WO1984000686A1 - Perfluorocarbon emulsions and their preparation and use in therapy - Google Patents

Perfluorocarbon emulsions and their preparation and use in therapy Download PDF

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Publication number
WO1984000686A1
WO1984000686A1 PCT/US1983/001237 US8301237W WO8400686A1 WO 1984000686 A1 WO1984000686 A1 WO 1984000686A1 US 8301237 W US8301237 W US 8301237W WO 8400686 A1 WO8400686 A1 WO 8400686A1
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pharmaceutical composition
oxygen
composition according
dispersion
aqueous pharmaceutical
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French (fr)
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John M Yuhas
Robert L Goodman
Robert E Moore
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Sunoco Inc R&M
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Sunoco Inc R&M
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Priority to NL8320264A priority Critical patent/NL8320264A/nl
Priority to FI841513A priority patent/FI841513A0/fi
Publication of WO1984000686A1 publication Critical patent/WO1984000686A1/en
Priority to SE8402098A priority patent/SE8402098L/xx
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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/10Dispersions; Emulsions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/10Dispersions; Emulsions
    • A61K9/107Emulsions ; Emulsion preconcentrates; Micelles
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0019Injectable compositions; Intramuscular, intravenous, arterial, subcutaneous administration; Compositions to be administered through the skin in an invasive manner
    • A61K9/0026Blood substitute; Oxygen transporting formulations; Plasma extender
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/02Halogenated hydrocarbons
    • A61K31/025Halogenated hydrocarbons carbocyclic
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/70Carbohydrates; Sugars; Derivatives thereof
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/70Carbohydrates; Sugars; Derivatives thereof
    • A61K31/7088Compounds having three or more nucleosides or nucleotides
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M2202/00Special media to be introduced, removed or treated
    • A61M2202/04Liquids
    • A61M2202/0468Liquids non-physiological
    • A61M2202/0476Oxygenated solutions

Definitions

  • This invention relates to the sensitization of hypoxic tumor cells to therapy, and in particular to methods, compositions and systems for sensitizing hypoxic tumor cells to radiation and/or to certain chemotherapeutic agents, whether the therapy is employed alone or in combination with agents which protect normal tissues from injury.
  • the invention further relates to diagnostic methods in support of the sensitization and therapy.
  • RS radiosensitization or radiosensitizing "RT” - radiotherapy or radiotherapeutic "CT” - chemotherapy or chemotherapeutic "RP” - radioprotection or radioprotective "CTP” - chemotherapeutic protective
  • Oxygen deficient (hypoxic) cells can be up to about three times more resistant to radiation than are well-oxygenated cells. These cells are relatively common in tumors but are rare in normal tissues, thereby giving the tumor cells a greater resistance to radiation than one observes in normal tissues. As a consequence, one often cannot deliver enough radiation to eradicate the tumor cells without incurring an una ⁇ ceptably high risk of severe injury to normal tissue. These same hypoxic cells are often resistant to those forms of chemotherapy which are oxygen dependent. In such chemotherapy, however, oxygen must often be supplied to the hypoxic cells for another reason in addition to maximal cell destruction: hypoxic cells are not actively growing (multiplying) and many of the more effective chemotherapeutic drugs cannot kill the cells unless they are growing.
  • hypoxic cells have low energy reserves and are thus believed less able to actively transport certain chemotherapeutic drugs across their membranes.
  • the Belgrad et al study is not useful as a guide or suggestion of the use of perfluorooctyl bromide or other PFC in hypoxic tumor cell therapy.
  • the study has little clinical relevance, and discourages further studies leading to clinical investigations.
  • hypoxia is invariably found in carcinoma and sarcoma but even in benign conditions (where the hypoxic cell tumors are not continually increasing in mass), radiotherapy and/or chemotherapy are sometimes prescribed in order to forestall cancerous conditions.
  • the present invention is therefore applicable both to malignant and benign hypoxic tumor cells.
  • the oxygen transfer compound if used systemically, will diffuse quickly through the vasculature, pick up oxygen in the lungs, remain in the cardiovascular system for about 10 to 12 days, (to permit periodic irradiation at controlled dosages) and then be rapidly eliminated, while producing no intolerable toxicity. Under such conditions sensitization to radiotherapy and/or chemotherapy can be maximized. However, residence times as short as 2 to 8 hours may be sufficient if only short term therapy is necessary.
  • hypoxic tumor cells as a prelude to highly beneficial radiotherapy and/or oxygen-dependent chemotherapy, is achieved by contacting the cells or vasculature thereof with an oxygen carrying perfluoro compound, wherein the perfluoro coirtpound is uniformly dispersed in small particle size in an aqueous medium.
  • the resulting aqueous dispersion is rendered isotonic Cor otherwise physiologically acceptabl to mammalian cells prior to use as a sensitizing agent by the addition of salts, buffering agents or other reagents known to be effective for this purpose.
  • the dispersion is injected intravenously, is carried through the lungs where it picks up oxygen, and then penetrates the region of the hypoxic tumor cells.
