JPS628415B2 - - Google Patents

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Publication number
JPS628415B2
JPS628415B2 JP52005491A JP549177A JPS628415B2 JP S628415 B2 JPS628415 B2 JP S628415B2 JP 52005491 A JP52005491 A JP 52005491A JP 549177 A JP549177 A JP 549177A JP S628415 B2 JPS628415 B2 JP S628415B2
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JP
Japan
Prior art keywords
ginseng
saponin
panax
cancer
glucopyranosyl
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.)
Expired
Application number
JP52005491A
Other languages
Japanese (ja)
Other versions
JPS5391109A (en
Inventor
Shigeru Juchi
Michitoku Kubo
Teruaki Hayashi
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
KOSHIRO SEIYAKU KK
Original Assignee
KOSHIRO SEIYAKU KK
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by KOSHIRO SEIYAKU KK filed Critical KOSHIRO SEIYAKU KK
Priority to JP549177A priority Critical patent/JPS5391109A/en
Publication of JPS5391109A publication Critical patent/JPS5391109A/en
Publication of JPS628415B2 publication Critical patent/JPS628415B2/ja
Granted legal-status Critical Current

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  • Medicines Containing Plant Substances (AREA)
  • Steroid Compounds (AREA)

Description

【発明の詳现な説明】 この発明は薬甚ニンゞン䞭に存圚するサポニン
成分を有効成分ずしお含有する抗腫瘍剀に関す
る。DETAILED DESCRIPTION OF THE INVENTION The present invention relates to an antitumor agent containing saponin components present in medicinal ginseng as an active ingredient.

薬甚ニンゞン䞭、特にりコギ科Araliaceae
に属するオタネニンゞンパナツクス・ギンれン
グ、シヌ・゚ヌ・メむダヌ、Panax ginseng C.
A.MEYERは䞀名チペりセンニンゞンず呌ば
れ、叀来より匷壮、匷粟、消炎、利尿、血圧降
䞋、抗糖尿甚の薬剀ずしお甚いられおきたこずは
広く知られるずころである。近時、これらの薬効
が、チペりセンニンゞン䞭のサポニン成分による
のではないかずの研究が進められおいる。しかし
ながらこのサポニン成分が抗腫瘍䜜甚、制ガン䜜
甚を有するこずは党く知られおいない。 Medicinal ginseng, especially Araliaceae
Panax ginseng (Panax ginseng, C.A. Meyer, Panax ginseng C.
A. MEYER), also known as Panax ginseng, is widely known to have been used as a tonic, tonic, anti-inflammatory, diuretic, blood pressure lowering, and anti-diabetic drug since ancient times. Recently, research has been underway to investigate whether these medicinal effects may be due to the saponin components in Panax ginseng. However, it is completely unknown that this saponin component has antitumor and anticancer effects.

この発明は、薬甚ニンゞン䞭のサポニン成分が
意倖にも抗腫瘍䜜甚ガンを含むを有するずい
う新しい知芋に基づいおなされたものである。 This invention was made based on the new finding that saponin components in medicinal ginseng unexpectedly have antitumor effects (including cancer).

この発明の䞀぀の芳点によれば、薬甚ニンゞン
のサポニン成分を有効成分ずしお含有する抗腫瘍
剀を提䟛するものである。 According to one aspect of the present invention, there is provided an antitumor agent containing saponin components of medicinal ginseng as an active ingredient.

この発明におけるサポニン成分を含有するニン
ゞンずしおは、オタネニンゞンが最も奜たしいも
のである。その他、これず類瞁怍物であるトチバ
ニンゞンパナツクス・ダポニカス、シヌ・゚
ヌ・メむダヌ、Panax japonicus C.A.
MEYER、アメリカニンゞンパナツクス・キ
ンキナホリりム、リンネ、Panax quinquefolium
LINNE、䞉䞃ニンゞンパナツクス・プ゜む
ド・ギンれング、ワヌリツヒPanax pseudo−
ginseng WALICHたたはパナツクス・ノトギン
れング・バヌキル、Panax notoginseng
BURKILLが挙げられる。 As the carrot containing the saponin component in this invention, Panax ginseng is the most preferred. Other related plants include Panax japonicus (Panax japonicus, Panax japonicus CA, Panax japonicus CA)
MEYER), American ginseng (Panax quinquefolium, Linnaeus, Panax quinquefolium)
LINNE), Panax pseudo-ginseng (Panax pseudo−)
ginseng WALICH or Panax notoginseng
BURKILL).

この発明のサポニン成分は、䞊蚘のごずきニン
ゞンを原料ずしお、その生薬から抜出分離、粟補
するかたたは䞊蚘のごずきニンゞンの根茎切片を
組織培逊し、次いで抜出分離、粟補するこずによ
぀お埗るこずができる。なおこの発明で単に“サ
ポニン成分”ず称する堎合は、これらの方法によ
぀お埗られる実質的にサポニン類のみからなる混
合物をいう。 The saponin component of the present invention can be obtained by extracting, separating, and purifying the herbal medicine using the above carrot as a raw material, or by tissue culturing the above-mentioned carrot rhizome section, and then extracting, separating, and purifying it. can. In the present invention, the term "saponin component" refers to a mixture substantially consisting only of saponins obtained by these methods.

