DOCSLIB.ORG

Physica Energetics' Quick Reference & Research Guide

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Physica Energetics' Quick Reference & Research Guide PHYSICA ENERGETICS’ QUICK REFERENCE & RESEARCH GUIDE BioToxicosis (60 mL/2 oz. Milieu Tinctures) Lymph 1 Acute TARGET Lymph/ECM drainage, excretion, acute reaction, inflammation INITIAL Lymph 2 Matrix TARGET Lymph/ECM drainage, xenobiotic accumulation, ground matrix disturbance, compensation DEEPER Lymph 3 Chronic TARGET Lymph/ECM drainage, de-compensation, rigid signals, degeneration DEEPEST Matrix Nutritionals 5-HTP Liposome Nanosphere Liposome Spray: Provides inhibitory neurotransmitter support, enhances serotonin, insomnia, improves mood, PMS, bipolar, fibromyalgia, depression, excessive appetite, carbohydrate cravings Acetyl L-Carnitine ADHD, Alzheimer’s, age related memory, transport fatty acids into the mitochondria of the cell Adrenal Life Force CFS, adrenal/thyroid axis, fatigue, depression, allergies, PMS Alkalize-C High Potency Buffered Vit C powder, alkalizing mineral drink, non-bowel tolerance, CFS, adrenal weakness Bio-A Curcumin Sustained release: Supports normal inflammatory response, down regulates COX-2 enzymes, inhibit TNFs (pro- Phytosome inflammatory cytokines), antioxidant, cardiac, IBS, Crohns, skin, Diabetes, increases bile flow, thins bile viscosity, hepato- protectant, Hypothyroid, allergies, arthritis, anti-oxidant, increases glutathione, free radical scavenger BioCatalase Nanosphere Liposome Lotion: Catalytic enzyme lotion: injuries, arthritis, musculo-skeletal, connective tissue, joints, Liposome Topical dermatitis, stings BioCell Salts Endocrine, mineralization, PMS/Menopause, CFS, energy BioHealth Matrix “Ultimate Daily Multiple”, Synergistic phyto-nutritional complex, amino acids, botanicals iron free multiple with additional endocrine and hormonal nutrition Bio-Omega 3 Unique, minimum 6.5:1 EPA/DHA ratio, anti-Inflammatory, prostaglandin precursors, anti-depressant, mood enhancer, calcium transport, brain function, ADD/ADHD, learning disorders, skin, thyroid support, digestive CataZyme-7 Digestive organic enzymes in a botanical base, for most digestive disorders with protease CataZyme-U Digestive organic enzymes in a soothing, mucilaginous, botanical base, gastrointestinal disorders, ulcers, gastritis, IBS, heals mucosal lining, allergies etc protease-free CoQ10 Liposome Nanosphere Liposome: Cardiac support, Mitochondrial support, gingivitis, periodontal disease, bio-films, immune fortifier, Tincture breast metabolism, increased oxygen to cell, obesity, clogged arteries, anti-aging, w/Vitamin E DHEA Liposomal Nanosphere Liposome: Hormonal insufficiencies, sexual function, adrenal fatigue, SLE, auto-immune Drops DIM Liposome Nanosphere Liposome: Estrogen metabolism in men/women, uterine, breast, prostate health, hormonal balance. Flora Syntropy “Right spinning” probiotic, survives antibiotics/gastric acids, exceptional bowel health/bacteria toxicity etc GALT Fortifier Gut Associated Lymphoid Tissue: Immune reconstituent, stimulates interlukin-2, cytokines & macrophage action, supports Peyers’ Patches, clears SI mucus, allergies GB-40 Yuan Source Gall bladder disorders, eg. bloating, belching, GERDS, digestive discomfort following meals, parasites Glutamine Complex Gastrointestinal problems, IBS, Dysbiosis, passive leaky gut, immune, infections, parasites, Crohns PLG-U Powder Glutathione (GSH) Nanosphere Liposome: Quintessential powerful antioxidant, liver/gall bladder detoxification, CFS, eye, brain, heavy metals, Liposome degenerative conditions Green Light High chlorophyll and additional green herbs for energy, fatigue, libido, digestive disturbances, ileo-cecal valve, hormonal Spagyric Tincture support, good source of iron and magnesium Green Tea Antioxidant, energy, neuro-protection, cardiovascular support, anti-viral/bacterial, degenerative