TW201904569A - 膀胱過動的預防劑或治療劑 - Google Patents
膀胱過動的預防劑或治療劑Info
- Publication number
- TW201904569A TW201904569A TW107118143A TW107118143A TW201904569A TW 201904569 A TW201904569 A TW 201904569A TW 107118143 A TW107118143 A TW 107118143A TW 107118143 A TW107118143 A TW 107118143A TW 201904569 A TW201904569 A TW 201904569A
- Authority
- TW
- Taiwan
- Prior art keywords
- group
- bladder
- hydrogen atom
- ala
- pharmaceutical composition
- Prior art date
Links
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- HCWCAKKEBCNQJP-UHFFFAOYSA-N magnesium orthosilicate Chemical compound [Mg+2].[Mg+2].[O-][Si]([O-])([O-])[O-] HCWCAKKEBCNQJP-UHFFFAOYSA-N 0.000 description 1
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- PLSARIKBYIPYPF-UHFFFAOYSA-H trimagnesium dicitrate Chemical compound [Mg+2].[Mg+2].[Mg+2].[O-]C(=O)CC(O)(CC([O-])=O)C([O-])=O.[O-]C(=O)CC(O)(CC([O-])=O)C([O-])=O PLSARIKBYIPYPF-UHFFFAOYSA-H 0.000 description 1
- 125000002221 trityl group Chemical group [H]C1=C([H])C([H])=C([H])C([H])=C1C([*])(C1=C(C(=C(C(=C1[H])[H])[H])[H])[H])C1=C([H])C([H])=C([H])C([H])=C1[H] 0.000 description 1
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- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/185—Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
- A61K31/19—Carboxylic acids, e.g. valproic acid
- A61K31/195—Carboxylic acids, e.g. valproic acid having an amino group
- A61K31/197—Carboxylic acids, e.g. valproic acid having an amino group the amino and the carboxyl groups being attached to the same acyclic carbon chain, e.g. gamma-aminobutyric acid [GABA], beta-alanine, epsilon-aminocaproic acid or pantothenic acid
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/28—Compounds containing heavy metals
- A61K31/295—Iron group metal compounds
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P13/00—Drugs for disorders of the urinary system
- A61P13/10—Drugs for disorders of the urinary system of the bladder
Landscapes
- Health & Medical Sciences (AREA)
- Veterinary Medicine (AREA)
- Chemical & Material Sciences (AREA)
- Medicinal Chemistry (AREA)
- Pharmacology & Pharmacy (AREA)
- Life Sciences & Earth Sciences (AREA)
- Animal Behavior & Ethology (AREA)
- General Health & Medical Sciences (AREA)
- Public Health (AREA)
- Epidemiology (AREA)
- Engineering & Computer Science (AREA)
- Bioinformatics & Cheminformatics (AREA)
- Urology & Nephrology (AREA)
- Chemical Kinetics & Catalysis (AREA)
- General Chemical & Material Sciences (AREA)
- Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
- Organic Chemistry (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
Abstract
既存之膀胱過動之治療藥有種種副作用之報告,而吾人係期待無副作用之膀胱過動之預防劑或治療劑。
本發明提供一種含有5-胺基乙醯丙酸(ALA)類作為有效成分之膀胱過動之預防劑或治療劑。
Description
本發明係有關用於預防或治療膀胱過動之醫藥組成物。