ニンゞンの生薬からサポニン成分を埗る方法ず
しおは䟋えば次のような方法で埗るこずができ
る。すなわち、原料ずなるニンゞンを脱脂せず
に、あるいは通垞の脂溶性有機溶媒を甚いお脱脂
埌、氎たたは䜎玚脂肪族アルコヌル類あるいは含
氎䜎玚脂肪族アルコヌルを甚いおその有効成分を
抜出し、抜出液を蒞発濃瞮しお抜出゚キスずす
る。これを−ブタノヌルに溶解し、該溶解液に
氎を加えお振盪した埌静眮しお䞍溶物質を陀去
し、−ブタノヌル局を蒞発也固する。残留物を
䜎玚脂肪族アルコヌルに溶解埌、゚ヌテル䞭に撹
拌泚入しお埗られた析出物を取すればよい特
公昭48−5016号参照。 Saponin components can be obtained from the herbal medicine of carrots, for example, by the following method. That is, the carrots used as raw materials are degreased without being defatted, or after being defatted using a normal fat-soluble organic solvent, and the active ingredients are extracted using water, lower aliphatic alcohols, or hydrous lower aliphatic alcohols, and the extract is made into an extract. is evaporated and concentrated to obtain an extract. This is dissolved in n-butanol, water is added to the solution, shaken and left to stand to remove insoluble substances, and the n-butanol layer is evaporated to dryness. After dissolving the residue in a lower aliphatic alcohol, the resulting precipitate may be collected by stirring and pouring into ether (see Japanese Patent Publication No. 5016/1983).

このようにしお埗られた抜出物は実質的にサポ
ニン成分のみを含むものであ぀お、そのたたこの
発明の有効成分ずしお䜿甚できる。 The extract thus obtained contains substantially only saponin components and can be used as is as an active ingredient in the present invention.

この発明によるサポニン成分は、原料ずする薬
甚ニンゞンの皮類や裁培幎数によ぀お構成される
成分の皮類・量に若干の差があるが、埌述するご
ずき匏、およびの化合物を含有
するものである。サポニン成分の党䜓の性状ずし
おは、いずれも黄癜色〜か぀色の粉末で苊味を有
し、氎、メタノヌル、垌メタノヌルに易溶、゚タ
ノヌルに可溶、クロロホルム、゚ヌテル、四塩化
炭玠に䞍溶である。たた酞加氎分解によ぀お必ず
氎可溶郚からブドり糖が埗られ、氎䞍溶物からパ
ナキサダむオヌルC30H52O3、mp205℃およ
びたたは、パナキサトリオヌルC30H52O4、
mp238〜239℃が埗られる。 The saponin component according to the present invention has some differences in the type and amount of the component depending on the type of medicinal ginseng used as raw material and the number of years of culturing, but the saponin component according to the following formulas (), () and () are used. It contains a compound. The overall properties of the saponin components are that they are all yellowish-white to colored powders with a bitter taste, easily soluble in water, methanol, and diluted methanol, soluble in ethanol, and insoluble in chloroform, ether, and carbon tetrachloride. . In addition, acid hydrolysis always yields glucose from the water-soluble portion, and panaxadiol (C 30 H 52 O 3 , mp205°C) and/or panaxatriol (C 30 H 52 O Four ,
mp238-239℃) is obtained.

たた組織培逊によりサポニンを埗るには䟋えば
ノツプKnop培逊液硫酞カルシりム1000
mg、硝酞カリりム250mg、硫酞マグネシ
りム250mg、第燐酞カリりム250mg
500ml、ヘラヌd′Hellerのミネラル液ml
、ブドり糖、ビタミンB10-6、ビオチン
10-6、カむネチン10-6、寒倩よりなる培
地にニンゞンの根の組織片を入れ、26℃に保぀お
培逊増殖せしめ、ニンゞンカルスを埗る。次いで
このカルスを同䞀の培地を甚いお倧量増殖させ、
このものを前蚘した抜出法ず同様にしお抜出粟補
するこずによ぀おサポニン成分を埗るこずができ
る。 In addition, to obtain saponin by tissue culture, for example, Knop culture solution (calcium sulfate 1000
mg/, potassium nitrate 250mg/, magnesium sulfate 250mg/, monobasic potassium phosphate 250mg/)
500ml, d'Heller mineral liquid 1ml/
, glucose 5%, vitamin B10 -6 g, biotin
A piece of carrot root tissue is placed in a medium containing 10 -6 g of kinetin, 10 -6 g of kinetin, and 1% agar, and cultured and grown at 26°C to obtain carrot callus. Next, this callus was grown in large quantities using the same medium,
A saponin component can be obtained by extracting and purifying this product in the same manner as the extraction method described above.

