JPS6042322A - Novel emulsified preparation - Google Patents
Novel emulsified preparationInfo
- Publication number
- JPS6042322A JPS6042322A JP15019983A JP15019983A JPS6042322A JP S6042322 A JPS6042322 A JP S6042322A JP 15019983 A JP15019983 A JP 15019983A JP 15019983 A JP15019983 A JP 15019983A JP S6042322 A JPS6042322 A JP S6042322A
- Authority
- JP
- Japan
- Prior art keywords
- water
- oil
- iodized
- aqueous solution
- emulsified
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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- Medicinal Preparation (AREA)
Abstract
Description
【発明の詳細な説明】
本発明は水、ヨード化油、水溶性有機ヨウ素化合物、界
面活性剤及び有効成分からなる乳化製剤に関する。DETAILED DESCRIPTION OF THE INVENTION The present invention relates to an emulsified formulation consisting of water, an iodized oil, a water-soluble organic iodine compound, a surfactant and an active ingredient.
本発明の製剤は水溶性の有効成分をリンパ管系に長時間
局在させることができるので、種々のリンパ管系の疾患
の予防及び治療に利用しうる。Since the formulation of the present invention can localize water-soluble active ingredients in the lymphatic system for a long time, it can be used for the prevention and treatment of various lymphatic system diseases.
ヨード化油を製剤に応用する試みはすでになでれている
。例えば今野等はヨード化油の一種であるヨード化ケシ
油脂肪酸エチルエステルをj匝瘍の栄養血管内に注入す
ると、腫瘍に選択的かつ長期に停滞することを発見し、
またこの特性を利用して親油性制癌剤スマンスクのヨー
ド化ケシ油脂肪酸エチルエステル溶液を肝動脈内に投与
すると、スマンスクが肝臓腫瘍に選択的に到達すること
を報告している(癌と治療、第9巻200〜2015頁
1982年)
又、本発明者の1人である井目等は、ヨード化ケシ油脂
肪酸エチルエステルに関してさらに研究を進め、これを
ラットの鼠径部リンパ節に注入すると、リンパ管内では
急速に分散せず、24時間後にもリンパ管系に局在する
ことを発見した。この事実は親油性の有効成分をヨード
化油に溶解した製剤はリンパ管系の各種疾患に有効であ
ることを推察させる。Attempts have already been made to apply iodized oils in formulations. For example, Konno et al. discovered that when iodized poppy oil fatty acid ethyl ester, which is a type of iodized oil, was injected into the feeding blood vessels of ulcers, it selectively remained in the tumor for a long time.
It has also been reported that, utilizing this property, when an iodized poppy oil fatty acid ethyl ester solution of the lipophilic anticancer drug Sumansuk is administered into the hepatic artery, Sumansuk selectively reaches liver tumors (Cancer and Treatment, Vol. (Vol. 9, pp. 200-2015, 1982) In addition, Ime et al., one of the inventors of the present invention, conducted further research on iodized poppy oil fatty acid ethyl ester, and found that when this was injected into the inguinal lymph nodes of rats, lymph It was discovered that it did not disperse rapidly within the ducts and was localized in the lymphatic system even after 24 hours. This fact suggests that preparations in which lipophilic active ingredients are dissolved in iodized oil are effective against various diseases of the lymphatic system.
しかしながら、多くの有効成分は水溶性であり、ヨード
化油には溶けないため、水溶性の有効成分を用いて上述
のような製剤を製造することは不可能である。However, it is not possible to produce such formulations using water-soluble active ingredients, since many active ingredients are water-soluble and not soluble in iodized oils.
そこで、本発明者等は水溶性の有効成分にも上述のよう
な製剤を製造すべく種々検討を行った結果、水、ヨード
化油、水溶性有機ヨウ素化合物、界面活性剤及び水溶性
の有効成分からなる乳化製剤は、経時安定性が良好で、
かつリンパ管系の疾患に有効であることを見い出した。Therefore, the present inventors conducted various studies in order to manufacture the above-mentioned formulations using water-soluble active ingredients. Emulsified formulations consisting of ingredients have good stability over time,
It was also found to be effective for diseases of the lymphatic system.
本発明は上記知見に基づき完成されたものである。The present invention has been completed based on the above findings.
