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3. Outstanding Survival and Regeneration Process by the Use of Intelligent Acellular Dermal Matrices and Mesenchymal Stem Cells in a Burn Pig Model

Author

Mansilla, E., Spretz, R., Larsen, G., Nuñez, L., Drago, H., Sturla, F., Marin, G.H., Roque, G., Martire, K., Díaz Aquino, V., Bossi, S., Gardiner, C., Lamonega, R., Lauzada, N., Cordone, J., Raimondi, J.C., Tau, J.M., Biasi, N.R., Marini, J.E., Patel, A.N., Ichim, T.E., Riordan, N., and Maceira, A.

Published
2010
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6. Optical properties of InAsBi and optimal designs of lattice-matched and strain-balanced III-V semiconductor superlattices.

Author

Webster, P. T., Shalindar, A. J., Riordan, N. A., Gogineni, C., Liang, H., Sharma, A. R., and Johnson, S. R.

Subjects
OPTICAL properties of indium arsenide, OPTIMAL designs (Statistics), III-V semiconductors, SUPERLATTICES, PHOTODIODES, MOLECULAR beam epitaxy
Abstract

The optical properties of bulk InAs0.936Bi0.064 grown by molecular beam epitaxy on a (100)- oriented GaSb substrate are measured using spectroscopic ellipsometry. The index of refraction and absorption coefficient are measured over photon energies ranging from 44 meV to 4.4 eV and are used to identify the room temperature bandgap energy of bulk InAs0.936Bi0.064 as 60.6 meV. The bandgap of InAsBi is expressed as a function of Bi mole fraction using the band anticrossing model and a characteristic coupling strength of 1.529 eV between the Bi impurity state and the InAs valence band. These results are programmed into a software tool that calculates the miniband structure of semiconductor superlattices and identifies optimal designs in terms of maximizing the electron-hole wavefunction overlap as a function of transition energy. These functionalities are demonstrated by mapping the design spaces of lattice-matched GaSb/InAs0.911Sb0.089 and GaSb/InAs0.932Bi0.068 and strain-balanced InAs/InAsSb, InAs/GaInSb, and InAs/InAsBi superlattices on GaSb. The absorption properties of each of these material systems are directly compared by relating the wavefunction overlap square to the absorption coefficient of each optimized design. Optimal design criteria are provided for key detector wavelengths for each superlattice system. The optimal design mid-wave infrared InAs/InAsSb superlattice is grown using molecular beam epitaxy, and its optical properties are evaluated using spectroscopic ellipsometry and photoluminescence spectroscopy. [ABSTRACT FROM AUTHOR]

Published
2016
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8. Measurement of InAsSb bandgap energy and InAs/InAsSb band edge positions using spectroscopic ellipsometry and photoluminescence spectroscopy.

Author

Webster, P. T., Riordan, N. A., Liu, S., Steenbergen, E. H., Synowicki, R. A., Zhang, Y.-H., and Johnson, S. R.

Subjects
*BAND gaps, *LATTICE dynamics, *X-ray diffraction measurement, *PHOTOLUMINESCENCE, *SPECTRUM analysis, *MATHEMATICAL models
Abstract

The structural and optical properties of lattice-matched InAs0.911Sb0.089 bulk layers and strain-balanced InAs/InAs1-xSbx (x∼0.1-0.4) superlattices grown on (100)-oriented GaSb substrates by molecular beam epitaxy are examined using X-ray diffraction, spectroscopic ellipsometry, and temperature dependent photoluminescence spectroscopy. The photoluminescence and ellipsometry measurements determine the ground state bandgap energy and the X-ray diffraction measurements determine the layer thickness and mole fraction of the structures studied. Detailed modeling of the X-ray diffraction data is employed to quantify unintentional incorporation of approximately 1% Sb into the InAs layers of the superlattices. A Kronig-Penney model of the superlattice miniband structure is used to analyze the valence band offset between InAs and InAsSb, and hence the InAsSb band edge positions at each mole fraction. The resulting composition dependence of the bandgap energy and band edge positions of InAsSb are described using the bandgap bowing model; the respective low and room temperature bowing parameters for bulk InAsSb are 938 and 750 meV for the bandgap, 558 and 383 meV for the conduction band, and -380 and -367 meV for the valence band. [ABSTRACT FROM AUTHOR]

Published
2015
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11. Business model innovation: a temporal perspective

Author

Riordan, N. O., O Reilly, P., Aidan Duane, and Andreev, P.

Subjects
NONE OF THESE
Abstract

Recent years have seen an explosion in the number of academic and practitioner-oriented publications on business models and business model innovation. Indeed, companies that traditionally focused on product and service innovation, are turning toward business model innovation as an alternative or complement to product or process innovation. Nevertheless, companies struggle to innovate the business models through which commercialisable new ideas and technologies will pass. At the same time, the literature remains skewed toward product and process innovation rather than business model innovation. This paper highlights the need for a temporal view of the business model innovation process and proposes a conceptual model of the business model innovation process to enable organizations to identify, model and prioritise potential business models for their technological innovation . It also develops a prioritisation framework to be used for ranking alternative business models, which serves as an input towards developing an IT-based business model decision support system.

Published
2014

18. Differential Effect of Alpha-lipoic Acid on Healthy Peripheral Blood Lymphocytes and Leukemic Cells.

Author

Mikirova, N. A., Jackson, J. A., and Riordan, N.

Subjects
LIPOIC acid, CELL lines, LYMPHOCYTES, FATTY acids, LEUKEMIA
Abstract

The article focuses on the study which reveals the differential effect of lipoic acid (LA) or also known as alpha-lipoic acid on healthy peripheral blood lymphocytes and leukemic cells. It mentions that LA is a sulfur-containing fatty acid that is found inside every cell of the body where it helps to regenerate the energy that keeps cells alive and functioning. It is found out that LA is preferentially cytoxic to the leukemic cell lines and may be considered for the treatment of leukemia.