conditions Catechins Gynostemma Adaptogenic Vasodilator, blood pressure, adrenal, liver, cholesterol, HDL, LDL, triglyceride regulation, bi-phasic effect on BioForce (GBF) brain, libido, anti aging (immortality herb/ Jiaogulan TCM), immune, high saponins (!), reduces blood sugar levels HepataGest Powder Digestive and liver support (Phase 1 & 2 & 3), supports all maintenance and detox, drainage programs HPA (Axis) Life Hypothalamus, Pituitary, Adrenal support, hormonal insufficiencies, CFS, energy, infertility, immune, prostate, PMS, Force menopause Hypo Zymase Dual phasic digestive support targeting the stomach and the small intestine (duodenum) for a wide variety of digestive disturbances. With correct proportions/ratios of HCl and other enzymes, botanicals etc Inflamma Life Force High potency anti-inflammatory, pain, cystic breast, sinusitis, plaquing, arthritis, joint pain, skin, etc Jambola Promotes normal blood sugar glucose levels, type II diabetes, metabolic/meta-obesity syndrome L-Arginine (SR) Sustained Release: Vasodilation, regulates nitric oxide, blood pressure, migraines/vascular headaches, libido, removes ammonia, strengthens vascular system, stimulates growth hormone/insulin, adrenal fatigue, low thyroid, energy, high BP Laminaria Brown algae concentrate/extract, (85%) fucoidans. Binds heavy metals, mercury detox radiation, low thyroid support, chelation, pathogens, weight loss, detox, apoptosis, natural iodine source, cardiac PHYSICA ENERGETICS’ QUICK REFERENCE & RESEARCH GUIDE Matrix Nutritionals Cont’d… LIFE Force Concentrated super food, digestive support, ICV, hormonal balance, high source of alkaline ash minerals Magnesium (buffered) Cardiac, BP, metabolic syndrome, Diabetes, PMS, neurological, depression, Autism, ADD/ADHD, migraines, muscular BisGlycinate skeletal support w/L-Taurine Melatonin Liposome Nanosphere Liposome Spray: Promotes sleep, regulates Circadian rhythms, jet lag, breast immune support MetaChlor Pure, premium-grade, naturally broken-cell wall Chlorella pyrenoidosa with CGF (Chlorella Growth Factors), heavy metals, chlorophyll, detoxification, GLA, anemia, digestive, RNA Methyl-B12 Nanosphere Liposome Spray: Mercury toxicity, Homocysteinemia, methylation pathways, B12 anemia, Autism, Liposome ADD/ADHD, depression, blood sugar MetPhos Gall bladder/stones, joint stiffness, cardiac, pyloric spasm, nausea, edema, calcium mobilization, mineralization, nerves NAC Forte Powerful antioxidant, liver detox, heavy metal detox, lungs, polycystic ovaries (PCOS), neurotransmitter building block, (N-acetyl cysteine) dental Nat Body CLR Systemic herbal cleansing, liver biliary tree, spleen, kidney, eliminatory organ detox and sustained support Nat Colon CLR Gentle colon cleanse and detoxification, parasites, Candida, diarrhea, constipation, non dependent forming Omega GOLD Anti-inflammatory, prostaglandin precursor, brain function, lowers cholesterol, calcium transport, prostate, breast, colon, pregnancy ADD/ADHD, skin conditions, mood enhancer, thyroid support, hypoglycemia Pancrea Life Force Nutrition for pancreas, blood sugar, metabolic syndrome, biliary stasis, allergies Phyto Antiox Antioxidant, OPCs, quercetin, green tea, turmeric, grape seed extract, acai berry, ICV, ignites enzymatic activity, alkaline- ash minerals, oxidative stress Phyto Cal-Mag Spagyric botanicals, muscle cramping, osteoporosis, osteo arthritis, estrogen support, fever, headaches, insomnia, w/Boron promotes bone growth, anxiety Pregnenolone Nanosphere Liposome: Brain, cognition, Alzheimer’s, anti-aging, hormonal insufficiencies, neuro-protective, depression Liposomal Drops Red Yeast Rice Promotes healthy cholesterol & triglyceride metabolism, normalizing elevated lipids, Diabetes, MetaObesity Syndrome, metabolic syndrome Saccharomyces C. difficile, diarrhea, antibiotic gastric upset, H. pylori, Dysbiosis, GI