomimetics, MAO) inhibitors and drugs binding to contractile proteins) were also studied. The only effective inhibitors of serotonin binding were reserpine, vinblastine and CZ-74, which caused 50% inhibition at 2 × 10-6 M, 7.5 × 10-6 M and 0.2 × 10-6M respectively.

Published

1976

29. Oral mixture of autologous colon-extracted proteins for the Crohn's disease: A double-blind trial.

Author

Israeli E, Zigmond E, Lalazar G, Klein A, Hemed N, Goldin E, and Ilan Y

Subjects

Administration, Oral, Adult, Cell Separation methods, Colon immunology, Colon metabolism, Crohn Disease diagnosis, Crohn Disease immunology, Crohn Disease metabolism, Double-Blind Method, Female, Flow Cytometry, Humans, Immune Tolerance drug effects, Immunity, Mucosal drug effects, Israel, Male, Middle Aged, Proteins immunology, Proteins isolation & purification, Remission Induction, Severity of Illness Index, T-Lymphocyte Subsets drug effects, T-Lymphocyte Subsets immunology, Time Factors, Treatment Outcome, Young Adult, Colon drug effects, Crohn Disease therapy, Desensitization, Immunologic methods, Proteins administration & dosage

Abstract

Aim: To evaluate the safety and efficacy of oral administration of Alequel™, an autologous protein-containing colon extract., Methods: A total of 43 patients were enrolled in a randomized, placebo-controlled, double-blind trial. Patients were orally administered with autologous protein-containing colon extract three doses of autologous study drug per week for 15 wk, for a total of 45 doses. Patients were followed for safety parameters. Remission was defined as a Crohn's disease activity index (CDAI) score of less than or equal to 150. All patients were followed for changes in subsets of T cells by fluorescence-activated cell sorting analysis., Results: Analysis was performed on a total number of evaluable patients of 14 in the study drug group and 15 in the placebo group. Treatment was well tolerated by all patients. No major treatment-related adverse events were reported or observed in any of the treated patients during the feeding or follow-up periods. Between weeks 6 and 9 of the study, six of the 14 (43%) evaluable subjects who received the study drug achieved a CDAI of 150 or lower. In contrast, five of the 15 (33%) evaluable subjects in the placebo group achieved remission. Between weeks 9 and 12, the remission rates were 50% and 33% for the drug group and placebo group, respectively. Among the drug-treated subjects who achieved remission, the effect of the drug was judged as stable in eight of the 14 subjects as measured by at least two CDAI scores indicating remission in the 15-wk treatment period. A decreased percentage of peripheral natural killer T regulatory cells (a decrease of 28% vs an increase of 16%) and an increased ratio of CD4(+)/CD8(+) T lymphocytes (an increase of 11% vs a decrease of 9%) were noted in subjects with a significant clinical response., Conclusion: Oral administration of the autologous colonic extract could be a safe and effective for the treatment of patients with moderate to severe Crohn's disease.

Published

2015