Published
2008

22. The King is Dead, Long Live the King: Entering A New Era of Stem Cell Research and Clinical Development

Author

Ichim Thomas, Riordan Neil H, and Stroncek David F

Subjects
Medicine
Abstract

Abstract In mid November the biopharma industry was shocked by the announcement from Geron that they were ending work on embryonic stem cell research and therapy. For more than 10 years the public image of all stem cell research has been equated with embryonic stem cells. Unfortunately, a fundamentally important medical and financial fact was being ignored: embryonic stem cell therapy is extremely immature. In parallel to efforts in embryonic stem cell research and development, scientists and physicians in the field of adult stem cells realized that the natural role of adult stem cells in the body is to promote healing and to act like endogenous "repair cells" and, as a result, numerous companies have entered the field of adult stem cell therapy with the goal of expanding numbers of adult stem cells for administration to patients with various conditions. In contrast to embryonic stem cells, which are extremely expensive and potentially dangerous, adult cell cells are inexpensive and have an excellent safety record when used in humans. Many studies are now showing that adult stem cells are practical, patient-applicable, therapeutics that are very close to being available for incorporation into the practice of medicine. These events signal the entrance of the field of stem cells into a new era: an era where hype and misinformation no longer triumph over economic and medical realities.

Published
2011
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23. Intravenous ascorbic acid to prevent and treat cancer-associated sepsis?

Author

Bogin Vladimir, Ancans Janis, Dasanu Constantin A, Alexandrescu Doru T, Miranda-Massari Jorge R, Gonzalez Michael J, Jackson James A, Mikirova Nina A, Hunninghake Ron, Luna Brandon, Braciak Todd, Minev Boris, Ichim Thomas E, Stevens R Brian, Markosian Boris, Koropatnick James, Chen Chien-Shing, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract The history of ascorbic acid (AA) and cancer has been marked with controversy. Clinical studies evaluating AA in cancer outcome continue to the present day. However, the wealth of data suggesting that AA may be highly beneficial in addressing cancer-associated inflammation, particularly progression to systemic inflammatory response syndrome (SIRS) and multi organ failure (MOF), has been largely overlooked. Patients with advanced cancer are generally deficient in AA. Once these patients develop septic symptoms, a further decrease in ascorbic acid levels occurs. Given the known role of ascorbate in: a) maintaining endothelial and suppression of inflammatory markers; b) protection from sepsis in animal models; and c) direct antineoplastic effects, we propose the use of ascorbate as an adjuvant to existing modalities in the treatment and prevention of cancer-associated sepsis.

Published
2011
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24. Prevention of hyperglycemia-induced myocardial apoptosis by gene silencing of Toll-like receptor-4

Author

Singh Manpreet, Shunnar Aminah, Lai Xiaoyan, Cheng Xiaoshu, Jiang Nan, Zhang Xusheng, Zheng Xiufen, Zhu Huaqing, Peng Tianqing, Zhang Yuwei, Riordan Neil, Bogin Vladimir, Tong Nanwei, and Min Wei-Ping

Subjects
Medicine
Abstract

Abstract Background Apoptosis is an early event involved in cardiomyopathy associated with diabetes mellitus. Toll-like receptor (TLR) signaling triggers cell apoptosis through multiple mechanisms. Up-regulation of TLR4 expression has been shown in diabetic mice. This study aimed to delineate the role of TLR4 in myocardial apoptosis, and to block this process through gene silencing of TLR4 in the myocardia of diabetic mice. Methods Diabetes was induced in C57/BL6 mice by the injection of streptozotocin. Diabetic mice were treated with 50 μg of TLR4 siRNA or scrambled siRNA as control. Myocardial apoptosis was determined by TUNEL assay. Results After 7 days of hyperglycemia, the level of TLR4 mRNA in myocardial tissue was significantly elevated. Treatment of TLR4 siRNA knocked down gene expression as well as diminished its elevation in diabetic mice. Apoptosis was evident in cardiac tissues of diabetic mice as detected by a TUNEL assay. In contrast, treatment with TLR4 siRNA minimized apoptosis in myocardial tissues. Mechanistically, caspase-3 activation was significantly inhibited in mice that were treated with TLR4 siRNA, but not in mice treated with control siRNA. Additionally, gene silencing of TLR4 resulted in suppression of apoptotic cascades, such as Fas and caspase-3 gene expression. TLR4 deficiency resulted in inhibition of reactive oxygen species (ROS) production and NADPH oxidase activity, suggesting suppression of hyperglycemia-induced apoptosis by TLR4 is associated with attenuation of oxidative stress to the cardiomyocytes. Conclusions In summary, we present novel evidence that TLR4 plays a critical role in cardiac apoptosis. This is the first demonstration of the prevention of cardiac apoptosis in diabetic mice through silencing of the TLR4 gene.

Published
2010
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25. Safety evaluation of allogeneic umbilical cord blood mononuclear cell therapy for degenerative conditions

Author

Luo Xiao-Ling, Zhang Min, Minev Boris, Min Wei-Ping, Wu Fang, Zhang Yun, Yang Wan-Zhang, Ramos Famela, Ichim Thomas E, Riordan Neil H, and Hu Xiang

Subjects
Medicine
Abstract

Abstract Background The current paradigm for cord blood transplantation is that HLA matching and immune suppression are strictly required to prevent graft versus host disease (GVHD). Immunological arguments and historical examples have been made that the use of cord blood for non-hematopoietic activities such as growth factor production, stimulation of angiogenesis, and immune modulation may not require matching or immune suppression. Methods 114 patients suffering from non-hematopoietic degenerative conditions were treated with non-matched, allogeneic cord blood. Doses of 1-3 × 107 cord blood mononuclear cells per treatment, with 4-5 treatments both intrathecal and intravenously were performed. Adverse events and hematological, immunological, and biochemical parameters were analyzed for safety evaluation. Results No serious adverse effects were reported. Hematological, immunological, and biochemical parameters did not deviate from normal ranges as a result of therapy. Conclusion The current hematology-based paradigm of need for matching and immune suppression needs to be revisited when cord blood is used for non-hematopoietic regenerative purposes in immune competent recipients.

Published
2010
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26. Nutraceutical augmentation of circulating endothelial progenitor cells and hematopoietic stem cells in human subjects

Author

Minev Boris, Swindlehurst Cathy A, Chan Kyle WH, Kenyon Julian, Hunninghake Ron, Jackson James A, Mikirova Nina A, Patel Amit N, Murphy Michael P, Smith Leonard, Ramos Famela, Ichim Thomas E, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract The medical significance of circulating endothelial or hematopoietic progenitors is becoming increasing recognized. While therapeutic augmentation of circulating progenitor cells using G-CSF has resulted in promising preclinical and early clinical data for several degenerative conditions, this approach is limited by cost and inability to perform chronic administration. Stem-Kine is a food supplement that was previously reported to augment circulating EPC in a pilot study. Here we report a trial in 18 healthy volunteers administered Stem-Kine twice daily for a 2 week period. Significant increases in circulating CD133 and CD34 cells were observed at days 1, 2, 7, and 14 subsequent to initiation of administration, which correlated with increased hematopoietic progenitors as detected by the HALO assay. Augmentation of EPC numbers in circulation was detected by KDR-1/CD34 staining and colony forming assays. These data suggest Stem-Kine supplementation may be useful as a stimulator of reparative processes associated with mobilization of hematopoietic and endothelial progenitors.