mucosal immune boulardii Forte Solray-D Liposome Nanosphere Liposome Spray: D3 with Vitamin K2 (MK7) bones, cardiac, immune, breast, prostate, colon, viral, calcitriol! SpectraLyte “Right-spinning” ionic trace minerals, electrolytes, Na/K pump, adjustments hold better, headaches, athletics, alkalizer, CFS, adrenal insufficiencies Thymus Life Force Immunomodulatory, maintain NK cell activity, induces Th-1 & T-cell support, antiviral, mold, Lyme, allergies, etc Thyro Life Force Low thyroid, thyroid, adrenal, hypothalamus, pituitary axis, fatigue, radiation protection, weight Vitamin B5 “Adrenal vitamin”, peristaltic action, neurotransmitter precursor, immune building, arthritis, lowers trigs/cholesterol Vitamin C Camu Nanosphere Liposome: Adrenal insufficiency, immune, protects liver from pathogens, energy, memory, etc Camu Liposome Wild Oregano Oil Respiratory infections, H. pylori, COX-2 inhibitor, pathogens Wild Bear Garlic Heavy metals, circulation, lowers BP, parasites, blood cleanser, natural anti-bacterial (“Allium Ursinum”) Xeno BioForce Phyto nutritional anti-xenobiotic, immune, long term and daily use, School children/adults (!), helps keep the mesenchyme clear, warming immune tea, airplane flu, city living, “buffers the onslaught to daily immune challenges” Flower Remedies (60 mL/2 oz. BioEnergetic Emotional Tinctures) Note: Pineal and Thymus sarcodes 6CH/ATP 5X Ultimate Fields Spagyric “Bach-like” flowers; all 38 in one specially prepared tincture, bioenergetically imprintable Ultimate Rescue Spagyric “Bach-like” Rescue Remedy Phenolics (60 mL/2 oz. Tincture) Note: Mesenchyme 6X, 9X, 6CH/ ATP 5X Ultimate Phenolics Phenolic Homaccord: all 37 phenolics - bioenergetically available for imprinting or stand alone Disclaimer: Limited to licensed Healing Arts Professionals for clinical research purposes only. This guide is not for public distribution. The commentary is not meant to diagnose, treat or replace conventional treatment, and has
Load more

Recommended publications
  • Effect of Liposome Composition and Other Factors on the Targeting of Liposomes to Experimental Tumors: Biodistribution and Imaging Studies1
    (CANCER RESEARCH SO.6371-6378. October I. 1990] Effect of Liposome Composition and Other Factors on the Targeting of Liposomes to Experimental Tumors: Biodistribution and Imaging Studies1 Alberto Gabizon,2 David C. Price, John Huberty, Robert S. Bresalier, and Demetrios Papahadjopoulos Cancer Research Institute ¡A.(j., I). P.] and Department of Radiology, [D. C. P., J. H.J, L'nirersity of California, San Francisco, California 9414}; (iastroinlestinal Research Laboratories, I eteram Administration Medical Center, and Department of Medicine, I 'nirersity of California, San Francisco, California 94121 [R. S. B.J; and Liposome Technology Inc., Mento Park, California 94025 ¡A.CiJ ABSTRACT temperature, cholesterol, and careful size control result in in hibition of RES uptake with concomitant enhancement of We have examined the distribution of radiolabeled liposomes in tumor- tumor uptake (5). bearing mice after i.v. injection. Two mouse tumors (B16 melanoma, In this report, we describe tissue distribution and imaging J6456 lymphoma) and a human tumor (LS174T colon carcinoma) inoc ulated i.m., S.C.,or in the hind footpad were used in these studies. When studies with transplantable mouse and human tumor models various liposome compositions with a mean vesicle diameter of ~ 100 nm using 3 different radiolabels of liposomes. The findings here were compared using a radiolabel of gallium-67-deferoxamine, optimal indicate that the concentration of liposome-encapsulated radio- tumor localization was obtained with liposomes containing a phosphati- labels in tumors is well above that of most other tissues and dylcholine of high phase-transition temperature and a small molar frac approximates the values obtained in the liver.