たた、この発明におけるサポニン成分䞭には次
の匏たたはで衚わされるギンれノサ
むドginsenoside類の少なくずも䞀皮類が含
たれ、必芁により匏で衚わされるβ−−
グルコピラノシルオレアネヌト−(3)−β−−グ
ルコピラノシル→−β−−グルクロノ
ピラノシドがさらに含たれおいる。 In addition, the saponin component in this invention contains at least one type of ginsenoside represented by the following formula () or (), and if necessary, β-D-
Further included is glucopyranosyloleanate-(3)-β-D-glucopyranosyl(1→2)-β-D-glucuronopyranoside.

匏 匏䞭、R1はβ−−グルコピラノシル→
−β−−グルコピラノシル基を瀺し、R2は
β−−グルコピラノシル→−β−−
グルコピラノシル基、α−−アラビノピラノシ
ル→−β−−グルコピラノシル基、β
−−キシロピラノシル−−β−−グ
ルコピラノシル基、α−−アラビノフラノシル
→−β−−グルコピラノシル基たたは−
β−−グルコピラノシル基を瀺す。 formula(): In the formula, R 1 is β-D-glucopyranosyl (1→
2) -β-D-glucopyranosyl group, R 2 is β-D-glucopyranosyl (1→6)-β-D-
Glucopyranosyl group, α-L-arabinopyranosyl (1→6)-β-D-glucopyranosyl group, β
-D-xylopyranosyl (1-6)-β-D-glucopyranosyl group, α-L-arabinofuranosyl (1→6)-β-D-glucopyranosyl group, or -
Indicates a β-D-glucopyranosyl group.

匏 匏䞭、R3はα−−ラムノピラノシル→
−β−−グルコピラノシル基、β−−グ
ルコピラノシル−−β−−グルコピラ
ノシル基、β−−グルコピラノシル基たたはα
−−ラムノピラノシル→−β−−グ
ルコピラノシル基を瀺し、R4は氎玠原子たたは
β−−グルコピラノシル基を瀺す。 formula(): In the formula, R 3 is α-L-rhamnopyranosyl (1→
2) -β-D-glucopyranosyl group, β-D-glucopyranosyl (1-2)-β-D-glucopyranosyl group, β-D-glucopyranosyl group or α
-L-rhamnopyranosyl (1→2)-β-D-glucopyranosyl group, and R 4 represents a hydrogen atom or a β-D-glucopyranosyl group.

匏 匏䞭、R5はβ−−グルコピラノシル基を瀺
し、R6はβ−−グルコピラノシル−−
β−−グルクロノピラノシル基を瀺す。 formula(): In the formula, R 5 represents β-D-glucopyranosyl group, and R 6 represents β-D-glucopyranosyl (1-2)-
Indicates a β-D-glucuronopyranosyl group.

匏および匏で衚わされるサポニン
はトリテルペンのダンマラン系配糖䜓に属するサ
ポニンである。これら匏および匏の
サポニンは、珟圚のずころ薬甚ニンゞンのみに特
異的に含たれるこずが刀明しおいるもので、この
発明による抗腫瘍剀ずしおの薬理掻性の䞻䜓を構
成するものず考えられる。 The saponins represented by formulas () and () belong to the dammarane glycosides of triterpenes. These saponins of formula () and formula () are currently known to be specifically contained only in medicinal ginseng, and are considered to constitute the main body of pharmacological activity as an antitumor agent according to the present invention. Conceivable.

匏で衚わされる化合物の個々の具䜓名ず
しおは、20S−プロトパナキサゞオヌル−−
〔−β−−グルコピラノシル−−β−
−グルコピラノシド〕−20−〔−β−−グル
コピラノシル→−β−−グルコピラノ
シド〕ギンれノサむドRb1、20S−プロトパナ
キサゞオヌル−−〔−β−−グルコピラノ
シル→−β−−グルコピラノシド〕−20
−〔−α−−アラビノピラノシル→−
β−−グルコピラノシド〕ギンれノサむド
Rb2、20S−プロトパナキサゞオヌル−−〔
−β−−グルコピラノシル→−β−
−グルコピラノシド〕−20−〔−α−−アラビ
ノフラノシル→−β−−グルコピラノ
シド〕ギンれノサむドRc、20S−プロトパナキ
サゞオヌル−−〔−β−−グルコピラノシ
ル→−β−−グルコピラノシド〕−20−
〔−β−−キシロピラノシル→−β−
−グルコピラノシド〕ギンれノサむドRb3お
よび20S−プロトパナキサゞオヌル−−〔−
β−−グルコピラノシル→−β−−
グルコピラノシド〕−20−〔−β−−グルコピ
ラノシド〕ギンれノサむドRbが挙げられる。 Specific names of the compounds represented by formula () include 20S-protopanaxadiol-3-
[0-β-D-glucopyranosyl(1-2)-β-
D-glucopyranoside]-20-[0-β-D-glucopyranosyl (1→6)-β-D-glucopyranoside] (ginzenoside Rb 1 ), 20S-protopanaxadiol-3-[0-β-D-glucopyranosyl (1→2)-β-D-glucopyranoside]-20
-[0-α-L-arabinopyranosyl (1→6)-
β-D-glucopyranoside] (ginzenoside
Rb 2 ), 20S-protopanaxadiol-3-[0
-β-D-glucopyranosyl (1→2)-β-D
-glucopyranoside]-20-[0-α-L-arabinofuranosyl (1→6)-β-D-glucopyranoside] (ginzenoside Rc), 20S-protopanaxadiol-3-[0-β-D- Glucopyranosyl (1→2)-β-D-glucopyranoside]-20-
[0-β-D-xylopyranosyl (1→6)-β-
D-glucopyranoside] (ginsenoside Rb 3 ) and 20S-protopanaxadiol-3-[0-
β-D-glucopyranosyl (1→2)-β-D-
glucopyranoside]-20-[0-β-D-glucopyranoside] (ginsenoside Rb).