Published
2010
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27. Circulating endothelial progenitor cells: a new approach to anti-aging medicine?

Author

Patel Amit N, Minev Boris, Swindlehurst Cathy A, Chan Kyle WH, Kenyon Julian, Hunninghake Ron, Jackson James A, Mikirova Nina A, Murphy Michael P, Smith Leonard, Alexandrescu Doru T, Ichim Thomas E, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract Endothelial dysfunction is associated with major causes of morbidity and mortality, as well as numerous age-related conditions. The possibility of preserving or even rejuvenating endothelial function offers a potent means of preventing/treating some of the most fearful aspects of aging such as loss of mental, cardiovascular, and sexual function. Endothelial precursor cells (EPC) provide a continual source of replenishment for damaged or senescent blood vessels. In this review we discuss the biological relevance of circulating EPC in a variety of pathologies in order to build the case that these cells act as an endogenous mechanism of regeneration. Factors controlling EPC mobilization, migration, and function, as well as therapeutic interventions based on mobilization of EPC will be reviewed. We conclude by discussing several clinically-relevant approaches to EPC mobilization and provide preliminary data on a food supplement, Stem-Kine, which enhanced EPC mobilization in human subjects.

Published
2009
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28. Non-expanded adipose stromal vascular fraction cell therapy for multiple sclerosis

Author

Rodriguez Jorge, Alfaro Miguel, Lara Fabian, Solano Fabio, Wang Hao, Min Wei-Ping, Ichim Thomas E, Riordan Neil H, Harman Robert J, Patel Amit N, Murphy Michael P, Lee Roland R, and Minev Boris

Subjects
Medicine
Abstract

Abstract The stromal vascular fraction (SVF) of adipose tissue is known to contain mesenchymal stem cells (MSC), T regulatory cells, endothelial precursor cells, preadipocytes, as well as anti-inflammatory M2 macrophages. Safety of autologous adipose tissue implantation is supported by extensive use of this procedure in cosmetic surgery, as well as by ongoing studies using in vitro expanded adipose derived MSC. Equine and canine studies demonstrating anti-inflammatory and regenerative effects of non-expanded SVF cells have yielded promising results. Although non-expanded SVF cells have been used successfully in accelerating healing of Crohn's fistulas, to our knowledge clinical use of these cells for systemic immune modulation has not been reported. In this communication we discuss the rationale for use of autologous SVF in treatment of multiple sclerosis and describe our experiences with three patients. Based on this rationale and initial experiences, we propose controlled trials of autologous SVF in various inflammatory conditions.

Published
2009
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29. Feasibility investigation of allogeneic endometrial regenerative cells

Author

Reid Michael, Woods Erik J, Min Wei-Ping, Wang Hao, Riordan Neil H, Ichim Thomas E, Patel Amit N, Zhong Zhaohui, Mansilla Eduardo, Marin Gustavo H, Drago Hugo, Murphy Michael P, and Minev Boris

Subjects
Medicine
Abstract

Abstract Endometrial Regenerative Cells (ERC) are a population of mesenchymal-like stem cells having pluripotent differentiation activity and ability to induce neoangiogenesis. In vitro and animal studies suggest ERC are immune privileged and in certain situations actively suppress ongoing immune responses. In this paper we describe the production of clinical grade ERC and initial safety experiences in 4 patients with multiple sclerosis treated intravenously and intrathecally. The case with the longest follow up, of more than one year, revealed no immunological reactions or treatment associated adverse effects. These preliminary data suggest feasibility of clinical ERC administration and support further studies with this novel stem cell type.

Published
2009
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30. Anti-angiogenic effect of high doses of ascorbic acid

Author

Ichim Thomas E, Mikirova Nina A, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract Pharmaceutical doses of ascorbic acid (AA, vitamin C, or its salts) have been reported to exert anticancer activity in vitro and in vivo. One proposed mechanism involves direct cytotoxicity mediated by accumulation of ascorbic acid radicals and hydrogen peroxide in the extracellular environment of tumor cells. However, therapeutic effects have been reported at concentrations insufficient to induce direct tumor cell death. We hypothesized that AA may exert anti-angiogenic effects. To test this, we expanded endothelial progenitor cells (EPCs) from peripheral blood and assessed, whether or not high dose AA would inhibit EPC ability to migrate, change energy metabolism, and tube formation ability. We also evaluated the effects of high dose AA on angiogenic activities of HUVECs (human umbilical vein endothelial cells) and HUAECs (human umbilical arterial endothelial cells). According to our data, concentrations of AA higher than 100 mg/dl suppressed capillary-like tube formation on Matrigel for all cells tested and the effect was more pronounced for progenitor cells in comparison with mature cells. Co-culture of differentiated endothelial cells with progenitor cells showed that there was incorporation of EPCs in vessels formed by HUVECs and HUAECs. Cell migration was assessed using an in vitro wound healing model. The results of these experiments showed an inverse correlation between AA concentrations relative to both cell migration and gap filling capacity. Suppression of NO (nitric oxide) generation appeared to be one of the mechanisms by which AA mediated angiostatic effects. This study supports further investigation into non-cytotoxic antitumor activities of AA.

Published
2008
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31. Allogeneic endometrial regenerative cells: An 'Off the shelf solution' for critical limb ischemia?