    [Show full text]
  • Liposome-Based Drug Delivery Systems in Cancer Immunotherapy
    pharmaceutics Review Liposome-Based Drug Delivery Systems in Cancer Immunotherapy Zili Gu 1 , Candido G. Da Silva 1 , Koen van der Maaden 2,3, Ferry Ossendorp 2 and Luis J. Cruz 1,* 1 Department of Radiology, Leiden University Medical Center, Albinusdreef 2, 2333 ZA Leiden, The Netherlands 2 Tumor Immunology Group, Department of Immunology, Leiden University Medical Center, Albinusdreef 2, 2333 ZA Leiden, The Netherlands 3 TECOdevelopment GmbH, 53359 Rheinbach, Germany Received: 1 October 2020; Accepted: 2 November 2020; Published: 4 November 2020 Abstract: Cancer immunotherapy has shown remarkable progress in recent years. Nanocarriers, such as liposomes, have favorable advantages with the potential to further improve cancer immunotherapy and even stronger immune responses by improving cell type-specific delivery and enhancing drug efficacy. Liposomes can offer solutions to common problems faced by several cancer immunotherapies, including the following: (1) Vaccination: Liposomes can improve the delivery of antigens and other stimulatory molecules to antigen-presenting cells or T cells; (2) Tumor normalization: Liposomes can deliver drugs selectively to the tumor microenvironment to overcome the immune-suppressive state; (3) Rewiring of tumor signaling: Liposomes can be used for the delivery of specific drugs to specific cell types to correct or modulate pathways to facilitate better anti-tumor immune responses; (4) Combinational therapy: Liposomes are ideal vehicles for the simultaneous delivery of drugs to be combined with other therapies, including chemotherapy, radiotherapy, and phototherapy. In this review, different liposomal systems specifically developed for immunomodulation in cancer are summarized and discussed. Keywords: liposome; drug delivery; cancer immunotherapy; immunomodulation 1. The Potential of Immunotherapy for the Treatment of Cancer Cancer immunotherapy has been widely explored because of its durable and robust effects [1].
    [Show full text]
  • Entrapment of Citrus Limon Var. Pompia Essential Oil Or Pure Citral in Liposomes Tailored As Mouthwash for the Treatment of Oral Cavity Diseases
    pharmaceuticals Article Entrapment of Citrus limon var. pompia Essential Oil or Pure Citral in Liposomes Tailored as Mouthwash for the Treatment of Oral Cavity Diseases 1, 1, 2 3 Lucia Palmas y , Matteo Aroffu y, Giacomo L. Petretto , Elvira Escribano-Ferrer , Octavio Díez-Sales 4, Iris Usach 4, José-Esteban Peris 2, Francesca Marongiu 1, Mansureh Ghavam 5, Sara Fais 6, Germano Orrù 6, Rita Abi Rached 7, Maria Letizia Manca 1,* and Maria Manconi 1 1 Department of Scienze della Vita e dell’Ambiente, Drug Science Division, University of Cagliari, 09124 Cagliari, Italy; [email protected] (L.P.); matteo.aroff[email protected] (M.A.); [email protected] (F.M.); [email protected] (M.M.) 2 Department of Chemistry and Pharmacy, University of Sassari, 07100 Sassari, Italy; [email protected] (G.L.P.); [email protected] (J.-E.P.) 3 Biopharmaceutics and Pharmacokinetics Unit, Institute for Nanoscience and Nanotechnology, University of Barcelona, 08193 Barcelona, Spain; [email protected] 4 Department of Pharmacy, Pharmaceutical Technology and Parasitology, University of Valencia, Burjassot, 46100 Valencia, Spain; [email protected] (O.D.-S.); [email protected] (I.U.) 5 Department of Range and Watershed Management, Faculty of Natural Resources and Earth Sciences, University of Kashan, Kashan 8731753153, Iran; [email protected] 6 Department of Surgical Science, University of Cagliari, Molecular Biology Service Lab (MBS), Via Ospedale 40, 09124 Cagliari, Italy; [email protected] (S.F.); [email protected] (G.O.) 7 Centre d’Analyses et de Recherche, Unité de Recherche TVA, Laboratoire CTA, Faculté des Sciences, Université Saint-Joseph, B.P.