  • the oxygen transferred from the perfluoro compound to the hypoxic cells sensitizes the cells.
  • the cells are irradiated and/or a CT agent is administered.
  • Cell destruction or reduced rate of growth can be monitored by biopsy, radioimaging or other technique..
  • Rowth as used herein means cell multiplication ; "control of growth” or similar term means cell destruction or decreased growth rate.
  • hypoxic tumor cells are oxygenated hyperbarically but at oxygen pressures and/or for periods substantially less severe than conventionally employed for treatment of hypoxia, and contact of the cells or vasculature thereof with the perfluoro compound thus supplements oxygen transfer to the cells.
  • This enhanced sensitization is then followed or accompanied by irradiation or chemotherapy in the conventional manner.
  • penetration of the perfluoro compound into the regions of the hypoxic tumor cells is monitored by systemic administration of a perfluoro compound which also has radiopaque properties, thereby permitting radioimaging.
  • a perfluoro compound which also has radiopaque properties thereby permitting radioimaging.
  • a variation of this approach is to incorporate into a dispersion containing an oxygen carrying perfluoro compound which does not have radioimaging properties, another compound which is an RI agent, thereby rendering the hypoxic cells susceptible to radioimaging.
  • RP and/or CTP agents are combined with the oxygen carrying PFC in the dispersion, or are separately delivered to the site of the hypoxia, in order to afford additional therapeutic response.
  • This effect is achieved through the ability of the perfluoro compound to sensitize the tumor cells, while the RP and CTP agents, since they are not absorbed by the tumor cells, shield the normal tissues from attack by radiation and the CT agents, respectively.
  • the same agent can be both radioprotective and chemotherapeutic protective.
  • the sensitizing agent of the invention is an aqueous dispersion of an oxygen carrying perfluoro compound and a dispersant (surfactant or emulsifier) which is effective for uniformly dispersing the perfluoro compound in the aqueous medium.
  • the dispersant is required because the perfluoro compounds are relatively hydrophobic and would otherwise tend to agglomerate in the mammalian body fluids through which the compound must pass and which serve to carry the compound to the hypoxic tumor cells or vasculature thereof.
  • the aqueous dispersion medium also permits addition of reagents for rendering the dispersion isotonic or otherwise physiologically acceptable to the cells.
  • the perfluoro compounds and dispersions thereof useful in this invention are those materials identified in the patent and other technical literature as synthet blood substitutes.
  • Representative of the patent literature disclosing such blood substitutes are U.S. Patents 3,641,167, 3,823,091, 3,911,138, 3,962,439, 3,993,581, 4,041,086, 4,105,798, and 4,325,972, the disclosures of which are incorported herein by reference. It will be apparent from a review of the foregoing patents and other literature that a wide variety of per fluorinated compounds when suitably dispersed in an aqueous medium can be used for the purposes of the present invention.
  • the perfluoro compounds thus include aliphatic (acyclic or cyclicl and aromatic compounds, whether perfluorinated hydrocarbons only or also containing heteroatoms such as oxygen, sulfur and/or nitrogen, and may be used singly or as mixtures of two or more.
  • perfluoro compound for use in specific cases in accordance with the invention will depend on a variety of factors, including whether the treatment is in conjunction with radiotherapy, chemotherapy, or both; the character and locus of the hypoxia; the potency of the perfluoro compound as a sensitizer; toxicity of the perfluoro compound to normal cells and to the host mammal; capability of forming sufficiently small particle size dispersions and sufficiently stable dispersions to diffuse rapidly to the region of the hypoxic cells; residence time in the mammal, including accummulation tendencies; and similar considerations familiar to those knowledgeable in the sensitization art.
  • Guidance for such selection can be obtained from the blood substitute art, particularly as to oxygen transport capability, dispersion particle size and stability, mammalian residence time, and cytotoxicity. Additionally, on the basis of the in vitro and in vivo studies reported and discussed hereinafter, guidance is provided for selection of perfluoro compound and treatment parameters in specific cases of sensitization.
  • Pororo compound or “perfluorocarbon” as used herein refers to a substantially fluorinated or completely fluorinated material which is generally but not necessarily a liquid at ambient temperature and pressure.
  • substantially fluorinated as used herein means that most of the hydrogen atoms of a compound have been replaced by fluorine atoms, such that further replacement does not substantially increase the oxygen transport capability of the material. It is believed that this level is reached when at least about 80-90% of the hydrogen atoms have been replaced by fluorine atoms. However, it is preferred that at least 95% of the hydrogen atoms have been replaced, more preferably at least 98% and most preferably, 100%. In the afore mentioned U.S.
  • Patents 3,911,138 and 4,105,798, the ability to transport oxygen is related to the solubility in the materials of a gas such as oxygen. These patents suggest that the perfluorinated materials will absorb 10-100 cc of oxygen per 100 cc of material at 25°C. and 760 milliliters of mercury.