本発明において使用するヨード化油としては、不飽和脂
肪酸及びそのエステル、さらにこれらを含む植物及び動
物性油脂類のヨード化物があげられ、具体的にはオリー
ブ油、落花生油、ヒマシ油、ヤシ油、綿実油、ゴマ油、
ケシ油、硬化ヒマシ油、ナタネ油、カカオ脂、卵黄脂、
牛脂、豚脂、ラノリン、鱈肝油等のヨード化物があげら
れる。これらヨード化油のヨード含量は15〜s o
W/W Li6、より好ましくは30〜45 W/W%
のものである。Iodized oils used in the present invention include unsaturated fatty acids and their esters, as well as iodized products of plant and animal fats and oils containing these, and specifically include olive oil, peanut oil, castor oil, coconut oil, cottonseed oil, sesame oil,
Poppy oil, hydrogenated castor oil, rapeseed oil, cocoa butter, egg yolk fat,
Examples include iodized products such as beef tallow, pork fat, lanolin, and cod liver oil. The iodine content of these iodized oils is 15 to s o
W/W Li6, more preferably 30-45 W/W%
belongs to.
このものの製剤含量に対する含有比率は99〜2、 O
W/W % 、好ましくは87−55 W/W %程度
である0
水溶性ヨウ素化合物としては水への溶解度が通常50%
以上、好ましくは40チ以上で、その水溶液の比重が1
・2−L5程度になるものであれば特に制限はなく、例
えばイオヵルム酸メグルミン、アジビオトンメグルミン
、イオトロクス酸プロビリオドン、メトリゾ酸、アミト
ドリゾ酸ナト1)、ラム、アミトドリゾ酸メグルミン、
メトリゾ酸ナトリウム、ヨーダミドメグルミン、イオタ
ラム酸ナトリウム、イオタラム酸メグルミン等があげら
れる。このものの製剤全量に対する使用比率は0・1〜
75W/w%、好捷シ<は4.5−55 W/W、%程
度である。The content ratio of this to the formulation content is 99-2, O
W/W %, preferably about 87-55 W/W %0 As a water-soluble iodine compound, the solubility in water is usually 50%.
or more, preferably 40 inches or more, and the specific gravity of the aqueous solution is 1
- There is no particular restriction as long as it is about 2-L5, for example, meglumine iocalmate, azibioton meglumine, proviriodone iotroxate, metrizoic acid, sodium amitodorizoate 1), rum, meglumine amitodorizoate,
Examples include sodium metrizoate, iodamide meglumine, sodium iothalamate, meglumine iothalamate, and the like. The usage ratio of this product to the total amount of the preparation is 0.1~
75 W/W%, and the efficiency is about 4.5-55 W/W%.
界面活性剤としては、物理的に安定な乳化製剤を作製で
きるものであれば特に制限はないが、好■
1、い1.7)よ6、ゆ、Tween B (3ヨ。。There are no particular restrictions on the surfactant as long as it can produce a physically stable emulsion, but preferred surfactants include 1, 1, 7), 6, Tween B, and 3.
−68■■
5pan85、蔗糖脂肪酸エステル類、レシチン等があ
げられる。-68■■ 5pan85, sucrose fatty acid esters, lecithin, etc.
このものの製剤全量に対する使用比率はα01+ 25
W/W%、好tL<は(11−15W/W%程度であ
る。The usage ratio of this product to the total amount of the preparation is α01+ 25
W/W%, preferably tL<, is about (11-15 W/W%).
本発明において使用する水は注射用の精製水が好捷しく
、その使用割合は製剤全量に対しa1〜64W/w係、
好ましくは2〜37 W/Wチ程度である。The water used in the present invention is preferably purified water for injection, and its usage ratio is a1 to 64 W/w based on the total amount of the preparation.
Preferably it is about 2 to 37 W/W.
有効成分としては特に制限はないが、水浴性のものが好
ましく、例えば制癌剤、具体的に例示するとアクチノマ
イシンD1塩酸アクラルピシン、塩酸ダウノルビシン、
シトシンアラビノシツド、塩酸プレオマイシン、硫酸ペ
プロマイシン、クロモマイシンA3、ネオカルチノスタ
チン、マイトマイシンC,硫mビンブラスチン、硫酸ビ
ンクリスチン、メルカプトプリンリボシド、フルオロウ
ラシル、ピシパニール、フトラフール、シタラビン、シ
クロホスファミド、カルボコン塩酸アンシタビン、シス
プラチン、L−アスパラギナーゼ、メトトレキザート、
及び塩酸クロルメチン−N −オキ7ド等があげられ、
その他、抗菌性物質、例エバセファロチン、セフメタゾ
ールなどのセファロスポリン系、セファマイシン系の抗
生物質やゲンタマイシンなどの抗生物質などがあげられ
、又塩酸リドカインなどの局所麻酔剤などがあげられる
。その使用割合は製剤全量に対し、[105〜1Q W
/W係、好ましくはα1−5Wβチ程度である。The active ingredient is not particularly limited, but it is preferably water-based, such as anticancer agents, such as actinomycin D1, aclarpicin hydrochloride, daunorubicin hydrochloride,
Cytosine arabinoside, pleomycin hydrochloride, pepromycin sulfate, chromomycin A3, neocarzinostatin, mitomycin C, vinblastine sulfate, vincristine sulfate, mercaptopurine riboside, fluorouracil, pisipanil, ftrafur, cytarabine, cyclophosphamide, carbocone Ancitabine hydrochloride, cisplatin, L-asparaginase, methotrexate,
and chlormethine-N-oxide hydrochloride, etc.