Author

Marleau Annette M, Chan Kyle, Angle Niren, Kambhampati Suman, Patel Amit N, Wang Hao, Murphy Michael P, Pyszniak Andrew, Carrier Ewa, Ichim Thomas E, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract Critical limb ischemia (CLI) is an advanced form of peripheral artery disease which is responsible for approximately 100,000 amputations per year in the US. Trials to date have reported clinical improvement and reduced need for amputation in CLI patients receiving autologous bone marrow or mobilized peripheral blood stem cells for stimulation of angiogenesis. While such treatments are currently entering Phase III trials, practical and scientific pitfalls will limit widespread implementation if efficacy is proven. Hurdles to be overcome include: a) reduced angiogenic potential of autologous cells in aged patients with cardiovascular risk factors; b) invasiveness/adverse effects of bone marrow extraction and G-CSF mobilization, respectively; and c) need for on-site cellular manipulation. The Endometrial Regenerative Cell (ERC) is a mesenchymal-like stem cell derived from the menstrual blood that is believed to be associated with endometrial angiogenesis. We discuss the possibility of using allogeneic ERCs as an "off the shelf" treatment for CLI based on the following properties: a) High levels of growth factors and matrix metalloprotease production; b) Ability to inhibits inflammatory responses and lack of immunogenicity; and c) Expandability to great quantities without loss of differentiation ability or karyotypic abnormalities.

Published
2008
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32. Exosomes as a tumor immune escape mechanism: possible therapeutic implications

Author

Hanley Harold H, Joyce James A, Hao Xishan, Ren Xiubao, Zheng Xiufen, Kaushal Shalesh, Zhong Zhaohui, Ichim Thomas E, Riordan Neil H, Koropatnick James, Bogin Vladimir, Minev Boris R, Min Wei-Ping, and Tullis Richard H

Subjects
Medicine
Abstract

Abstract Advances in cancer therapy have been substantial in terms of molecular understanding of disease mechanisms, however these advances have not translated into increased survival in the majority of cancer types. One unsolved problem in current cancer therapeutics is the substantial immune suppression seen in patients. Conventionally, investigations in this area have focused on antigen-nonspecific immune suppressive molecules such as cytokines and T cell apoptosis inducing molecules such as Fas ligand. More recently, studies have demonstrated nanovesicle particles termed exosomes are involved not only in stimulation but also inhibition of immunity in physiological conditions. Interestingly, exosomes secreted by cancer cells have been demonstrated to express tumor antigens, as well as immune suppressive molecules such as PD-1L and FasL. Concentrations of exosomes from plasma of cancer patients have been associated with spontaneous T cell apoptosis, which is associated in some situations with shortened survival. In this paper we place the "exosome-immune suppression" concept in perspective of other tumor immune evasion mechanisms. We conclude by discussing a novel therapeutic approach to cancer immune suppression by extracorporeal removal of exosomes using hollow fiber filtration technology

Published
2008
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33. Endometrial regenerative cells: A novel stem cell population

Author

Ge Wei, Wang Hao, Jackson James, Yin Zhenglian, Rogers Andrea, Zhong Jie, Ichim Thomas E, Meng Xiaolong, Bogin Vladimir, Chan Kyle W, Thébaud Bernard, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract Angiogenesis is a critical component of the proliferative endometrial phase of the menstrual cycle. Thus, we hypothesized that a stem cell-like population exist and can be isolated from menstrual blood. Mononuclear cells collected from the menstrual blood contained a subpopulation of adherent cells which could be maintained in tissue culture for >68 doublings and retained expression of the markers CD9, CD29, CD41a, CD44, CD59, CD73, CD90 and CD105, without karyotypic abnormalities. Proliferative rate of the cells was significantly higher than control umbilical cord derived mesenchymal stem cells, with doubling occurring every 19.4 hours. These cells, which we termed "Endometrial Regenerative Cells" (ERC) were capable of differentiating into 9 lineages: cardiomyocytic, respiratory epithelial, neurocytic, myocytic, endothelial, pancreatic, hepatic, adipocytic, and osteogenic. Additionally, ERC produced MMP3, MMP10, GM-CSF, angiopoietin-2 and PDGF-BB at 10–100,000 fold higher levels than two control cord blood derived mesenchymal stem cell lines. Given the ease of extraction and pluripotency of this cell population, we propose ERC as a novel alternative to current stem cells sources.

Published
2007
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34. Stem Cell Therapy for Autism

Author

Smith Leonard, Morales Frank, Glenn Eduardo, Solano Fabio, Ichim Thomas E, Zabrecky George, and Riordan Neil H

Subjects
Medicine
Abstract

Abstract Autism spectrum disorders (ASD) are a group of neurodevelopmental conditions whose incidence is reaching epidemic proportions, afflicting approximately 1 in 166 children. Autistic disorder, or autism is the most common form of ASD. Although several neurophysiological alterations have been associated with autism, immune abnormalities and neural hypoperfusion appear to be broadly consistent. These appear to be causative since correlation of altered inflammatory responses, and hypoperfusion with symptology is reported. Mesenchymal stem cells (MSC) are in late phases of clinical development for treatment of graft versus host disease and Crohn's Disease, two conditions of immune dysregulation. Cord blood CD34+ cells are known to be potent angiogenic stimulators, having demonstrated positive effects in not only peripheral ischemia, but also in models of cerebral ischemia. Additionally, anecdotal clinical cases have reported responses in autistic children receiving cord blood CD34+ cells. We propose the combined use of MSC and cord blood CD34+cells may be useful in the treatment of autism.

Published
2007
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35. Cord blood in regenerative medicine: do we need immune suppression?

Author

Marleau Annette M, Chan Kyle, Riordan Neil H, and Ichim Thomas E

Subjects
Medicine
Abstract

Abstract Cord blood is currently used as an alternative to bone marrow as a source of stem cells for hematopoietic reconstitution after ablation. It is also under intense preclinical investigation for a variety of indications ranging from stroke, to limb ischemia, to myocardial regeneration. A major drawback in the current use of cord blood is that substantial morbidity and mortality are associated with pre-transplant ablation of the recipient hematopoietic system. Here we raise the possibility that due to unique immunological properties of both the stem cell and non-stem cell components of cord blood, it may be possible to utilize allogeneic cells for regenerative applications without needing to fully compromise the recipient immune system. Issues raised will include: graft versus host potential, the immunogeneicity of the cord blood graft, and the parallels between cord blood transplantation and fetal to maternal trafficking. The previous use of unmatched cord blood in absence of any immune ablation, as well as potential steps for widespread clinical implementation of allogeneic cord blood grafts will also be discussed.