    [Show full text]
  • In Vitro Release Test Methods for Drug Formulations for Parenteral Applications
    dx.doi.org/10.14227/DT250418P8 Reprinted with permission. Copyright 2018. The United States Pharmacopeial Convention. All rights reserved. In Vitro Release Test Methods for Drug Formulations for Parenteral Applications Vivian Gray,a Susan Cady,b David Curran,c James DeMuth,d Okponanabofa Eradiri,e Munir Hussain,f Johannes Krämer,g John Shabushnig,h Erika Stippler,i,j a V. A. Gray Consulting, Inc, Hockessin, DE. b Boehringer Ingelheim Animal Health, North Brunswick, NJ. c GlaxoSmithKline R&D, King of Prussia, PA. d University of Wisconsin, Madison, WI. e Food and Drug Administration, Silver Spring, MD.—The views presented in this article do not necessarily reflect those of the FDA. No official support or endorsement by the Food and Drug Administration is intended or should be inferred. f Bristol-Myers Squibb Company, New Brunswick, NJ. (Retired). g PHAST, Homburg, Germany. h Insight Pharma Consulting, LLC, Marshall, MI. i United States Pharmacopeia, Rockville, MD. j Correspondence should be addressed to: Desmond G Hunt, Principal Scientific Liaison, US Pharmacopeial Convention, 12601 Twinbrook Parkway, Rockville, MD 20852-1790; tel: +1.301.816.8341; email: [email protected] ABSTRACT In vitro drug release testing for parenteral drug formulations could benefit from more regulatory guidance and compendial information as this testing is a part of current expectations for drug product approval. This Stimuli article discusses in vitro drug release methods for those parenteral drug formulations that are not solutions and explores the challenges involved in using these methods for each formulation type. INTRODUCTION particulate matter, sterility, bacterial endotoxins, water his Stimuli article is the work of some members of the content, aluminum content, and content uniformity.
    [Show full text]
  • Preparation and Evaluation of Liposome Containing Clove Oil
    PREPARATION AND EVALUATION OF LIPOSOME CONTAINING CLOVE OIL By Pilaslak Akrachalanont A Thesis Submitted in Partial Fulfillment of the Requirements for the Degree MASTER OF PHARMACY Program of Pharmaceutical Technology Graduate School SILPAKORN UNIVERSITY 2008 PREPARATION AND EVALUATION OF LIPOSOME CONTAINING CLOVE OIL By Pilaslak Akrachalanont A Thesis Submitted in Partial Fulfillment of the Requirements for the Degree MASTER OF PHARMACY Program of Pharmaceutical Technology Graduate School SILPAKORN UNIVERSITY 2008 !"#$% &'(% !)%*+!,-.&"-#,//1(",$3 .!('1( $3! ,!" 4"-#2552 .)6.&$3! ,!" The graduate school, Silpakorn University has approved and accredited the thesis title of Preparation and Evaluation of Liposome Containing Clove Oil submitted by Miss Pilaslak Akarachalanon as a partial fulfillment of the requirements for the degree of master of pharmacy, program of pharmaceutical technology. (Associate Professor Sirichai Chinatangkul, Ph.D.) Dean of graduate school ./.../... The Thesis advisors 1. Associate Professor Somlak Kongmuang, Ph.D. 2. Assistant Professor Police Captain Malai Sathirapund 3. Associate Professor Uthai Sotanaphun, Ph.D. The Thesis Examination Committee Chairman (Parichat Chomto, Ph.D.) ../../.. .Member (Prof. Garnpimol Rittidej, Ph.D.) ../../.. .Member (Assoc.Prof. Somlak Kongmuang, Ph.D.) ../../.. .Member Member (Assist.Prof. Pol.Capt. Malai Sathirapund) (Assoc.Prof. Uthai Sotanaphun, Ph.D.) ../../.. ../../ 47353202 : MAJOR : PHARMACEUTICAL TECHNOLOGY KEY WORDS : LOPOSOME / CLOVE OIL / EUGENOL / THIN FILM METHOD PILASLAK AKRACHALANONT : PREPARATION AND EVALUATION OF LIPOSOME CONTAINING CLOVE OIL. THESIS ADVISORS : ASSOC.PROF.SOMLAK KONGMUANG, Ph.D., ASSIST.PROF POL.CAPT. MALAI SATHIRAPUND, AND ASSOC.PROF. UTHAI SOTANAPHUN, Ph.D. 117 pp. This research particularly focuses on preparation of liposomes which can efficiently maintain stability and quality of clove oil. The research method used in this study can be divided into five main steps.