匏で衚わされる化合物の具䜓名ずしは
20S−プロトパナキサトリオヌル−−〔−α
−−ラムノピラノシル→−β−−グ
ルコピラノシド〕−20−−β−−グルコピラ
ノシドギンれノサむドRe、20S−プロトパナ
キサトリオヌル−−−β−−グルコピラノ
シル→−β−−グルコピラノシドギ
ンれノサむドRf、20S−プロトパナキサトリオ
ヌル−−20−ゞ−−β−−グルコピラノ
シドギンれノサむドRg1、20S−プロトパナキ
サトリオヌル−−−α−−ラムノピラノシ
ル→−β−−グルコピラノシドギン
れノサむドRg2および20S−プロトパナキサトリ
オヌル−−〔−β−−グルコピラノシル
→−β−−グルコピラノシド〕−20−
−β−−グルコピラノシドギンれノサむド20
−グルコ−Rfが挙げられる。 What is the specific name of the compound represented by formula ()?
20S-protopanaxatriol-6-[0-α
-L-rhamnopyranosyl (1→2)-β-D-glucopyranoside] -20-0-β-D-glucopyranoside (ginzenoside Re), 20S-protopanaxatriol-6-0-β-D-glucopyranoside (1→ 2) -β-D-glucopyranoside (ginzenoside Rf), 20S-protopanaxatriol-6-,20-di-0-β-D-glucopyranoside (ginzenoside Rg 1 ), 20S-protopanaxatriol-6-0 -α-L-rhamnopyranosyl (1→2)-β-D-glucopyranoside (ginzenoside Rg 2 ) and 20S-protopanaxatriol-6-[0-β-D-glucopyranosyl (1→2)-β-D- Glucopyranoside〕-20-0
-β-D-glucopyranoside (ginzenoside 20
-Gluco-Rf).

なおオタネニンゞン䞭には前述した匏
およびの構造匏を有するサポニンの
他に、匏の骚栌を有するず考えられるギン
れノサむドRaず称せられおいる構造未定のサポ
ニンおよび匏の骚栌を有するず考えられる
ギンれノサむドRhず称せられおいる構造未定の
サポニンも含たれおおり、これらの物質もこの発
明のサポニン成分に含たれるChem Pharm
Bull.22(2)421〜4281974および薬孊雑誌
94(2)252〜2601974参照。 In addition, Panax ginseng contains the aforementioned formula (),
In addition to saponins having the structural formulas () and (), saponins of undetermined structure called ginsenoside Ra, which is thought to have the skeleton of formula (), and ginsenoside Rh, which is thought to have the skeleton of formula (). These substances are also included in the saponin component of this invention (Chem Pharm,
Bull., 22(2) , 421-428 (1974) and Pharmaceutical Journal
94(2) , 252-260 (1974)).

前述した個々の化合物は、前述のごずくしお埗
られたサポニン成分をたずえばクロロホルムメ
タノヌル氎系あるいは−ブタノヌル酢酞
氎系の展開溶剀を甚いたシリカゲルカラムクロマ
トグラフむヌ、高速液䜓クロマトグラフむヌなど
により各構成サポニンに分離、粟補するこずによ
぀お埗るこずができる。しかしながら、経枈的芋
地から個々の構成サポニンに分離しお䜿甚するよ
り、混合物ずしお甚いた方が奜たしい。 The above-mentioned individual compounds can be prepared by mixing the saponin component obtained as described above with, for example, a chloroform/methanol/water system or n-butanol/acetic acid/
It can be obtained by separating and purifying each constituent saponin by silica gel column chromatography, high performance liquid chromatography, etc. using an aqueous developing solvent. However, from an economical point of view, it is preferable to use the saponins as a mixture rather than separating them into the individual constituent saponins.

サポニン成分はヒトに察する抗腫瘍剀ずしお極
めお有甚なものであり、適甚範囲が広く、か぀副
䜜甚がほずんど認められない。 Saponin components are extremely useful as antitumor agents for humans, have a wide range of application, and have almost no side effects.