Published
2007
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36. Therapeutic use of Aldara™ in chronic myeloid leukemia

Author

Marleau Annette M, Lipton Jeffrey H, Riordan Neil H, and Ichim Thomas E

Subjects
Medicine
Abstract

Abstract The potent clinical responses seen in patients with chronic myeloid leukemia (CML) after administration of donor-specific lymphocytes, as well as the correlation between the presence of antigen specific T cells and prolonged remission in these patients, suggests a role for the immunological control of CML. Here we propose Aldara™, a clinically used formulation of imiquimod, as an agent for augmenting immune responses to CML antigens. Our proposition is based upon 3 tenets: 1) Endogenous dendritic cells (DC) of CML patients, which are known to be derived from the malignant clone, express and present various leukemic antigens; 2) CML-antigen reactive T cell clones exist in the patient but in many situations are ineffectively stimulated to cause significant hematological responses; and 3) Antigen presentation by mature, activated DC, which endogenously express CML-antigens may endow the pre-existing ineffective T cell responses with ability to control CML progression. The practical use of Aldara™ as a localized activator of DC in the context of present day leukemic therapeutics, as well as various properties of this unique immune modulator will be discussed.

Published
2007
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37. Induction of antitumor immunity through xenoplacental immunization

Author

Agadjanyan Michael G, Szczurko Orest M, Sher Salman, Yijian Li, Izadi Hamid, Riordan Neil H, Popov Igor A, Kusznieruk Kornel P, Zhong Zhaohui, Tullis Richard H, Harandi Amir, Reznik Boris N, Mamikonyan Grigor V, and Ichim Thomas E

Subjects
Medicine
Abstract

Abstract Historically cancer vaccines have yielded suboptimal clinical results. We have developed a novel strategy for eliciting antitumor immunity based upon homology between neoplastic tissue and the developing placenta. Placenta formation shares several key processes with neoplasia, namely: angiogenesis, activation of matrix metalloproteases, and active suppression of immune function. Immune responses against xenoantigens are well known to break self-tolerance. Utilizing xenogeneic placental protein extracts as a vaccine, we have successfully induced anti-tumor immunity against B16 melanoma in C57/BL6 mice, whereas control xenogeneic extracts and B16 tumor extracts where ineffective, or actually promoted tumor growth, respectively. Furthermore, dendritic cells were able to prime tumor immunity when pulsed with the placental xenoantigens. While vaccination-induced tumor regression was abolished in mice depleted of CD4 T cells, both CD4 and CD8 cells were needed to adoptively transfer immunity to naïve mice. Supporting the role of CD8 cells in controlling tumor growth are findings that only freshly isolated CD8 cells from immunized mice were capable of inducing tumor cell caspases-3 activation ex vivo. These data suggest feasibility of using xenogeneic placental preparations as a multivalent vaccine potently targeting not just tumor antigens, but processes that are essential for tumor maintenance of malignant potential.

Published
2006
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38. A novel method of modifying immune responses by vaccination with lipiodol-siRNA mixtures

Author

Yijian Li, Zhong Zaohui, Izadi Hamid, Riordan Neil H, Popov Igor A, Ichim Thomas E, Sher Salman, and Oleinik Eugenia K

Subjects
Medicine
Abstract

Abstract The dendritic cell (DC) possesses the ability to stimulate both T helper 1 (Th1) and Th2 responses depending on activation stimuli. Although it is known that chemically or genetically modified DC can be used therapeutically to steer immune responses towards either Th1 or Th2, cellular therapy with ex vivo manipulated DC is clinically difficult. Here we demonstrate a novel method of switching immune responses from Th1 to Th2 through in vivo immune modulation by administration of siRNA. We demonstrate that siRNA targeting of the IL-12p35 gene leads to a Th2 bias in vitro through an IL-10 dependent mechanism. In vivo administration of siRNA admixed with the oil-based contrast agent lipiodol in the presence of antigen and adjuvant induced a deviation in recall response to reduced production of IFN-γ and augmented IL-4 response using either KLH or ovalbumin. This simple method of in vivo modification of immune response possesses therapeutic potential in Th1-mediated diseases such as multiple sclerosis and autoimmune diabetes.

Published
2006
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39. "I'm not being serviced; I'm being cared for": A mixed methods study of patients' and nurses' perceptions of community oncology nursing delivered by a Community Intervention Team.

Author

O'Connor Power F, Beatty S, Dunne N, O'Connell L, O' Riordan N, Sloane H, Prizeman G, O'Sullivan K, Butler É, Howlin C, and Byrne G

Subjects
Attitude of Health Personnel, Hospitals, Humans, Oncology Nursing, Patient Satisfaction, Neoplasms therapy, Nurses
Abstract

Purpose: Many patients do not have access to community oncology nursing care in a primary setting and are completely reliant on tertiary hospital care. The aim of this study is to gain an understanding of oncology patients' and nurses' perceptions of community oncology nursing, delivered by an urban Community Intervention Team (CIT) in Ireland., Methods: A descriptive, concurrent mixed methods approach was used which included semi-structured interviews with 14 oncology patients and an online survey of 27 hospital and community nurses. Thematic analysis and descriptive statistics were used to analyse the data., Results: Six broad themes captured patients' views. Right care related to patients' satisfaction with the range of care available. Right place reflected positive views of the physical setting and the option for homecare for those that needed it. Right time represented patients' comments about the increased appointment efficiency, flexibility, and availability of the service out-of-hours, compared to hospital-based care. Right people was based on patients' portrayals of community cancer nurses as professional, confident, friendly, reassuring and relatable. Integration and communication reflected the communication between the services and patients' impressions of how the services were integrated together. The last theme was improvements to the CIT service. Hospital nurses reported satisfaction with the CIT service while CIT nurses responses suggest the need for better communication with hospital partners., Conclusion: Patients had positive perceptions of the service provided by the CIT. Both hospital and community cancer nurses were satisfied with the service and reported that they would like to see an expansion of community oncology nursing services delivered by the CIT., (Copyright © 2022. Published by Elsevier Ltd.)

Published
2022
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40. Cellular immunotherapy of cancer: an overview and future directions.