    [Show full text]
  • Ph and Temperature Dual-Sensitive Liposome Gel Based on Novel Cleavable Mpeg-Hz-CHEMS Polymeric Vaginal Delivery System
    International Journal of Nanomedicine Dovepress open access to scientific and medical research Open Access Full Text Article Original RESEARCH pH and temperature dual-sensitive liposome gel based on novel cleavable mPEG-Hz-CHEMS polymeric vaginal delivery system Daquan Chen1,2 Background: In this study, a pH and temperature dual-sensitive liposome gel based on a Kaoxiang Sun1,2 novel cleavable hydrazone-based pH-sensitive methoxy polyethylene glycol 2000-hydrazone- Hongjie Mu1 cholesteryl hemisuccinate (mPEG-Hz-CHEMS) polymer was used for vaginal administration. Mingtan Tang3 Methods: The pH-sensitive, cleavable mPEG-Hz-CHEMS was designed as a modified pH- Rongcai Liang1,2 sensitive liposome that would selectively degrade under locally acidic vaginal conditions. The Aiping Wang1,2 novel pH-sensitive liposome was engineered to form a thermogel at body temperature and to degrade in an acidic environment. Shasha Zhou1 Results: A dual-sensitive liposome gel with a high encapsulation efficiency of arctigenin was Haijun Sun1 formed and improved the solubility of arctigenin characterized by Fourier transform infrared 1 Feng Zhao spectroscopy and differential scanning calorimetry. The dual-sensitive liposome gel with 1 Jianwen Yao a sol-gel transition at body temperature was degraded in a pH-dependent manner, and was 1,2 Wanhui Liu stable for a long period of time at neutral and basic pH, but cleavable under acidic conditions 1School of Pharmacy, Yantai (pH 5.0). Arctigenin encapsulated in a dual-sensitive liposome gel was more stable and less University, 2State Key Laboratory toxic than arctigenin loaded into pH-sensitive liposomes. In vitro drug release results indicated of Longacting and Targeting Drug Delivery Systems, Yantai, 3School of that dual-sensitive liposome gels showed constant release of arctigenin over 3 days, but showed Pharmaceutical Sciences, Shandong sustained release of arctigenin in buffers at pH 7.4 and pH 9.0.
    [Show full text]
  • Ambisome® (Amphotericin B) Liposome for Injection
    AmBisome® (amphotericin B) liposome for injection DESCRIPTION AmBisome® for Injection is a sterile, non-pyrogenic lyophilized product for intravenous infusion. Each vial contains 50 mg of amphotericin B, USP, intercalated into a liposomal membrane consisting of approximately 0.64 mg alpha tocopherol, USP; 52 mg cholesterol, NF; 84 mg distearoyl phosphatidylglycerol, sodium salt; 213 mg hydrogenated soy phosphatidylcholine. In addition, 27 mg disodium succinate hexahydrate and 900 mg sucrose, NF are used as a buffer. AmBisome may contain hydrochloric acid and/or sodium hydroxide as pH adjusters. Following reconstitution with Sterile Water for Injection, USP, the resulting pH of the suspension is between 5-6. AmBisome is a true single bilayer liposomal drug delivery system. Liposomes are closed, spherical vesicles created by mixing specific proportions of amphophilic substances such as phospholipids and cholesterol so that they arrange themselves into multiple concentric bilayer membranes when hydrated in aqueous solutions. Single bilayer liposomes are then formed by microemulsification of multilamellar vesicles using a homogenizer. AmBisome consists of these unilamellar bilayer liposomes with amphotericin B intercalated within the membrane. Due to the nature and quantity of amphophilic substances used, and the lipophilic moiety in the amphotericin B molecule, the drug is an integral part of the overall structure of the AmBisome liposomes. AmBisome contains true liposomes that are less than 100 nm in diameter. A schematic depiction of the liposome is presented below. Note: Liposomal encapsulation or incorporation into a lipid complex can substantially affect a drug’s functional properties relative to those of the unencapsulated drug or non-lipid associated drug. In addition, different liposomal or lipid-complex products with a common active ingredient may vary from one another in the chemical composition and physical form of the lipid component.
    [Show full text]
  • United States Patent (19) 11) Patent Number: 4,767,615 Geho Et Al
    United States Patent (19) 11) Patent Number: 4,767,615 Geho et al. 45 Date of Patent: "Aug. 30, 1988 54; DENTAL THERAPY BY VESICLEDELIVERY 4,603,044 7/1986 Geho ....................................... 514/3 (75) Inventors: W. Blair Geho; Joseph Jacob; John R. OTHER PUBLICATIONS Lau, all of Wooster, Ohio Accepted Dental Therapeutics, 38th Ed., American Den 73) Assignee: Technology Unlimited, Inc., Wooster, tal Association, Chicago, Ill. 1979, p. 343. Ohio Jones et al. in Chemical Week, McGraw-Hill Inc., Jul. *) Notice: The portion of the term of this patent 30, 1986, pp. 426-5129, "Liposome Research: New Path subsequent to Jul. 29, 2003 has been for Drug Delivery'. disclaimed. Primary Examiner-Ronald W. Griffin (21) Appl. No.: 877,862 Assistant Examiner-F. T. Moezie (22 Filed: Jun. 24, 1986 Attorney, Agent, or Firm-Frijouf, Rust & Pyle 57 ABSTRACT Related U.S. Application Data A known procedure is used to prepare liposomes of 63 Continuation-in-part of Ser. No. 606,714, May 3, 1984, bipolar lipid membrane which are permeable and hence Pat. No. 4,603,044. "leak' their contents at a rate which is variable by 51) Int. Cl................................................. A61K 7/16 choice. The liposome is supplied with medication or 52 U.S. Cl. ........................................ 424/57; 424/49; cosmetic material for the oral cavity, or specifically for 424/54 the teeth and gums. The liposome is then attached to a 58) Field of Search ....................... 424/19, 21, 22, 27, molecule that has affinity for the hydroxyapatite. Thus, 424/28, 38, 49, 54, 57 the liposome will bind to oral cavity hydroxyapatite and (56) References Cited bathe the surrounding support surface with its contents for extended hours of service.