  • perfluoro compounds preferred for use in this invention are the perfluorinated derivatives of chemically inert C 9 -C 18 polycyclic compounds such as bicyclononanes (e.g., bicyclo [3.3.1] nonane, 2,6-dimethylbicyclo [3.3.11 nonane, 3-methylbicyclo [3.3.1] nonane and trimethylbicyclo [3.3.1] nonane); adamantane and alkyl (C 1 -C 6 ) adamantanes such as methyl and dimethyl adamantane, ethyl and diethyladamantane, trimethyladamantane, ethylmethyladamantane, ethyldimethyladamantane and tri ethyladamantane; methyldiadamantane and trimethyldiadamantane; methyl and dimethylbicyclooctanes; tetrahydrobinor-S, pinane,
  • Hetero atom perfluoro compounds include F-tributyl amine, F-tripropyl amine and
  • Aromatic and aliphatic compounds include F-naphthalene, F-1-methyl-naphthalene, F-n-methyl morpholine, F-n-heptane and 1,2-bis-nonylfluorobutylethylene
  • fluorine atoms of the foregoing materials may be substituted by other halogen atoms such as bromine, included among these compounds, are, for example, monobrominated compounds such as 1-bromopentadecafluoro-4-isopropylcyclohexane, 1-bromotridecafluoro-hexane,
  • the compounds When bromo or iodo atoms appear in the perfluoro compounds, the compounds tend to be radiopaque while also retaining a large measure of their oxygen transporting capabilities.
  • the radiopacity renders these compounds useful as radioimaging (RI) agents, and therefore these compounds in some cases can be used not only as sensitizing agents but also as RI agents, alone or in combination with other sensitizers and/or RI agents, It is known that the rate of transpiration of perfluorinated hydrocarbons from lower mammals is in the order: tricyclics > bicyclics > alkyl monocyclics > paraffinics.
  • a tricyclic perfluoro compound will be preferred over other perfluoro compounds.
  • a bicyclic or monocyclic perfluoro compound might be chosen.
  • perfluoro compounds for use in the invention on the basis of relative inertness (chemical and biological), good dispersability and residence time are the perfluoro C 9 -C 18 polycyclic hydrocarbons of U.S. Patent 4,105,798, and particularly F-dimethyladamantane, F- trimethylbicyclononane, F-tricyclo [5.2.1.0 2,6 ] decane,
  • the preferred dispersants for uniformly dispersing the perfluoro compounds in an aqueous medium are the non-ionic surfactants.
  • ionic or amphoteric surfactants may be used to disperse the perfluoro compounds. Because systemic treatments require careful attention to physiological acceptability of the compounds, such as isotonic character, ionic surfactants are less desirable, although it is possible to offset or moderate their ionic character by formulating the dispersions with electrolytes or other additives.
  • Suitable nonionic surfactants include aliphatic materials such as block copolymers of ethylene oxide and propylene oxide comprising a hydrophobic propylene oxide section combined with one or more hydrophilic ethylene oxide sections, for example the "Pluronic” (trademark) surfactants available from BASF-Wyandotte, Inc.
  • aromatic types may also be used, such as alkylphenoxypolyethoxyethanols having alkyl groups of about 7 to 18 carbon atoms and 1 to 60 or more oxyethylene units, for example: heptylphenoxypolyethoxyethanols, octylphenoxy polyethoxyethanols, methyloctylphenoxypolyethoxyethanols, nonylphenoxypolyethoxyethanols, dodecylphenoxypolyethoxy ethanols, and the like; polyethoxyethanol derivatives of methylene linked alkylphenols; sulfur-containing analogs of the foregoing; ethylene oxide derivatives of long-chain carboxylic acids, such as lauri ⁇ , myristic, palmitic, oleic, and the like or mixtures of acids such as are found in tall oil containing 1 to 60 oxyethylene units per molecule; and analogous ethylene oxide condensates of long-chain or branched-chain amines, such as dodec
  • Naturally occurring emulsifiers or derivatives thereof are also useful. These include the alginates, cellulose derivatives such as methyl cellulose and carboxymethyl cellulose, water soluble gums such as gum arabic and gum tragacanth, the phospholipids (.such as lecithin and yolk phospholipid), and the sterols.
  • Nonionic fluorine containing surfactants are particularly preferred.
  • the fluorinated alkyl esters are one class of these surfactants, and are commercially available from 3M Company under the designations FC-93, FC-95, FC-128, FC-143, FC-430 and FC-431.
  • the more preferred nonionic, fluorine containing surfactants from the standpoint of their exceptional ability to form dispersions which maintain a range of small particle size over substantial periods of time, of the order of 35 weeks to a year or more, even at room temperature, are the fluorinated amidoamine oxides described in U.S. Patents 3,828,085 to Price et al, and 3,547,995 to Bartlett, the disclosures of which are incorporated herein by reference. These compounds may be generally described by the Formula (1):
  • R f is a perfluoroalkyl radical of 4 to about 25 carbon atoms or a polyfluoroalkoxyalkyl radical wherein the alkoxy group may contain 3 to about 40 carbon atoms of which at least a major portion thereof are perfluorinated and the alkyl group may contain 2 to about 40 carbon atoms, fluorinated or unfluorinated;
  • Y is hydrogen or alkyl of 1 to 6 carbon atoms;
  • R is an alkylene radical of the formula:
  • R 5 and R 6 are each alkyl radicals of 1 to 6 carbon atoms or hydroxy-terminated alkyl radicals of 2 to 6 carbon atoms. In all cases the alkoxy, alkyl and alkylene groups may be straight or branched chain.