Author

Tao Z, Li S, Ichim TE, Yang J, Riordan N, Yenugonda V, Babic I, and Kesari S

Subjects
Animals, Dendritic Cells immunology, Genetic Therapy, Humans, Lymphocyte Activation, Lymphocytes, Tumor-Infiltrating immunology, Neoplasms immunology, RNA Interference, Repressor Proteins, T-Lymphocytes immunology, Tumor Microenvironment, Dendritic Cells transplantation, Immunotherapy, Adoptive methods, Lymphocytes, Tumor-Infiltrating transplantation, Neoplasms therapy, Receptors, Steroid genetics, T-Lymphocytes transplantation
Abstract

The clinical success of checkpoint inhibitors has led to a renaissance of interest in cancer immunotherapies. In particular, the possibility of ex vivo expanding autologous lymphocytes that specifically recognize tumor cells has attracted much research and clinical trial interest. In this review, we discuss the historical background of tumor immunotherapy using cell-based approaches, and provide some rationale for overcoming current barriers to success of autologous immunotherapy. An overview of adoptive transfer of lymphocytes, tumor infiltrating lymphocytes and dendritic cell therapies is provided. We conclude with discussing the possibility of gene-manipulating immune cells in order to augment therapeutic activity, including silencing of the immune-suppressive zinc finger orphan nuclear receptor, NR2F6, as an attractive means of overcoming tumor-associated immune suppression.

Published
2017
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41. High-Dose Intravenous Vitamin C Treatment of a Child with Neurofibromatosis Type 1 and Optic Pathway Glioma: A Case Report.

Author

Mikirova N, Hunnunghake R, Scimeca RC, Chinshaw C, Ali F, Brannon C, and Riordan N

Subjects
Child, Preschool, Dose-Response Relationship, Drug, Humans, Injections, Intravenous, Magnetic Resonance Imaging, Male, Neurofibromatosis 1 complications, Neurofibromatosis 1 diagnosis, Optic Nerve Glioma complications, Optic Nerve Glioma diagnosis, Vitamins administration & dosage, Ascorbic Acid administration & dosage, Neurofibromatosis 1 drug therapy, Optic Nerve Glioma drug therapy
Abstract

BACKGROUND In neurofibromatosis type 1 (NF1) disease, the loss of the tumor suppressor function of the neurofibromin gene leads to proliferation of neural tumors. In children, the most frequently identified tumor is the optic pathway glioma. CASE REPORT We describe the case of a 5-year-old child who was diagnosed with NF1 and optic pathway tumor onset at the age of 14 months. Because of the tumor progression, chemotherapy with carboplatin and vincristine was prescribed at this early age and continued for one year. As the progression of disease continued after chemotherapy, the child, at the age of 2.8 years, was started on high-dose intravenous vitamin C (IVC) treatment (7-15 grams per week) for 30 months. After 30 months, the results of IVC treatments demonstrated reduction and stabilization of the tumors in the optic chiasm, hypothalamus, and left optic nerve according to radiographic imaging. The right-sided optic nerve mass seen before IVC treatment disappeared by the end of the treatment. CONCLUSIONS This case highlights the positive effects of treating NF1 glioma with IVC. Additional studies are necessary to evaluate the role of high-dose IVC in glioma treatment., Competing Interests: Conflicts of Interest: None declared

Published
2016
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42. Modulation of Cytokines in Cancer Patients by Intravenous Ascorbate Therapy.

Author

Mikirova N, Riordan N, and Casciari J

Subjects
Adult, Antineoplastic Agents administration & dosage, Ascorbic Acid administration & dosage, Biomarkers, Tumor metabolism, Case-Control Studies, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Inflammation, Infusions, Intravenous, Male, Middle Aged, Neoplasms drug therapy, Neovascularization, Pathologic, Proto-Oncogene Proteins c-myc metabolism, Up-Regulation, ras Proteins metabolism, Ascorbic Acid therapeutic use, Cytokines metabolism, Neoplasms metabolism
Abstract

Background: Cytokines play an important role in tumor angiogenesis and inflammation. There is evidence in the literature that high doses of ascorbate can reduce inflammatory cytokine levels in cancer patients. The objective of this study was to investigate the effect of treatment by intravenous vitamin C (IVC) on cytokines and tumor markers., Material/methods: With the availability of protein array kits allowing assessment of many cytokines in a single sample, we measured 174 cytokines and additional 54 proteins and tumor markers in 12 cancer patients before and after a series of IVC treatments., Results: Presented results show for our 12 patients the effect of treatment resulted in normalization of many cytokine levels. Cytokines that were most consistently elevated prior to treatments included M-CSF-R, Leptin, EGF, FGF-6, TNF-α, β, TARC, MCP-1,4, MIP, IL-4, 10, IL-4, and TGF-β. Cytokine levels tended to decrease during the course of treatment. These include mitogens (EGF, Fit-3 ligand, HGF, IGF-1, IL-21R) and chemo-attractants (CTAC, Eotaxin, E-selectin, Lymphotactin, MIP-1, MCP-1, TARC, SDF-1), as well as inflammation and angiogenesis factors (FGF-6, IL-1β, TGF-1)., Conclusions: We are able to show that average z-scores for several inflammatory and angiogenesis promoting cytokines are positive, indicating that they are higher than averages for healthy controls, and that their levels decreased over the course of treatment. In addition, serum concentrations of tumor markers decreased during the time period of IVC treatment and there were reductions in cMyc and Ras, 2 proteins implicated in being upregulated in cancer.

Published
2016
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43. Metabolic correction: a functional biochemical mechanism against disease--Part 1: concept and historical background.

Author

González MJ, Miranda-Massari JR, Duconge J, Allende-Vigo MZ, Jiménez-Ramírez FJ, Cintrón K, Rodríguez-Gómez JR, Rosario G, Ricart C, Santiago-Cornier JA, Zaragoza-Urdaz R, Vázquez A, Hickey S, Jabbar-Berdiel M, Riordan N, Ichim T, Santiago O, Alvarado G, and Vora P

Subjects
Food, Genetic Variation, Humans, Metabolic Diseases genetics, Minerals metabolism, Vitamins metabolism, Enzymes metabolism, Metabolic Diseases physiopathology, Micronutrients metabolism
Abstract

Human physiology depends on countless biochemical reactions, numerous of which are co-dependent and interrelated. The speed and level of completion of reactions usually depend on the availability of precursors and enzymes. The enzymatic activity depends on the bioavailability of micronutrient cofactors such as vitamins and minerals. In order to achieve a healthy physiological state, the organism requires that biochemical reactions occur at a controlled rate. To achieve this state it is required that metabolic reactions reach what can be considered an optimal metabolic equilibrium. A combination of genetic makeup, dietary patterns, trauma, disease, toxins, medications, and environmental stressors can elevate the demand for the nutrients needed to reach this optimal metabolic equilibrium. In this, part 1, the general concept of metabolic correction is presented with an elaboration explaining how this concept is increasing in importance as we become aware of the presence of genetic variants that affect enzymatic reactions causing metabolic disturbances that themselves favor or promote the disease state. In addition, part 1 reviews how prominent scientists have contributed in fundamental ways to our understanding of the importance of micronutrients in health and disease and in the development of the metabolic correction concept.