Other examples include antibacterial substances such as cephalosporins such as evacephalothin and cefmetazole, antibiotics such as cephamycins and gentamicin, and local anesthetics such as lidocaine hydrochloride. The usage rate is [105~1Q W
/W ratio, preferably about α1-5Wβchi.
本発明の製剤を製造するには例えば次のようにすればよ
い。即ち、まずヨード化油2・0〜99重量部好ましく
は87〜33重量部に界面活性剤001〜25重量部、
好ましくはα1〜15重量部添加して均一に混合する。For example, the preparation of the present invention may be produced as follows. That is, first, 2.0 to 99 parts by weight of iodized oil, preferably 87 to 33 parts by weight, 0.0 to 25 parts by weight of surfactant,
Preferably, α1 to 15 parts by weight are added and mixed uniformly.
別に精製水に水溶性有機ヨウ素化合物をその水溶液の比
重が1.2〜15、好ましくは1.25〜1.4となる
ように添加溶解する。このときの水溶性有機ヨウ素化合
物の濃度は約20〜9. Q W/W %、好ましくは
45〜80 W/W %程度となる。次いでこの液に有
効成分を加え均一に溶解させる。Separately, a water-soluble organic iodine compound is added and dissolved in purified water so that the specific gravity of the aqueous solution is 1.2 to 15, preferably 1.25 to 1.4. The concentration of the water-soluble organic iodine compound at this time is about 20 to 9. Q W/W %, preferably about 45 to 80 W/W %. Next, the active ingredient is added to this liquid and uniformly dissolved.
上記のようにして得られンζヨード化油と水溶液を合し
、ホモジナイザー、シェーカーなどを用い通常の方法で
乳化をすればよい。通常10〜60分で乳化は完了する
。ヨード化油に対する水溶液の使用割合は容量比でα0
1〜4、好ましくは01〜2程度である。The ζ-iodized oil obtained as described above and an aqueous solution may be combined and emulsified using a homogenizer, shaker, etc. in a conventional manner. Emulsification is usually completed in 10 to 60 minutes. The ratio of aqueous solution to iodized oil is α0 by volume.
1 to 4, preferably about 01 to 2.
本発明の乳化製剤はリンパ系や腫瘍部分に有効成分を選
択的にかつ長期に停滞させうるものなので、有効成分と
して制癌剤を用い、リンパ系や腫瘍の栄養血管に木兄8
A製剤を直接投与すると極めて効率よ〈制癌効果が発揮
される。特に最近の腺癌の治療法は、制癌剤の多剤併用
が常識化しているが、本発明の製剤を利用すると1種な
いし数種の親油性制癌剤をヨード化油層に1種ないし数
種の親水性制癌剤を水溶性有機ヨウ素化合物の水溶液に
加えて多剤併用することが可能であり、制癌効果をより
高めることができる。The emulsified preparation of the present invention is capable of selectively retaining active ingredients in the lymphatic system and tumor areas for a long period of time.
When Preparation A is directly administered, it exhibits an extremely efficient anticancer effect. Particularly in recent treatments for adenocarcinoma, it has become common practice to use multiple anticancer drugs in combination, but when using the preparation of the present invention, one or more lipophilic anticancer drugs are added to the iodized oil layer. It is possible to use multiple anticancer drugs in combination by adding them to an aqueous solution of a water-soluble organic iodine compound, and the anticancer effect can be further enhanced.
次に、本発明の内容および効果を実施例および実験例に
おいて具体的に説明する。Next, the contents and effects of the present invention will be specifically explained in Examples and Experimental Examples.