この発明における抗腫瘍剀の投䞎量は病状に応
じお異なるが、成人に察する内服の堎合、サポニ
ン成分ずしお日あたり50〜1000mg、奜たしくは
100〜300mgを〜回に分けお投䞎するこずによ
぀お効力を発揮するこずができる。たた倖甚の堎
合は〜10芪氎軟膏たたは疎氎軟膏の圢で甚い
る。適甚範囲ずしおは胃癌、盎腞癌、乳癌、子宮
癌、口腔癌、食道癌、胆癌、胆管癌、胆道癌、膵
臓癌、腎腫瘍、前立腺癌、亜性甲状線腫瘍、肺
癌、脳腫瘍、肝臓癌、舌癌、胞腺腫、皮膚癌、肉
腫などガンを含めたほずんどあらゆる腫瘍に察し
お有効である。 The dosage of the antitumor agent in this invention varies depending on the disease state, but when administered internally to adults, the saponin component is 50 to 1000 mg per day, preferably
It can be effective by administering 100 to 300 mg in two to three doses. For external use, it is used in the form of a 1-10% hydrophilic ointment or hydrophobic ointment. Applicable ranges include stomach cancer, rectal cancer, breast cancer, uterine cancer, oral cavity cancer, esophageal cancer, bile cancer, bile duct cancer, biliary tract cancer, pancreatic cancer, kidney tumor, prostate cancer, subthyroid tumor, lung cancer, brain tumor, and liver cancer. It is effective against almost all tumors including cancer, such as tongue cancer, thymoma, skin cancer, and sarcoma.

この発明による抗腫瘍剀は、この発明のサポニ
ン成分単䜓、たたはサポニン成分ず固䜓もしくは
液䜓に賊圢剀ずからなるものである。そしお投䞎
法ならびに投䞎の剀型ずしおは、通垞、散剀、錠
剀、乳剀、カプセル剀、茶剀、顆粒剀、液剀酒
粟剀、チンキ剀、流゚キス剀、シロツプ剀などを
含むなどの内服の圢がある。たた泚射剀、点滎
剀の圢で䜓内泚入するか、あるいは軟膏剀、液
剀、倖甚散剀、シツプ剀、坐薬、噎霧剀、滋逊浣
腞剀、乳剀などの圢で倖甚であ぀おもよい。ここ
に䜿甚される固䜓たたは液䜓の賊圢剀ずしおは、
圓該分野で公知のものが䜿甚される。ただ前述し
たような回の投䞎量に必芁なこの発明の化合物
を含むように補剀化するのが望たしい。 The antitumor agent according to the present invention consists of the saponin component of the present invention alone, or the saponin component and a solid or liquid excipient. The administration method and dosage form are usually powders, tablets, emulsions, capsules, teas, granules, liquids (including spirits, tinctures, liquid extracts, syrups, etc.) and other oral medications. It has a shape. It may also be injected into the body in the form of injections or drops, or externally administered in the form of ointments, liquids, external powders, syrups, suppositories, sprays, nourishing enemas, emulsions, and the like. Solid or liquid excipients used here include:
Those known in the art are used. It may be desirable to formulate the compound to contain the required amount of the compound for a single dose, such as those described above.

いく぀かの具䜓䟋を挙げるず散剀、その他の内
服甚粉末剀における賊圢剀ずしおは、乳糖、柱
粉、デキストリン、リン酞カルシりム、炭酞カル
シりム、合成および倩然ケむ酞アルミニりム、酞
化マグネシりム、也燥氎酞化アルミニりム、ステ
アリン酞マグネシりム、重炭酞ナトリりム、也燥
酵母などが挙げられ、倖甚散剀の堎合は酞化亜
鉛、タルク、柱粉、カオリン、ホり酞末、ステア
リン酞亜鉛、ステアリン酞マグネシりム、炭酞マ
グネシりム、沈降炭酞カルシりム、次没食子酞ビ
スマス、硫酞アルミニりムカリりム末などが挙げ
られる。液剀における賊圢剀ずしおは氎、グリセ
リン、プロピレングリコヌル、単シロツプ、゚タ
ノヌル、脂肪油、゚チレングリコヌル、ポリ゚チ
レングリコヌル、゜ルビトヌルなどが挙げられ
る。さらに軟膏剀の堎合には脂肪、脂肪油、ラノ
リン、ワセリン、グリセリン、ミツロり、モクロ
り、パラフィン、流動パラフむン、暹脂、高玚ア
ルコヌル、プラスチツクス、グリコヌル類、氎、
界面掻性剀などを組み合わせお぀く぀た疎氎性基
剀あるいは芪氎性基剀乳剀性基剀、氎溶性基材
および懞濁剀性基剀を含むが賊圢剀ずしお䜿甚
される。 Excipients in powders and other powders for internal use include lactose, starch, dextrin, calcium phosphate, calcium carbonate, synthetic and natural aluminum silicates, magnesium oxide, dry aluminum hydroxide, stearin, to name a few specific examples. Magnesium acid, sodium bicarbonate, dried yeast, etc., and for external powders, zinc oxide, talc, starch, kaolin, boric acid powder, zinc stearate, magnesium stearate, magnesium carbonate, precipitated calcium carbonate, hypogallic acid. Examples include bismuth and potassium aluminum sulfate powder. Excipients for liquid preparations include water, glycerin, propylene glycol, simple syrup, ethanol, fatty oils, ethylene glycol, polyethylene glycol, sorbitol, and the like. Furthermore, in the case of ointments, fats, fatty oils, lanolin, petrolatum, glycerin, beeswax, Japanese wax, paraffin, liquid paraffin, resins, higher alcohols, plastics, glycols, water,
Hydrophobic bases or hydrophilic bases (including emulsion bases, water-soluble bases, and suspension bases) prepared by combining surfactants and the like are used as excipients.