  • Preferred subclasses of the surfactants of the foregoing patents are those of the following Formulas (2) and (3) : wherein n is at least 3 (preferably 3-10), x is at least
  • y is at least 1 (preferably 2-6)
  • R 1 and R 2 independently are alkyl radicals containing 1-6 carbon atoms. wherein n is at least (preferably 3-10) , z is at least 1
  • R 1 and R 2 independently are alkyl radicals containing 1-6 carbon atoms.
  • aqueous dispersions of the invention are prepared by any mixing technique which will provide a uniform blend of the ingredients, and preparation accord ingly may be readily accomplished by the skilled formulator.
  • a suitable pH range is 7.2-7.4.
  • the additives commonly used to render fluids physiologically acceptable are buffers such as sodium bicarbonate, and mixtures such as Ringer's Solution.
  • sorbitol Other materials conventionally employed in pharmaceutical preparations and known to the skilled formulator may also be added to the dispersions. These include viscosity modifiers, stabilizers (against degradation due to freezing or contamination, for example) , anti-freeze agents, diluents, encoding agents, and the like. Among such additives may be mentioned glycerin, dimethyl sulfoxide (“DMSO”) , various gelatins both natural and synthetic, and polyols such as sorbitol.
  • DMSO dimethyl sulfoxide
  • various gelatins both natural and synthetic
  • polyols such as sorbitol.
  • the perfluoro compound and surfactant components may be blended into water in any proportions which will provide uniform dispersions. Typical proportions are about 5 to 50% perfluoro compound based on the volume of the total composition and about 0.5 to 10% of the surfactant based on the total weight of the composition. Preferred proportions are about 10-30% by volume of the perfluoro compound and about 2-5% by weight of the surfactant, but proportions in particular cases may be varied depending on disperability of the PFC, particle size desired, and similar consideration
  • the aqueous dispersions more usually comprise emulsions, preferably of the oil-in-water type but also including water-in-oil emulsions. In some cases the emulsions have a very fine particle size and appear transparent or solution-like to the unaided eye.
  • the micro-emulsions which can be formulated with the dispersants of U.S. Patent 3,828,085 have this characteristic and are preferred. Colloidal suspensions, while not excluded from use in this invention, are less preferred, particularly for systemic administration, because of their larger particle size range and less stability.
  • the above-identified blood substitute and surfactant patents provide excellent guidance to formulation of the dispersions, and attention is directed to the patents for such purpose.
  • aqueous dispersions containing the oxygen transporting perfluoro compound when used as sensitizers in accordance with the invention, may be administered to a mammal locally or in any systemic fashion, whether intravenous, subcutaneous, intramuscular, parenteral, intraperitoneal or oral.
  • administration will be systemic and at a site enabling the dispersion to traverse the lungs to pick up oxygen and to transport the oxygen to the hypoxic tumor cells.
  • Dosages of the dispersion will be predetermined in accordance with the site and character of the hypoxia, whether or not the treatment is a supplement to hyperbaric oxygen treatment, the systemic tolerance (toxicity) of the mammal to the specific formulation, and other factors known to the therapist.
  • fluorocrits (cc of PFC per 100 ml blood) of the perfluoro compound should be in the range of about 3-10%, although lower or higher fluorocrits in special circumstances may be sufficient or required.
  • the fluorocrit need not be over 3.5%, and the partial pressure of oxygen in the inspired air may be up to about 2 atmospheres at 100% oxygen.
  • hyperbaric oxygen administration would be 30 minutes at 2 atmospheres 100% oxygen pressure, and these conditions are known to be well within tolerated levels.
  • the duration, con tent and pressure of the primary oxygenation in specific cases again will depend upon various factors, such as the health of the mammal or patient, the site of the hypoxia, and other conditions familiar to the ratio- or chemo therapist.
  • Contact of the PFC dispersion may be with the hypoxic cells or with the tumor cell vasculature, such that the oxygen carried by the PFC may transfer to the tumor/ vasculature interface.
  • the ideal may be direct contact between the PFC dispersion and the hypoxic cells, this may not be achievable and in fact is not required, since excess oxygen, wherever present in the tumor mass, will tend to become distributed throughout the mass, and thus reach the hypoxic cells.