Published
2015

44. Clinical experience with intravenous administration of ascorbic acid: achievable levels in blood for different states of inflammation and disease in cancer patients.

Author

Mikirova N, Casciari J, Riordan N, and Hunninghake R

Subjects
Administration, Intravenous, Adult, Aged, Aged, 80 and over, Ascorbic Acid blood, Biomarkers, Tumor metabolism, C-Reactive Protein metabolism, Female, Humans, Male, Middle Aged, Ascorbic Acid administration & dosage, Ascorbic Acid therapeutic use, Inflammation blood, Inflammation drug therapy, Neoplasms blood, Neoplasms drug therapy
Abstract

Background: Ascorbic acid (vitamin C, ascorbate) is a key water soluble antioxidant that, when administered in doses well above its recommended dietary allowance, may have preventative and therapeutic value against a number of pathologies. The intravenous administration of high dose ascorbate (IVC) has increased in popularity among complementary and alternative medicine practitioners: thousands of patients received IVC, at an average dose of 0.5 g/kg, without significant side effects. While IVC may have a variety of possible applications, it has generated the most interest for its potential use in treating cancer., Methods: Medical records of patients with cancer treated with IVC at the Riordan Clinic were retrospectively reviewed. Cancer patients, for whom plasma ascorbate concentration data before and after treatment were available, along with C-reactive protein (CRP) measurements, were chosen for analysis., Results: The results of the analysis can be summarized as follows. IVC produces peak plasma ascorbate concentrations on the order of ten millimolars with lower peak plasma concentrations obtained in cancer patients as compared to healthy subjects. Cancer patients who are deficient in vitamin C prior to therapy tend to achieve lower plasma levels post infusion. High inflammation or tumor burdens, as measured by CRP or tumor antigen levels, tend to lower peak plasma ascorbate levels after IVC. When compared to patients with localized tumors, patients with metastatic tumors tend to achieve lower post infusion plasma ascorbate concentrations., Conclusions: The data indicate that, while potentially therapeutic plasma ascorbate concentrations can be achieved with IVC, levels attained will vary based on tumor burden and degree of inflammation (among other factors). Evidence suggests that IVC may be able to modulate inflammation, which in turn might improve outcomes for cancer patients. IVC may serve as a safe, adjunctive therapy in clinical cancer care.

Published
2013
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45. Vitamin D concentrations, endothelial progenitor cells, and cardiovascular risk factors.

Author

Mikirova NA, Belcaro G, Jackson JA, and Riordan NH

Subjects
Adult, Aged, Antigens, CD34 biosynthesis, Blood Pressure, Cholesterol, HDL metabolism, Humans, Lipoproteins, LDL metabolism, Middle Aged, Risk Factors, Time Factors, Triglycerides metabolism, Cardiovascular Diseases drug therapy, Endothelial Cells cytology, Stem Cells cytology, Vitamin D blood
Abstract

Our study aimed to establish the association of vitamin D status with the level of circulating endothelial progenitor cells (EPCs) and circulating angiogenic cells (CACs) and to demonstrate the effect of vitamin D on the level of lipoproteins responsible for increased cardiovascular risk and high blood pressure. 41 healthy adults were selected. EPCs were defined as CD34+/KDR+ cells, and CACs were defined as cells that expressed endothelial markers after incubation of mononuclear blood cells with endothelial growth factors during 5 days. We found a positive association between EPCs, CACs and the level of vitamin D and an inverse correlation between several subclasses of lipoproteins. The level of vitamin D higher than 40 ng/ml demonstrated a positive effect on regulation of blood pressure, and there was significant difference in cholesterol/HDL ratio, very low-density lipoproteins, and triglycerides for groups of subjects with varying levels of vitamin D.

Published
2010

46. Circulating endothelial progenitor cells and erectile dysfunction: possibility of nutritional intervention?

Author

Ichim TE, Zhong Z, Mikirova NA, Jackson JA, Hunninghake R, Mansilla E, Marín G, Núñez L, Patel AN, Angle N, Murphy MP, Dasanu CA, Alexandrescu DT, Bogin V, and Riordan NH

Subjects
C-Reactive Protein metabolism, Granulocyte-Macrophage Colony-Stimulating Factor metabolism, Hematopoietic Stem Cell Mobilization methods, Humans, Inflammation, Male, Nutritional Sciences, Penis pathology, Treatment Outcome, Endothelial Cells cytology, Erectile Dysfunction drug therapy, Stem Cells cytology
Abstract

To provide an overview of molecular and cellular processes involved in erectile dysfunction (ED) with emphasis on circulating endothelial progenitor cells (EPC) and discuss possible nutraceutical means of intervention. A review of literature on Pubmed related to EPC and ED was conducted. Patients with ED appear to possess a reduced number of circulating EPC, which is associated with poor endothelial function possibly as a result of underlying low-grade inflammation. Several studies support the possibility of improving erectile function by inhibition of inflammation as well as administration of various stem cell types. One particularly interesting approach is nutraceutical supplementation to increase circulating EPC, as demonstrated in the product Stem-Kine. Interventions aimed at increasing circulating EPC may have potential in treatment of vascular ED.

Published
2010

47. The lysosomotropic agent, hydroxychloroquine, delivered in a biodegradable nanoparticle system, overcomes drug resistance of B-chronic lymphocytic leukemia cells in vitro.