䞀方、この発明によるサポニン成分の毒性はマ
りスに腹腔内投䞎した堎合、LD50は637mgKgで
著しく毒性が少なく、しかも溶血䜜甚は認められ
なか぀た。 On the other hand, when the saponin component according to the present invention was administered intraperitoneally to mice, the toxicity was extremely low with an LD 50 of 637 mg/Kg, and no hemolytic effect was observed.

次にこの発明による補造䟋および治隓䟋を述
べ。 Next, manufacturing examples and clinical trial examples according to this invention will be described.

補造䟋 オタネニンゞン幎生の也燥根10Kgを现切
し100づ぀のメタノヌルで時間づ぀回加熱
抜出し、抜出液を合しお10たで濃瞮した。濃瞮
液を100の゚ヌテル䞭に撹拌しながら陀々に少
量ず぀泚入し、析出物を分取した埌、゚ヌテル臭
のなくなるたで也燥した。生成物を10の氎飜和
−ブタノヌルを甚いお玄時間ず぀回蒞気济
䞊で撹拌しながら溶解させた。埗られた溶液を
の−ブタノヌル飜和氎を甚いお回氎掗しお
借雑する糖類や色玠を氎に移行させお取り陀き、
分離した氎飜和−ブタノヌル局を80℃以䞋で枛
圧蒞留、也固した。残留物をのメタノヌルに
溶かし、60の゚ヌテル䞭に撹拌䞋に泚入した。
日静眮埌、析出物を別し、60℃以䞋で枛圧也
燥しおニンゞンサポニン260を埗た。Production example 10 kg of dried roots of Panax ginseng (4th grade) were cut into small pieces, heated and extracted three times for 3 hours each with 100 methanol, and the extracts were combined and concentrated to 10. The concentrated solution was gradually poured into 100% ether in small portions with stirring, and the precipitate was separated and dried until the ether odor disappeared. The product was dissolved with stirring on a steam bath three times for about 1 hour each with 10 parts of water-saturated n-butanol. The obtained solution is 3
Rinse three times with n-butanol saturated water to remove contaminating sugars and pigments by transferring them to the water.
The separated water-saturated n-butanol layer was distilled under reduced pressure at 80° C. or lower to dryness. The residue was dissolved in 3 parts of methanol and poured into 6 parts of ether with stirring.
After standing for one day, the precipitate was separated and dried under reduced pressure at 60° C. or lower to obtain 260 g of carrot saponin.

このようにしお補造したニンゞンサポニンを䜿
甚しお次の治隓䟋を埗た。 The following clinical trial examples were obtained using the carrot saponin thus produced.

治隓䟋  62才男子、病理組織孊的に胃癌の蚺断を受けた
が、胃摘陀術を拒吊したため手術せず、日圓り
200mgのニンゞンサポニンを回に分けお空腹
時、投䞎した。投薬開始時、䜓重36Kg、赀血球数
415䞇、癜血球数6600、顔面蒌癜で心窩郚痛激し
く觊蚺にお腫瘀を認めた。投薬ケ月后心窩郚痛
は消倱し、䜓重41Kgず増加した。顔色も良くなり
胃透芖にお小さいニツシ゚を認めるのみずなり朰
瘍ず蚺断された。さらにケ月投䞎后には、疲劎
感が党くなくなり、食欲も増加し䜓重42.5Kgずな
る。この時内芖鏡怜査及び生怜では朰瘍の瘢痕を
認めるのみずなり、瘢痕郚生怜でも悪性所芋は党
く芋られなか぀た。人参サポニン投䞎后、自他芚
症状及び怜査所芋においお、人参サポニンによる
急性、亜急性の毒性を暗瀺するものは党くなく、
ケ月の投䞎にお極めお著効を瀺した䟋である。Clinical trial case 1: A 62-year-old male was histopathologically diagnosed with gastric cancer, but he refused gastrectomy, so he did not undergo surgery and
200 mg of carrot saponin was administered in two doses on an empty stomach. At the start of medication, weight 36 kg, red blood cell count
4,150,000, white blood cell count 6,600, facial pallor, severe epigastric pain, and palpation revealed a mass. One month after starting the medication, the epigastric pain disappeared and the patient's weight increased to 41 kg. The patient's complexion improved, and gastric fluoroscopy revealed only a small tumor, which was diagnosed as an ulcer. Furthermore, after one month of administration, the patient's feeling of fatigue disappeared completely, his appetite increased, and he weighed 42.5 kg. At this time, endoscopy and biopsy revealed only an ulcer scar, and a biopsy of the scar area showed no malignant findings. After administration of ginseng saponin, there were no subjective symptoms or test findings that suggested acute or subacute toxicity due to ginseng saponin.
This is an example of an extremely effective effect after two months of administration.