    [Show full text]
  • Development of Cationic Liposome Formulations for Intratracheal Gene Therapy of Early Lung Cancer
    © 2000 Nature America, Inc. 0929-1903/00/$15.00/ϩ0 www.nature.com/cgt Development of cationic liposome formulations for intratracheal gene therapy of early lung cancer Yiyu Zou,1 Gang Zong,1 Yi-He Ling,2 and Roman Perez-Soler2 1Department of Cancer Biology, University of Texas MD Anderson Cancer Center, Houston, Texas 77030; and 2New York University, Rita J. & Stanley Kaplan Comprehensive Cancer Center, New York, New York 10016. Regional (intratracheal or aerosol) delivery of cationic liposome-DNA complexes for gene therapy of lung disease offers distinct advantages over systemic (intravenous) administration. However, optimal formulations for early lung cancer treatment have not been established. Therefore, we investigated Ͼ50 different liposome and micelle formulations for factors that may affect their transcription efficiency and tested the ideal formulations in an in vivo mouse model. Our data showed that cationic liposomes were generally more effective at transfecting genes than were micelles of the same lipid composition, thus suggesting a role for the bilayer structure in facilitating transfection. In addition, the transfection efficiency of liposome-delivered genes was highly dependent upon the lipid composition, lipid/DNA ratio, particle size of the liposome-DNA complex, and cell lines used. By optimizing these factors in vitro and in vivo, we developed a novel liposome formulation (DP3) suitable for intratracheal administration. Using G67 liposome as control, we found that DP3 was more effective than G67 in vitro and as effective as G67 at both preventing lung tumor growth and prolonging survival in our lung cancer mouse model. We observed a positive correlation between the in vitro p53 function and the in vivo antitumoral activities of liposome-p53 formulations, which had not been reported previously in studies of an intravenous liposome gene delivery system.
    [Show full text]
  • WO 2015/120389 Al 13 August 2015 (13.08.2015) P O P C T
    (12) INTERNATIONAL APPLICATION PUBLISHED UNDER THE PATENT COOPERATION TREATY (PCT) (19) World Intellectual Property Organization International Bureau (10) International Publication Number (43) International Publication Date WO 2015/120389 Al 13 August 2015 (13.08.2015) P O P C T (51) International Patent Classification: AO, AT, AU, AZ, BA, BB, BG, BH, BN, BR, BW, BY, A61K 31/35 (2006.01) A61M 16/10 (2006.01) BZ, CA, CH, CL, CN, CO, CR, CU, CZ, DE, DK, DM, A61P 37/08 (2006.01) DO, DZ, EC, EE, EG, ES, FI, GB, GD, GE, GH, GM, GT, HN, HR, HU, ID, IL, IN, IR, IS, JP, KE, KG, KN, KP, KR, (21) International Application Number: KZ, LA, LC, LK, LR, LS, LU, LY, MA, MD, ME, MG, PCT/US20 15/0 15029 MK, MN, MW, MX, MY, MZ, NA, NG, NI, NO, NZ, OM, (22) International Filing Date: PA, PE, PG, PH, PL, PT, QA, RO, RS, RU, RW, SA, SC, ' February 2015 (09.02.2015) SD, SE, SG, SK, SL, SM, ST, SV, SY, TH, TJ, TM, TN, TR, TT, TZ, UA, UG, US, UZ, VC, VN, ZA, ZM, ZW. (25) Filing Language: English (84) Designated States (unless otherwise indicated, for every (26) Publication Language: English kind of regional protection available): ARIPO (BW, GH, (30) Priority Data: GM, KE, LR, LS, MW, MZ, NA, RW, SD, SL, ST, SZ, 61/937,928 10 February 2014 (10.02.2014) US TZ, UG, ZM, ZW), Eurasian (AM, AZ, BY, KG, KZ, RU, 61/971,709 28 March 2014 (28.03.2014) US TJ, TM), European (AL, AT, BE, BG, CH, CY, CZ, DE, 61/978,71 1 11 April 2014 ( 11.04.2014) us DK, EE, ES, FI, FR, GB, GR, HR, HU, IE, IS, IT, LT, LU, LV, MC, MK, MT, NL, NO, PL, PT, RO, RS, SE, SI, SK, 62/105,423 20 January 20 15 (20.01.2015) us SM, TR), OAPI (BF, BJ, CF, CG, CI, CM, GA, GN, GQ, (71) Applicant: PATARA PHARMA, LLC [US/US]; 11455 GW, KM, ML, MR, NE, SN, TD, TG).