  • the dosage of the sensitizing agent prior to irradiation and/or chemotherapy will also be controlled by various conditions, including the rate at which the perfluoro compound travels to the hypoxic tumor cells, the degree of sensitization desired, and the cardiovascular half-life residence time of the dispersion in the cardiovascular system and in the hypoxic tissues. For some treatments, including the rate at which the perfluoro compound travels to the hypoxic tumor cells, the degree of sensitization desired, and the cardiovascular half-life residence time of the dispersion in the cardiovascular system and in the hypoxic tissues. For some treatments, including the rate at which the perfluoro compound travels to the hypoxic tumor cells, the degree of sensitization desired, and the cardiovascular half-life residence time of the dispersion in the cardiovascular system and in the hypoxic tissues. For some treatments, including the rate at which the perfluoro compound travels to the hypoxic tumor cells, the degree of sensitization desired, and the cardiovascular half-life residence time of the dispersion in the cardiovascular system and in the hypoxic tissues
  • an acceptable cardiovascular (serum) half-life can be as brief as about 2 to 4 hours. This duration indicates that the perfluoro compound moves rapidly to the hypoxic tumor cells and transfers its oxygen to the cells.
  • an outstanding property of the preferred dispersions of the invention is an extremely small particle size, which particle size is maintained over substantial periods. The small particle size enables the dispersions to quickly traverse the vasculature to the site of the hypoxia. For example, an average particle size of 0.05 to 0.2 micron has been observed and has been maintained for several months and up to a year or more.
  • the dispersions may be oxygenated prior to infusion into the mammalian body and this may be expedient when injection is at or near the site of the hypoxia rather than at a site where oxygen transfer from the lungs and arteries is anticipated.
  • Prior oxygenation in such manner may be accomplished by any means, such as flushing or blanketing a vessel containing the dispersion with oxygen or air, or bubbling oxygen or air through the dispersion prior to administration.
  • preoxygenation in the manner described may also be practiced. In every case of preoxygenation, however, there may be a loss of oxygen prior to entry of the dispersion into the region of the hypoxic tumor cells, that is, during transit of the dispersion to the cells; hence, preoxygenation generally is not preferred.
  • irradiation can be accomplished by external application or by internal placement of radiation sources near or at the site of the hypoxia. Accordingly, the irradiation may be achieved with x-rays, gamma rays, neutrons and the like, or with implanted radium, iridium or cesium sources. Conventional radiation therapy (200 rads per day, five days per week for six to eight weeks) may be employed but dosage and total duration of treatment may be adjusted as required in particular circumstances.
  • the sensitizing method of the invention will be effective for all types of hypoxic tumor cells, whether such cells be in suspension (as in leukemia) or in solid form, but the invention is particularly effective for solid tumors Because systemic distribution of the dispersions is rapid, primarily due to the extremely small and stable particle size of the preferred dispersions of the invention, hypoxia at practically any site may be sensitized in accordance with the invention.
  • Chemotherapy is often used in combination with radiotherapy to destroy or control hypoxic tumor cells and therefore the sensitization techniques of the invention can be applied simultaneously or sequentially to chemotherapy and radiotherapy.
  • a sensitizer dispersion will normally be selected which has the cardiovascular residence time effective to cover the duration of both treatments, or if the residence time is short, the sensitizer dosage can be suitably increased or adjusted.
  • some chemotherapeutic agents are oxygen dependent in terms of requiring oxygen for active transport of the CT drug into the cell, for cell cycling control or CT enhancement. Hence, oxygen must be supplied in free form or by means of a carrier.
  • the perfluoro compounds of the present invention and their dispersions are capable of transferring large quantities of oxygen, it can be expected that chemotherapy based upon drugs which are oxygen dependent will be benefited by formulating the drugs with an RS agent of the present invention, or sequentially administering the RS and CT agents.
  • Methotrexate is an example of a CT drug thought to require oxygen for active transport into the cell.
  • Vinblastine and Vincristine are drugs which require oxygen for cell cycling.
  • CT drugs which may not be oxygen dependent may also be administered in conjunction with the sensitizing techniques of the invention.
  • Androgens Estrogens, Anti-estrogen, Progestins, Adrenal Steroids, Nitrogen Mustard, Chlorambucil, Phenylalanine Mustard, Cyclophosphamide, Thio-TEPA, Busulfan, 6-Mercaptopurine, 6-Thioguanine, 5-Fluorouracil, Cytosine Arabinoside, Adriamycin, Dactinomycin, Daunomycin, Bleomycin, Mithramcycin, Mitomycin-C, BCNU, CCNU, Methyl-CCNU, DTIC, Hydroxyurea, Cis-Platinum (cis-platinum (II) diamminedichloride) , Procarbazine, Hexamethylmelamine, L-Asparaginase, and the like.
  • Androgens Estrogens, Anti-estrogen, Prog
  • perfluoro compounds useful as RS agents but which also have radiopaque properties are particularly valuable for the purposes of the present invention.
  • Such compounds include brominated perfluorohydrocarbons such as F-perfluoroctylbromide and brominated perfluoroethers, such as F-1-bromobutylisopropylether, F-1-bromoethylisopropyl ether and other brominated perfluoro organo ethers described, for example, in U.S. Patent 3,453,333.
  • the radioimaging properties of such compounds permit monitoring of their RS effects as well as toxicity to surrounding normal cells and hence serve as diagnostic agents as well as RS agents.