治隓䟋  52才女子、癌性腹膜炎を䌎぀た胃癌の患者。癌
は胃党䜓に広たり、腹膜、膵臓、シナニツツラ及
び小腞ぞ浞最しおおり、切陀術が䞍可胜な症䟋で
ある。自芚症状ずしお腹痛及び食后嘔吐感を蚎え
おおり、䟿秘がちで排䟿前には特に腹痛が匷か぀
た。顔面は蒌癜で極めお衰匱の激しい症䟋であ぀
たのでニンゞンサポニン日圓り、200mg回に
分けお空腹時、投䞎した。投䞎后週でやや腹痛
が緩和し始め、半流動食ではあるが摂取量の増加
が芋られた。投䞎埌週で䜓重はKg増加し腹痛
は時々感ずる皋床にたで軜快したが、排䟿前の痛
みは軜快せず又食后の嘔吐感にも䜙り著倉は芋ら
れなか぀た。Trial case 2: A 52-year-old female patient with gastric cancer accompanied by cancerous peritonitis. The cancer has spread throughout the stomach and has invaded the peritoneum, pancreas, tunica, and small intestine, making resection impossible. The patient complained of abdominal pain and a feeling of vomiting after eating, and was prone to constipation, with abdominal pain especially severe before defecation. Since the patient's face was pale and he was extremely weak, we administered 200 mg of carrot saponin per day in two divided doses on an empty stomach. Two weeks after administration, abdominal pain began to ease slightly, and an increase in intake was observed, albeit on a semi-liquid diet. Five weeks after administration, the body weight increased by 1 kg, and the abdominal pain was relieved to the extent that it was sometimes felt, but the pain before defecation was not alleviated, and no significant change was observed in the feeling of vomiting after eating.

治隓䟋  44才女子、乳癌で第腰怎ぞの転移が認めら
れ、腰痛が激しく、歩行困難を蚎えおいた。ニン
ゞンサポニン療法ずしお、ニンゞンサポニン日
圓り100mgを回に分けお空腹時、投䞎した。投
䞎開始時、赀血球数380䞇、癜血球数6000、赀血
球沈降速床時間倀20、時間倀46であ぀た。投
薬週后に腰痛がやや軜快し、顔色も良くなり始
め、週后には痛みが完党に消倱し、歩行可胜ず
な぀た。この時赀血球数400䞇、癜血球数6400、
赀血球沈降速床時間倀16、時間倀36であ぀
た。たた骚転移郚の線怜査所芋で、転移の進行
は党く芳察されなか぀た。ニンゞンサポニン投䞎
開始以后、食欲の増進を認めたが䜓重には倉化が
芋られなか぀た。たた週間の投䞎期間䞭、ニン
ゞンサポニンによる副䜜甚を暗瀺する自他芚症状
は党く認められなか぀た。Trial case 3 A 44-year-old female was diagnosed with breast cancer that had metastasized to the first lumbar vertebrae, and complained of severe lower back pain and difficulty walking. As carrot saponin therapy, 100 mg of carrot saponin per day was administered in two divided doses on an empty stomach. At the start of administration, the red blood cell count was 3.8 million, the white blood cell count was 6000, and the erythrocyte sedimentation rate was 20 for 1 hour and 46 for 2 hours. One week after taking the medication, the patient's lower back pain was slightly relieved and her complexion began to improve, and after five weeks, the pain completely disappeared and she was able to walk again. At this time, the number of red blood cells was 4 million, the number of white blood cells was 6400,
The erythrocyte sedimentation rate was 16 at 1 hour and 36 at 2 hours. Furthermore, X-ray examination findings of the bone metastasis site showed no progression of metastasis at all. After the administration of carrot saponin was started, an increase in appetite was observed, but no change in body weight was observed. Furthermore, during the 5-week administration period, no subjective or objective symptoms suggesting side effects caused by carrot saponin were observed.