実施例1
ヨード化ケシ油脂肪酸エチルエステル(ヨウ素含有率約
40 W/W%) 7.3@J%Tween ao [
124■
me、 5pan 85 n 47mlの混合溶液と、
塩酸プレオマイシン300岬力価、01Mリン酸ナトリ
ウム緩衝液(pH5・0)α36d1アミトドリゾ酸メ
グルミンの75チ水溶液(比重1.213 ) 1.5
2dの混合溶液とをホモジナイザーで十分に攪拌し乳化
させ乳化製剤10mを得る。Example 1 Iodinated poppy oil fatty acid ethyl ester (iodine content approximately 40 W/W%) 7.3@J% Tween ao [
124■me, 5pan 85n 47ml mixed solution,
Pleomycin hydrochloride 300 Misaki titer, 01M sodium phosphate buffer (pH 5.0) α36d1 aqueous solution of meglumine amitodrizoate (specific gravity 1.213) 1.5
2d and the mixed solution were thoroughly stirred and emulsified using a homogenizer to obtain 10 m of emulsified preparation.
実施例2
ヨード化ゴマ油(ヨウ素含有率約3 b W/W、%
)7.5rd、ポリオキシエチレン硬化ヒマク油誘導体
■
HCO−600,25p、 5pan ao 0.5m
(7)混合溶液と、5−フルオロウラシル100■、イ
オタラム酸メグルミンの65%水溶液(比重1..27
)1・65#l/の混合溶液とをホモジナイザーで十分
に攪拌し、乳化させ乳化製剤10dを得る。Example 2 Iodized sesame oil (iodine content approximately 3 b W/W, %
) 7.5rd, polyoxyethylene hydrogenated castor oil derivative ■ HCO-600, 25p, 5pan ao 0.5m
(7) Mixed solution, 5-fluorouracil 100μ, and 65% aqueous solution of meglumine iothalamate (specific gravity 1..27)
) 1.65#l/mixed solution is sufficiently stirred with a homogenizer to emulsify and obtain emulsified preparation 10d.
実施例3
ヨード化落花生油脂肪酸プロピルエステル(ヨ■
つ素含有率約” ”9v%’) 7.Otrtl、Tw
een 800.51m11卵黄レシチン0.5Ofの
混合溶液と、モジナイザーで十分に攪拌し乳化させ乳化
製剤10sJを得る。Example 3 Iodized peanut oil fatty acid propyl ester (iodine content approx. 9v%) 7. Otrtl, Tw
A mixed solution of een 800.51ml11 egg yolk lecithin 0.5Of is thoroughly stirred and emulsified using a modinizer to obtain 10 sJ of an emulsified preparation.
実施例4
実施例1にオL、、テTween’ B Oを0− i
mg %5pan85を0.6縦用い、又、プレオマ
イシンのかわ抄にゲンタマイシン150Wiを使用する
以外は実施例1と同様にして乳化剤10dを得る。Example 4 In Example 1, 0-i
Emulsifier 10d was obtained in the same manner as in Example 1, except that 0.6 mg%5pan85 was used vertically and gentamicin 150Wi was used in the pleomycin wash.
実験例1
本発明の乳化製剤の物理的安定性の確認実験(1) 試
料
A−1:実施例1で得た乳化製剤。比重1・28゜A−
2=実施例1におけるアミトドリゾ酸メグルミン75%
水溶液の代わりに、
蔗糖75%水溶液(比重1.1a)を
用いて調製した乳化製剤。Experimental Example 1 Experiment to confirm the physical stability of the emulsified formulation of the present invention (1) Sample A-1: Emulsified formulation obtained in Example 1. Specific gravity 1.28゜A-
2 = 75% meglumine amitodorizoate in Example 1
An emulsion preparation prepared using a 75% sucrose aqueous solution (specific gravity 1.1a) instead of an aqueous solution.
A−3=実施例1におけるアミトドリゾ酸メグルミン7
5%水溶液の代わりに、
塩化ナトリウム20チ水溶液(比重
1.1S)を用いて調製した乳化製剤。A-3 = Amitodorizoate meglumine 7 in Example 1
An emulsion preparation prepared using a 20% sodium chloride aqueous solution (specific gravity 1.1S) instead of a 5% aqueous solution.
B−18実施例2で得た乳化製剤。B-18 Emulsified formulation obtained in Example 2.
B−2:実施例2におけるイオタラム酸メグルミン65
%水溶液の代わりに蔗糖
65%水溶液(比重1・16)を用い
て調製した乳化製剤。B-2: Meglumine iothalamate 65 in Example 2
An emulsified preparation prepared using a 65% sucrose aqueous solution (specific gravity 1.16) instead of a 65% aqueous solution.
B−3:実施例2におけるイオタラム酸メグルミン65
チ水溶液の代わりに、塩
化ナトリウム20%水溶液(比重
1.15)を用いて調製した乳化、製剤。B-3: Meglumine iothalamate 65 in Example 2
Emulsions and formulations prepared using a 20% aqueous sodium chloride solution (specific gravity 1.15) instead of an aqueous solution of sodium chloride.