    [Show full text]
  • Liposomal Formulations in Clinical Use: an Updated Review
    pharmaceutics Review Liposomal Formulations in Clinical Use: An Updated Review Upendra Bulbake †, Sindhu Doppalapudi †, Nagavendra Kommineni and Wahid Khan * Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research, Hyderabad 500037, India; [email protected] (U.B.); [email protected] (S.D.); [email protected] (N.K.) * Correspondence: [email protected] † These authors contributed equally to this work. Academic Editor: Murali Mohan Yallapu Received: 16 January 2017; Accepted: 23 March 2017; Published: 27 March 2017 Abstract: Liposomes are the first nano drug delivery systems that have been successfully translated into real-time clinical applications. These closed bilayer phospholipid vesicles have witnessed many technical advances in recent years since their first development in 1965. Delivery of therapeutics by liposomes alters their biodistribution profile, which further enhances the therapeutic index of various drugs. Extensive research is being carried out using these nano drug delivery systems in diverse areas including the delivery of anti-cancer, anti-fungal, anti-inflammatory drugs and therapeutic genes. The significant contribution of liposomes as drug delivery systems in the healthcare sector is known by many clinical products, e.g., Doxil®, Ambisome®, DepoDur™, etc. This review provides a detailed update on liposomal technologies e.g., DepoFoam™ Technology, Stealth technology, etc., the formulation aspects of clinically used products and ongoing clinical trials on liposomes. Keywords: liposomes; therapeutics; drug delivery; liposome technology; nanotechnology; clinical trials; marketed products 1. Introduction The concept of liposomal drug delivery system has revolutionised the pharmaceutical field. Alec Bangham, in 1961 [1], first described liposomes. Since then active research in the field of liposomes have been carried out and their applications are now well established in various areas, such as drug, biomolecules and gene delivery [2].
    [Show full text]
  • 54292-Daunoxome-Package-Insert-US-Original.Pdf
    DaunoXome® (daunorubicin citrate liposome injection) Rx only WARNINGS 1. Cardiac function should be monitored regularly in patients receiving DaunoXome (daunorubicin citrate liposome injection) because of the potential risk for cardiac toxicity and congestive heart failure. Cardiac monitoring is advised especially in those patients who have received prior anthracyclines or who have pre-existing cardiac disease or who have had prior radiotherapy encompassing the heart. 2. Severe myelosuppression may occur. 3. DaunoXome should be administered only under the supervision of a physician who is experienced in the use of cancer chemotherapeutic agents. 4. Dosage should be reduced in patients with impaired hepatic function. (See DOSAGE AND ADMINISTRATION) 5. A triad of back pain, flushing, and chest tightness has been reported in 13.8% of the patients (16/116) treated with DaunoXome in the Phase III clinical trial, and in 2.7% of treatment cycles (27/994). This triad generally occurs during the first five minutes of the infusion, subsides with interruption of the infusion, and generally does not recur if the infusion is then resumed at a slower rate. DESCRIPTION DaunoXome (daunorubicin citrate liposome injection) is a sterile, pyrogen-free, preservative-free product in a single use vial for intravenous infusion. DaunoXome contains an aqueous solution of the citrate salt of daunorubicin encapsulated within lipid vesicles (liposomes) composed of a lipid bilayer of distearoylphosphatidylcholine and cholesterol (2:1 molar ratio), with a mean diameter of about 45 nm. The lipid to drug weight ratio is 18.7:1 (total lipid:daunorubicin base), equivalent to a 10:5:1 molar ratio of distearoylphosphatidylcholine:cholesterol:daunorubicin.
    [Show full text]