  • the dispersions containing the perfluoro compounds may be formulated with other, known, radiopaque agents in order to provide a similar opportunity for monitoring radiosensitization potential.
  • the radioimaging may be practiced as in conventional radiography or computer axial tomography (CAT) radiography, or by the newer NMR techniques.
  • the brominated compounds as RI agents may be used neat or in aqueous dispersion, for example as oil-in-water or water-in-oil emulsions containing about 10-90% by volume of water and about 0.5-10% by weight of a dispersant.
  • Radioprotection may also be practiced in conjunction with the radiosensitization of the invention.
  • Radioprotective agents are those which preferentially protect normal tissues from radiation injury. When practiced with radiosensitization, the objective is to reduce injury to the normal tissues, which injury may occur when the RS agents are used in the absence of the RP agents.
  • Sulfhydryl- containing agents generally are known to be effective RP materials, such as aminoethylisothiuronium or the phosphorothioate derivatives of beta-mercaptoethylamine reviewed in the article by J. M. Yuhas, "On the Potential Application of Radioprotective Drugs in Solid Tumor Radiotherapy," appearing in Radiation - Drug Interactions in the Treatment of Cancer, edited by G. H.
  • a surfactant solution was prepared by dispersing in water a sufficient amount of the following amidoamine oxide surfactant ("AAO") to provide a 2% by weight solution:
  • Dispersion A The dispersion (hereinafter identified as "Dispersion A”) was then filtered through a 0.22 micron "Millipore” Ctrademark) filter and kept refrigerated at 4oC. until use.
  • Multicellular tumor spheroids are produced by placing 10 6 MCa-11 murine mammary tumor cells in 10 mis of Eagles Basal Medium (“EBME”) , Grand Island Biological Co., catalog No.” 420-1200, into a 100 mm petri dish which has been base coated with 0.75% noble agar in the EBME. Within 7-10 days spherical aggregates of tumor cells appear and are then ready for study.
  • the PFC dispersion to be tested is adjusted to 290 milliosmoles, osmolarity with powdered tissue culture medium and adjusted to pH 7.2 to 7.4 with 0.1N NaOH or HCl. Other details of preparation and use of the MTS are given in J. M.
  • Either standard tissue culture medium (EBME) or the PFC dispersion is gassed with 100% oxygen for a period of fifteen minutes and then transferred, along with the spheroids, into non-heparinized capillary tubes and sealed. At intervals of 0 to 60 minutes later the tubes are exposed to graded doses of 250 kVp X-rays, and within 30 minutes thereafter are removed, washed with medium and placed individually in agar coated 16 mm wells along with 1.5 cc of medium. Using a dissecting scope at 40 power the spheroids are sized three times weekly and the medium is changed twice weekly.
  • EBME tissue culture medium
  • the PFC dispersion is gassed with 100% oxygen for a period of fifteen minutes and then transferred, along with the spheroids, into non-heparinized capillary tubes and sealed. At intervals of 0 to 60 minutes later the tubes are exposed to graded doses of 250 kVp X-rays, and within 30 minutes thereafter are removed, washed with medium
  • Dispersions A and B provided similar levels of toxicity and radiosensitivity.
  • the toxicity exhibited by Dispersions A and B is considered negligible and likely to be relatively tolerable in the cardiovascular system.
  • the toxicity exhibited by Dis persion C although higher than that of Dispersions A and B, does not disqualify Dispersion C from use as a sensitizer in mammals; such toxicity is relative to various factors. such as RS reagent and radiation dosage, and tumor type and location, and therefore Dispersion C would not necessarily be excluded from clinical evaluation.
  • the data of Tables I and II is not directly comparable; larger spheroids were used in the experiments reported in Table I than were used in the experiments reported in Table II. However, the larger spheroids provide added bias (larger spheroids are more difficult to sensitize) and therefore the results of Table I indicate highly beneficial sensitization.
  • Dispersion C is a more effective radiosensitizer than either Dispersion A or Dispersion B. This is in all probability not true for two reasons.
  • the studies with Dispersion C were preliminary and involved MTS with a smaller fraction of radioresistant hypoxic cells at the time of treatment than was the case for the studies with Dispersions A and B.
  • Dispersion C was, in itself, growth inhibitory, and it is likely that this property in some way enhanced the tumor cell destruction
  • Example 3 In Vivo Studies (Residence Times) The rate of clearance of PFC Dispersions A and B from the circulation was evaluated in both Fisher 344 rats and BALB/c mice (females in both cases). The dispersions were injected intravenously to a PFC dose equal to one-third of the circulatory volume, which is equal to 6% of body weight. Within 30 minutes of . injection, the animal returns to the normovolemic state as evidenced by the fact that the fluorocrit equals 3.1% compared to the theoretical estimate of 3.3% for these Dispersions. At graded intervals through 8 hours after injection, blood is drawn in microcapillary tubes from the supraorbital sinus. Following centrifugation for 15 minutes at 12,000 times gravity, the fluorocrit
  • CPFC as a percent of the blood volume
  • hematocrit is read on a microscope.