治隓䟋  62才男子、腹腔内転移を䌎なう盎腞癌の患者。
臍郚に腫瘀を觊知し、自芚症状ずしお腰痛及び排
䟿時肛門郚の痛みを蚎えおいた。赀血球数415
䞇、癜血球数7300、線怜査で肺ぞの転移は認め
られなか぀た。治隓䟋ず同様にニンゞンサ
ポニン日あたり100mgを回に分けお空腹時に
投䞎した。投䞎週后には、腰痛が緩和し始め、
食欲も増加し始めた。しかし排䟿時の肛門郚の痛
みは軜快しなか぀た。この時、赀血球数439䞇、
癜血球数8900でリンパ球の増加が芳察された。こ
の時から投䞎量を日圓り200mg回に増量
しされに週間の連続投䞎を行な぀た結果、臍郚
の腫瘀は、わずかに觊知される皋床にたで瞮少し
腰痛は完党に消倱した。Trial case 4: A 62-year-old male patient with rectal cancer with intra-abdominal metastasis.
A mass was palpated in the umbilical region, and the patient complained of lower back pain and pain in the anal region during defecation. Red blood cell count 415
The patient's white blood cell count was 7,300, and X-rays showed no metastasis to the lungs. As in Trial Examples 1 and 3, 100 mg of carrot saponin per day was administered in two divided doses on an empty stomach. Four weeks after administration, lower back pain began to ease,
My appetite also started to increase. However, the pain in the anal region during defecation did not subside. At this time, the number of red blood cells was 4.39 million,
White blood cell count was 8900 and an increase in lymphocytes was observed. From this time on, the dose was increased to 200mg per day (twice) and continuous administration was carried out for 4 weeks.As a result, the mass in the umbilicus shrank to the extent that it could be slightly palpated, and the lower back pain completely disappeared. Disappeared.

Claims (1)

【特蚱請求の範囲】  薬甚ニンゞンのサポニン成分を有効成分ずし
お含有する抗腫瘍剀。  薬甚ニンゞンがオタネニンゞンパナツク
ス・ギンれング、シヌ・゚ヌ・メむダヌ、トチ
バニンゞンパナツクス・ダポニカス、シヌ・゚
ヌ・メむダヌ、アメリカニンゞンパナツク
ス・キンキナホリりム、リンネ、䞉䞃ニンゞン
パナツクス・プ゜むド・ギンれング、ワヌリツ
ヒたたはパナツクス・ノトギンれング、バヌキ
ルである特蚱請求の範囲第項蚘茉の抗腫瘍
剀。  薬甚ニンゞンがオタネニンゞンである特蚱請
求の範囲第項蚘茉の抗腫瘍剀。  薬甚ニンゞンのサポニン成分が特蚱請求の範
囲第項たたは第項蚘茉のニンゞンよりの抜出
物である特蚱請求の範囲第項たたは第項蚘茉
の抗腫瘍剀。[Scope of Claims] 1. An antitumor agent containing saponin components of medicinal ginseng as an active ingredient. 2. Medicinal carrots include Panax ginseng (Panatucus ginseng, C.A. Meyer), Horse chestnut ginseng (Panatchus japonicus, C.A. Meyer), American ginseng (Panatucus cinquefolium, Linnaeus), Panax ginseng (Panatucus pseudoginseng, C.A. Meyer), The antitumor agent according to claim 1, which is Panax or Panax notoginseng, Burkil). 3. The antitumor agent according to claim 1, wherein the medicinal ginseng is Panax ginseng. 4. The antitumor agent according to claim 2 or 3, wherein the saponin component of medicinal ginseng is an extract from ginseng according to claim 2 or 3.
JP549177A 1977-01-20 1977-01-20 Antitumor agent Granted JPS5391109A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP549177A JPS5391109A (en) 1977-01-20 1977-01-20 Antitumor agent

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP549177A JPS5391109A (en) 1977-01-20 1977-01-20 Antitumor agent

Publications (2)

Publication Number Publication Date
JPS5391109A JPS5391109A (en) 1978-08-10
JPS628415B2 true JPS628415B2 (en) 1987-02-23

Family

ID=11612705

Family Applications (1)

Application Number Title Priority Date Filing Date
JP549177A Granted JPS5391109A (en) 1977-01-20 1977-01-20 Antitumor agent

Country Status (1)

Country Link
JP (1) JPS5391109A (en)

Families Citing this family (7)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPS6147411A (en) * 1984-08-15 1986-03-07 Dai Ichi Seiyaku Co Ltd Promoter for hair growth
KR940000234B1 (en) * 1989-09-04 1994-01-12 김송배 Novel pharmaceutical composition having an antitumor activity and a process for preparation thereof
TWI222357B (en) 2000-01-11 2004-10-21 Medical & Pharm Ind Tech & Dev Anti-ulcer pharmaceutical composition and the preparation and use thereof
CN104069344A (en) * 2014-06-10 2014-10-01 于䞜旭 Traditional Chinese medicine composition for treating cancer and preparation and preparation method thereof
CN108186899A (en) * 2018-03-07 2018-06-22 韊雄悬 A kind of Chinese medicine composition for treating tumour and preparation method and application
CN109498666A (en) * 2019-01-25 2019-03-22 江苏农牧科技职䞚孊院 A kind of impurity-removing method of response phase method optimization notoginseng haulm saponin extract solution
CN109731022A (en) * 2019-03-23 2019-05-10 河北厚執汉方医疗噚械股仜有限公叞 A kind of the health-preserving granula foot patch and its processing method of supplementing qi and nourishing yin

Also Published As

Publication number Publication date
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