Author

Mansilla E, Marin GH, Nuñez L, Drago H, Sturla F, Mertz C, Rivera L, Ichim T, Riordan N, and Raimondi C

Subjects
Cell Survival drug effects, Drug Delivery Systems, Drug Resistance, Neoplasm, Humans, Leukemia, Lymphocytic, Chronic, B-Cell pathology, Microscopy, Confocal, Spectrometry, Fluorescence, Hydroxychloroquine administration & dosage, Leukemia, Lymphocytic, Chronic, B-Cell drug therapy, Nanoparticles administration & dosage
Abstract

Nonviral delivery systems are relatively easy to produce in the large scale, are safe, and elicit a negligible immune response. Nanoparticles (NPs) offer promise as nonviral vectors as biocompatible and -degradable carriers of drugs with targeting to specific sites by surface receptors of monoclonal antibodies (mAbs). We investigated the effect of four PEG-PLGA (polyethylene glycol-polylactic-co-glycolic acid) NP systems on drug-resistant B-chronic lymphocytic leukemia (B-CLL) cells in vitro, three of them encapsulating the drug, hydroxylchloroquine (HDQ), two with NP surface coatings of mAbs (NP1) CD20, (NP2) CD19, and CD20, and one (NP3) with no mAb, but tagged with the fluorescent marker, fluorescein isothiocyanate. The fourth NP system (NP4) was coated with anti-CD19/FITC and anti-CD20/Alexa-Fluor((R)) antibodies, but did not contain the active drug, HCQ. Our data indicate that PEG-PLGA nanoparticles with surface mAbs are suitable for selective drug delivery to B-CLL cells and produce a strong apoptotic effect when loaded with the lysosomotropic agent, HDQ.

Published
2010
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48. Prevention of venous thrombosis in long-haul flights with Flite Tabs: the LONFLIT-FLITE randomized, controlled trial.

Author

Cesarone MR, Belcaro G, Nicolaides AN, Ricci A, Geroulakos G, Ippolito E, Brandolini R, Vinciguerra G, Dugall M, Griffin M, Ruffini I, Acerbi G, Corsi M, Riordan NH, Stuard S, Bavera P, Di Renzo A, Kenyon J, and Errichi BM

Subjects
Adult, Aerospace Medicine, Aged, Capsules, Drug Combinations, Edema etiology, Edema prevention & control, Exercise, Female, Fibrin Fibrinogen Degradation Products analysis, Fibrinogen analysis, Flavonoids adverse effects, Humans, Leg blood supply, Male, Middle Aged, Plant Extracts, Platelet Aggregation Inhibitors adverse effects, Risk Factors, Subtilisins adverse effects, Ultrasonography, Veins diagnostic imaging, Venous Thrombosis etiology, Venous Thrombosis physiopathology, Flavonoids administration & dosage, Platelet Aggregation Inhibitors administration & dosage, Subtilisins administration & dosage, Travel, Venous Thrombosis prevention & control
Abstract

The aim of this study was to evaluate the development of edema, and superficial and deep vein thrombosis (DVT) prophylaxis with an oral profibrinolytic agent (Flite Tabs, 150 mg pinokinase, Aidan, Tempe, AZ, USA) in long-haul flights (7-8 hours), in high-risk subjects. A group of 300 subjects was included; 76 were excluded for several problems including concomitant treatments; 204 were randomized into 2 groups (active treatment or placebo) to evaluate the effects of prophylaxis with Flite Tabs. An exercise program was used in both groups. The femoral, popliteal, tibial, and superficial veins were scanned with ultrasound before and within 90 minutes after flights. Of the included subjects, 92 of 103 controls and 94 of 101 treated subjects completed the study. Dropouts were due to connection problems. Age, gender, and risk distribution were comparable in the groups. In the treatment group, no DVT was observed. In the control group, 5 subjects (5.4%) had a DVT and there were 2 superficial thromboses (7 events in 92 subjects; 7.6%). At inclusion, edema was comparable in the 2 groups. After flights there was an increase in score in controls (+12%) in comparison with a decrease (-15%) in the Flite Tabs group (the difference in variation was statistically significant). Intention-to-treat analysis for thrombotic events shows 18 failures in controls (11 lost to follow-up + 7 thrombotic events) of 92 subjects (19.6%) in comparison with 7 failures (of 94 subjects, equivalent to 7.4%) in the treatment group (p < 0.05). Events were asymptomatic. In conclusion, Flite Tabs were effective in reducing thrombotic events and in controlling edema in high-risk subjects in long flights.

Published
2003
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49. Limb pain associated with an undiagnosed hemoglobinopathy and pseudononcyesis.

Author

Stevens-Simon C and Riordan N

Subjects
Adolescent, Female, Humans, Pregnancy, Recurrence, Risk Factors, Anemia, Sickle Cell complications, Anemia, Sickle Cell diagnosis, Arm, Leg, Pain etiology, Pregnancy Complications, Hematologic diagnosis, Pregnancy in Adolescence
Abstract

Over a 2-month period, a 16-yr-old African-American female presented with recurrent episodes of severe, migratory limb pain. Sickle cell C disease was ultimately diagnosed. She adamantly denied sexual activity but was found to be 28 weeks pregnant. Her limb pain was probably triggered by the metabolic and hemodynamic demands of pregnancy. The case illustrates the importance of thoroughly examining patients with recurrent, unexplained physical complaints.

Published
2002
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50. Retrospective analysis of the effects of low-dose, high frequency human growth hormone on serum lipids and prostate specific antigen.

Author

Chein E, Gonzalez MJ, and Riordan NH

Abstract

Background. Elevated serum total cholesterol (TC) and triglycerides (TG) are risk factors for atherosclerosis and ischemic heart disease. Adult growth hormone deficiency (AGHD) is associated with elevated TC and TG. Many treatment protocols for AGHD use relatively high doses of growth hormone (GH) given at low frequency, which is associated with increased incidences of edema, joint pains, and carpal tunnel syndrome. We have treated > 2200 patients using a low-dose high frequency (LDHF) dosing regimen of GH which results in similar beneficial subjective responses, and fewer of the side-effects associated with the higher-dosage treatment at a substantial cost savings. Clinically, in addition to increased insulin-like growth factor I (IGF-I), we observed lower TG and TC levels and no elevation of prostate specific antigen levels in treated patients. Methods. A retrospective analysis of IGF-I, TG, TC, and PSA data from our patient population was performed to test our hypothesis that positive objective responses of IGF-I, TG, and TC occur and that elevation of PSA does not occur in response to LDHF dosing regimen of GH. The mean duration of treatment of the analyzed data ranged from 181 to 259 days. Results. The mean plasma IGF-I level rose significantly (p<.00001) to a level 37% greater than baseline with treatment. TC and TG decreased significantly (p<.001) in those patients with elevated baseline values, and did not change significantly in those with normal baseline values. PSA concentrations decreased non-significantly during treatment, and few cases of edema, joint pain, or carpal tunnel were reported. Conclusions. Treatment of AGHD using the LDHF dosing regimen of GH resulted in significant increases in IGF-I, significant reductions in TC and TG levels in patients with elevated baseline values, no increase in PSA concentrations, and fewer side effects than other dosing regimens.

Published
2001
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