  • the PFC collects as a pellet in the bottom of the tubes, followed by the red blood cells and the plasma, thus forming distinct layers. All data are normalized to the 30 minute centrifugation reading and the rate of decline of the fluorocrit is estimated from a standard single compartment exponential decay curve defined by:
  • Example 4 The MTS experiments of Example 2 were repeated in all essential respects with Dispersion B but using spheroids derived from human tumor lines which contain hypoxic cells when grown as MTS. As shown in Table III below, some toxicity was observed in all cases but the levels are considered relatively tolerable. Moderate radiosensitizing is apparent for the two neuroblastoma cell lines but very high radio-sensitization is shown with respect to the melanoma line. The latter is an outstanding result due to the prevalence and high risks known for this form of hypoxic tumor cells. Very little RS effect is shown for the osteosar ⁇ oma cell line but these results are only preliminary and the exposure was at a low radiation level.
  • Radiosensitization of the 3M2N mammary tumor growing in the right hind leg of Fisher -344 rats was studied. At 10-14 days after subcutaneous transplantation in the rats the tumors were 6-8 mm in diameter and ready for treatment. The control animais either received no treatment or received various radiation doses. The other animals received I.V. infusion of 20 ml/kg of Dispersion B (20% w/v) followed by 30 minutes breathing of 95% O 2 /5% CO 2 gas mixture (at 1 atm) and then by the various radiation doses of x-rays. Prior to and three times weekly after treatment, the two orthogonal diameters of the tumors were measured in situ and averaged.
  • Table V below expresses the results of the study as the time required for the tumors to grow 8mm beyond their size at the time of treatment.
  • the data show that the enhancement produced by the PFC dispersion increases with radiation dose, and also that the growth delay per rad is significantly higher in the PFC- treated group than in the control. That the enhancement is due to the combination of the PFC dispersion and breathing of the gas mixture is evident from Table VI below in that none of the control treatments were capable of producing the growth delay of the combination.
  • Example 7 In Vitro Chemosensitization The potentiation by PFC dispersions of chemotherapeutic agents was demonstrated by the anti-tumor effect of methotrexate ("MTX") in NB-100 neuroblastoma multicellular tumor spheroids ("MTS").
  • MTX methotrexate
  • MTS neuroblastoma multicellular tumor spheroids
  • the spheroids were exposed to from 0 to 5x10 -6 molar methotrexate in control medium and in Dispersion B equilibrated with a 95% O 2 /5% CO 2 mixture.
  • Table VII show that the PFC dispersion enhanced the effectiveness of MTX as evidenced by the delay in growth relative to the spheroids treated only with MTX.
  • sensitization to MTX in these spheroids can be achieved by gassing with the gas mixture in medium alone, such sensitization requires 1 to 2 hour pretreatment as opposed to only 30 minutes with the PFC dispersion, thus clearly demonstrating the feasibility of elevating the therapeutic index of this important anti-cancer drug with PFC.
  • the preferential solubility of lipophilic drugs in PFC compositions not only provides a means for enhancing the delivery of such drugs in animals but also opens up opportunity for controlling residence time of the drug in the animal, for example by prolonging release of the drug from PFC circulating to the plasma and target organs.
  • sustained low level delivery of a drug for a prolonged period is made possible with an aqueous delivery system.
  • Enhancement of Chemotherapy This example illustrates enhancement of anti-tumor action of Vincristine, a lipophilic drug to which tumors are normally resistent at least to non-lethal doses thereof.
  • the enhancement is believed due to the preferential solubility of the drug in the PFC material.
  • the MCa-11 mammary carcinoma was transplanted into the thigh of BALB/c mice and grown to a diameter of 6mm, at which time the mice were treated.
  • Control mice received an injection of saline, while Vincristine treatment consisted of a single dose of 1.5 mg/kg of Vincristine administered intraperitoneally.
  • PFC treatment consisted of an i.v. injection of 20 ml/kg of Dispersion B, followed by two hours of breathing carbogen C95% O 2 /5% CO 2 ) , and injection of saline of Vincristine as before, followed by another two hours of carbogen breathing. It was observed that the Vincristine treatment alone had no effect on tumor growth.