(2) 実験方法
試料A−1〜B−5の6種の乳化製剤10rneヲ容量
10 mlのメヌシリンダーに注入し、注入直後50分
、1,2.24及び72時間後における外観の変化を肉
眼観察した。評価は、次の通り。(2) Experimental method: Inject 10 volumes of six types of emulsified preparations, Samples A-1 to B-5, into a 10 ml menu cylinder, and observe changes in appearance 50 minutes immediately after injection, 1, 2, 24, and 72 hours later. Observed with the naked eye. The evaluation is as follows.
++:十分乳化している。++: Sufficiently emulsified.
+ :やや相分離気味。+: Slight phase separation.
± :大分相分離し穴。±: Hole with large phase separation.
−一完全に相分離した。- Complete phase separation.
(3) 結果と考察
下表の観察結果から明らかなように、水層の比重が1.
25以上である本発明の乳化製剤A−1及びB−1は、
水溶性ヨード化合物の代わりに、水浴液の比重が1・2
以下である蔗糖や塩化ナトリウムを用いた製化製剤に比
較して時間の経過に対して、相分離することなく安定に
乳化していることがわかる。(3) Results and Discussion As is clear from the observation results in the table below, the specific gravity of the water layer is 1.
The emulsified formulations A-1 and B-1 of the present invention having a molecular weight of 25 or more are:
Instead of water-soluble iodine compounds, the specific gravity of the water bath liquid is 1.2.
It can be seen that compared to the following formulations using sucrose and sodium chloride, the emulsification is stable over time without phase separation.
実験例2
担癌ラットに対する投与実験
(1) 実験方法
Don ryu系ラットの右腸骨リンパ節にAH−66
を移植し、翌日より連続5日間、本発明における実施例
1の乳化製剤o、1m6(塩酸プレオマイシンとして3
my力価含准)を投与し2Yoこの際比較対照として
塩酸プレオマイシン3■を含む水溶液を静脈内に投与し
た。Experimental Example 2 Administration experiment on tumor-bearing rats (1) Experimental method AH-66 was administered to the right iliac lymph node of Don ryu rats.
was transplanted, and for 5 consecutive days starting from the next day, 1 m6 of the emulsified preparation o of Example 1 of the present invention (3 m6 as pleomycin hydrochloride) was added.
At this time, as a control, an aqueous solution containing 3 pleomycin hydrochloride was administered intravenously.
(2) 結果と考察 投与60日後の生存率を次表に示す。(2) Results and discussion The survival rate 60 days after administration is shown in the following table.
実施例1の乳化製剤のリン・;筒内投与は、常法である
水溶液の静脈内投与より秀れア’t 市114&効果を
示していることがわかる。It can be seen that in-cylinder administration of the emulsified preparation of Example 1 has a superior effect to intravenous administration of an aqueous solution, which is a conventional method.
特許出願人2 日本化薬株式会社Patent applicant 2 Nippon Kayaku Co., Ltd.
Claims (1)
面活性剤及び有効成分からなる乳化製剤。(1) An emulsified preparation consisting of water, iodized oil, a water-soluble organic iodine compound, a surfactant, and an active ingredient.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP15019983A JPS6042322A (en) | 1983-08-19 | 1983-08-19 | Novel emulsified preparation |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP15019983A JPS6042322A (en) | 1983-08-19 | 1983-08-19 | Novel emulsified preparation |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPS6042322A true JPS6042322A (en) | 1985-03-06 |
| JPH0524132B2 JPH0524132B2 (en) | 1993-04-06 |
Family
ID=15491679
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP15019983A Granted JPS6042322A (en) | 1983-08-19 | 1983-08-19 | Novel emulsified preparation |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JPS6042322A (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP0532703A1 (en) * | 1990-06-08 | 1993-03-24 | IBAH, Inc. | Process for preparing microemulsion |
| CN110302434A (en) * | 2019-07-14 | 2019-10-08 | 大连医科大学 | A kind of Lipiodol embolizatim agent and preparation method thereof for being easy to inject |
-
1983
- 1983-08-19 JP JP15019983A patent/JPS6042322A/en active Granted
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| EP0532703A1 (en) * | 1990-06-08 | 1993-03-24 | IBAH, Inc. | Process for preparing microemulsion |
| CN110302434A (en) * | 2019-07-14 | 2019-10-08 | 大连医科大学 | A kind of Lipiodol embolizatim agent and preparation method thereof for being easy to inject |
Also Published As
| Publication number | Publication date |
|---|---|
| JPH0524132B2 (en) | 1993-04-06 |
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