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US4956390A (en) * 1987-08-25 1990-09-11 Air Products And Chemicals, Inc. Gas transport employing perfluorobutyldecalin
EP0279379B1 (en) * 1987-02-20 1992-11-04 Air Products And Chemicals, Inc. Interstitial administration of perfluorchemical emulsions for reoxygenation of hypoxic tumor cells
WO1993018748A1 (en) * 1992-03-19 1993-09-30 Allergan, Inc. Compositions comprising a drug delivery vehicle suspended in a nonaqueous fluorinated liquid
EP0491685A4 (en) * 1989-08-28 1993-10-13 K. Michael Sekins Lung cancer hyperthermia via ultrasound and/or convection with perfluorocarbon liquids
US5480914A (en) * 1994-05-06 1996-01-02 Allergan, Inc. Nonaqueous thixotropic drug delivery suspensions and methods of their use
US5518731A (en) * 1990-09-27 1996-05-21 Allergan, Inc. Nonaqueous fluorinated drug delivery vehicle suspensions
US5562608A (en) * 1989-08-28 1996-10-08 Biopulmonics, Inc. Apparatus for pulmonary delivery of drugs with simultaneous liquid lavage and ventilation
US6113919A (en) * 1991-07-17 2000-09-05 Alliance Pharmaceutical Corp. Preparations comprising a fluorocarbon or a highly fluorinated compound and a lipophilic/fluorophilic compound and their uses
US6458376B1 (en) 1990-09-27 2002-10-01 Allergan, Inc. Nonaqueous fluorinated drug delivery suspensions
EP2587917A4 (en) * 2010-07-01 2015-05-06 Mtm Res Llc FLUORCHEMICAL ANTIFIBROBLAST EMULSION THERAPIES

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JPS59130813A (ja) * 1983-01-14 1984-07-27 Green Cross Corp:The 癌化学療法補助剤
JPS59130812A (ja) * 1983-01-14 1984-07-27 Green Cross Corp:The 癌化学療法補助剤
CA1257828A (en) * 1984-04-16 1989-07-25 William Mccormick Perfluoro compound dispersions containing reduced amounts of surfactant and process of preparation
US4815446A (en) * 1985-05-09 1989-03-28 Alpha Therapeutic Corporation Process for treating metastasis of cancerous tumors
DE4221268C2 (de) * 1992-06-26 1997-06-12 Lancaster Group Ag Verwendung eines Dermatikums zur Unterstützung des Sauerstofftransportes in der Haut
DE4221256C2 (de) * 1992-06-26 1997-07-10 Lancaster Group Ag Galenische Zusammensetzung für die topische Anwendung
US5643601A (en) * 1992-06-26 1997-07-01 Lancaster Group Ag Phospholipid-and fluorocarbon-containing cosmetic
AU4645099A (en) 1998-07-09 2000-02-01 Yoram Harth Apparatus and method for efficient high energy photodynamic therapy of acne vulgaris and seborrhea
US20040122492A1 (en) 1999-07-07 2004-06-24 Yoram Harth Phototherapeutic treatment of skin conditions
GB0200721D0 (en) * 2002-01-14 2002-02-27 Univ Bristol Toxicity test
RU2440158C2 (ru) * 2010-02-25 2012-01-20 Юрий Александрович Белый Способ фотодинамической терапии субъектов, страдающих злокачественными опухолями

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Cited By (15)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP0279379B1 (en) * 1987-02-20 1992-11-04 Air Products And Chemicals, Inc. Interstitial administration of perfluorchemical emulsions for reoxygenation of hypoxic tumor cells
US4956390A (en) * 1987-08-25 1990-09-11 Air Products And Chemicals, Inc. Gas transport employing perfluorobutyldecalin
US5562608A (en) * 1989-08-28 1996-10-08 Biopulmonics, Inc. Apparatus for pulmonary delivery of drugs with simultaneous liquid lavage and ventilation
EP0491685A4 (en) * 1989-08-28 1993-10-13 K. Michael Sekins Lung cancer hyperthermia via ultrasound and/or convection with perfluorocarbon liquids
US5707352A (en) * 1989-08-28 1998-01-13 Alliance Pharmaceutical Corp. Pulmonary delivery of therapeutic agent
US5788665A (en) * 1989-08-28 1998-08-04 Alliance Pharmaceutical Corp. Apparatus for pulmonary therapy
US6166092A (en) * 1989-08-28 2000-12-26 Alliance Pharmaceutical, Corp. Fluorocarbon compositions for pulmonary therapy
US6242472B1 (en) 1989-08-28 2001-06-05 Alliance Pharmaceutical Corp. Methods for the pulmonary delivery of biological agents
US5518731A (en) * 1990-09-27 1996-05-21 Allergan, Inc. Nonaqueous fluorinated drug delivery vehicle suspensions
US6458376B1 (en) 1990-09-27 2002-10-01 Allergan, Inc. Nonaqueous fluorinated drug delivery suspensions
US6113919A (en) * 1991-07-17 2000-09-05 Alliance Pharmaceutical Corp. Preparations comprising a fluorocarbon or a highly fluorinated compound and a lipophilic/fluorophilic compound and their uses
US6528545B1 (en) * 1991-07-17 2003-03-04 Jean G. Riess Preparations comprising a fluorocarbon or highly fluorinated compound and a lipophilic/fluorophilic organic compound, and their uses
WO1993018748A1 (en) * 1992-03-19 1993-09-30 Allergan, Inc. Compositions comprising a drug delivery vehicle suspended in a nonaqueous fluorinated liquid
US5480914A (en) * 1994-05-06 1996-01-02 Allergan, Inc. Nonaqueous thixotropic drug delivery suspensions and methods of their use
EP2587917A4 (en) * 2010-07-01 2015-05-06 Mtm Res Llc FLUORCHEMICAL ANTIFIBROBLAST EMULSION THERAPIES

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