膀胱過動為以尿意急迫感為必須症狀,有伴隨夜間頻尿或頻尿症狀之症候群。此處,尿意急迫感為「突然引起不能忍受之強的尿意,很難說明與通常尿意之不同者」,惟,其病態生理或發症機序尚未解明。又,已知膀胱過動於40歲以上之男女,8人中有1人有該症狀。
作為膀胱過動之治療劑,主要使用鹽酸丙哌維林(Propiverine HCl)及鹽酸奧昔布寧(Oxybutynin HCl)等抗膽鹼劑。抗膽鹼劑阻礙使副交感神經亢進之乙醯膽鹼的作用,其結果阻礙排尿促進。近年來,作為與抗膽鹼劑具有不同作用機序之膀胱過動之治療劑,使用β3腎上腺素受體激動劑(專利文獻1)。β3腎上腺素受體激動劑與上述抗膽鹼劑相反,已知為存在於膀胱之β3腎上腺素受體,更進一步使交感神經亢進者。
[專利文獻1]WO2004/041276
上述抗膽鹼劑有排出障礙、口渇等副作用之報告。又,關於β3腎上腺素受體激動劑亦有以口渇、便秘、發疹、蕁麻疹等為主要副作用之報告。因此,考慮到提昇膀胱過動病患之生活品質(QOL),期待無副作用之膀胱過動之預防/改善劑之製劑。
本發明人等對於可成為無副作用之膀胱過動之預防/改善劑之化合物進行深入研究時,令人驚奇的發現5-胺基乙醯丙酸類(於本專利申請之說明書中亦稱為「ALA類」)具有膀胱過動之改善作用,因而完成本發明。
5-胺基乙醯丙酸(於本專利申請之說明書中亦稱為「ALA類」)廣泛存在於動物、植物或菌類,為生體內含有之天然胺基酸之一種。已知ALA對於生體具有高的安全性,已知可用於光動力學治療之光增感劑、植物成長調節劑、除草劑、魚類病原性微生物、寄生蟲感染之治療、豬成長促進劑等。惟,ALA對於膀胱過動之作用至今仍未知。
亦即,本發明於一實施形態中,為使用於膀胱過動的預防或治療之醫藥組成物,且為含有下述式(I) 表示之化合物或其鹽之醫藥組成物R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)(式中,R1表示氫原子或醯基,R2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基)。
又,本發明之特徵為於一實施形態中,上述膀胱過動為呈現頻尿症狀之膀胱過動。
又,本發明之特徵為於一實施形態中,R1為由氫原子、碳數1至8之烷醯基及碳數7至14之芳醯基所構成之群組選擇者,R2為由氫原子、直鏈或支鏈狀之碳數1至8之烷基、碳數3至8之環烷基、碳數6至14之芳基及碳數7至15之芳烷基所構成之群組選擇者。
又,本發明之特徵為於一實施形態中,R1及R2為氫原子。
又,本發明之特徵為於一實施形態中,另含有一種或二種以上含有金屬之化合物。
又,本發明之特徵為於一實施形態中,含有金屬之化合物為含有鐵、鎂、鋅、鎳、釩、銅、鉻、鉬或鈷之化合物。
又,本發明之特徵為於一實施形態中,含有金屬之化合物為含有鐵、鎂或鋅之化合物。
又,本發明之特徵為於一實施形態中,含有金屬之化合物為含有鐵之化合物。
又,本發明之特徵為於一實施形態中,上 述含有鐵之化合物為檸檬酸亞鐵鈉。
本發明之其他實施形態係有關為了膀胱過動之預防劑或治療劑的製造,使用下述式(I)表示之化合物或其鹽R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)(式中,R1表示氫原子或醯基,R2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基)。
本發明之其他實施態樣係有關預防或治療膀胱過動之方法,為包含對於對象投予治療上有效量之下述式(I)表示之化合物或其鹽之步驟之方法R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)(式中,R1表示氫原子或醯基,R2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基)。
又,將上述所敍述之本發明之一或複數特徴任意組合之發明亦包含於本發明之範圍。
第1圖表示於對照群及各實驗群,1次排尿量之圖。
第2圖表示於對照群及各實驗群,24小時排尿量之圖。
第3圖表示於對照群及各實驗群,24小時飲水量之圖。
第4圖表示於對照群及各實驗群,排尿肌活動狀態之圖。
第5圖表示於對照群及各實驗群,比較排尿間隔(秒)之圖。
第6圖表示於對照群及各實驗群,比較膀胱血流量之圖。
第7圖表示於對照群及各實驗群,比較於膀胱組織中VEGF表現量之圖。
第8圖表示於對照群及各實驗群,比較於膀胱組織中MDA表現量之圖。
第9圖表示於對照群及各實驗群,比較於膀胱組織中NGF表現量之圖。
第10圖表示於對照群及各實驗群,比較於膀胱組織中Nrf2表現量之圖。
本發明係有關用於預防或治療膀胱過動之醫藥組成物。於本發明,「膀胱過動」係指以尿意急迫感為必須症狀,有伴隨頻尿、夜間頻尿、急迫性尿失禁症狀之症候群。亦即,有頻尿/尿意急迫感、未呈現失禁症狀亦包含於本發明之膀胱過動。
於本發明,「頻尿」為膀胱過動主要症狀之一,係指例如從起床後到就寢之間有8次以上尿意或是於就寢中有1次以上尿意之症狀。
本說明書,ALA類係指ALA、其衍生物或 該等之鹽。
於本說明書,ALA係指5-胺基乙醯丙酸。ALA亦稱為δ-胺基乙醯丙酸,為胺基酸之1種。
ALA之衍生物可例示下述式(I)表示之化合物。於式(I),R1表示氫原子或醯基,R2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基。又,於式(I),ALA相當於R1及R2為氫原子之情況。
R
1
-NHCH
2
COCH
2
CH
2
COOR
2
(I)
ALA類只要於生體內以式(I)之ALA或其衍生物之狀態作為有效成分作用即可,亦可作為以經生體內之酵素分解之前藥(前驅體)投予。
式(I)之R1之醯基可列舉甲醯基、乙醯基、丙醯基、丁醯基、異丁醯基、戊醯基、異戊醯基、三甲基乙醯基、己醯基、辛醯基、苯甲基羰基等直鏈或支鏈狀之碳數1至8之烷醯基,或苯甲醯基、1-萘甲醯基、2-萘甲醯基等碳數7至14之芳醯基。
式(I)之R2之烷基可列舉甲基、乙基、丙基、異丙基、丁基、異丁基、第二丁基、第三丁基、戊基、異戊基、新戊基、己基、庚基、辛基等直鏈或支鏈狀之碳數1至8之烷基。
式(I)之R2之環烷基可列舉環丙基、環丁基、環戊基、環己基、環庚基、環辛基、環十二烷基、1-環己烯基等飽和或部分不飽和鍵結合存在之碳數3至8之環烷 基。
式(I)之R2之芳基可列舉苯基、萘基、蒽基、菲基等碳數6至14之芳基。
式(I)之R2之芳烷基,芳基部分可列示與上述芳基相同之基,烷基部分可例示與上述烷基相同之基,具體而言,可列舉苯甲基、苯乙基、苯基丙基、苯基丁基、二苯甲基、三苯甲基、萘甲基、萘乙基等碳數7至15之芳烷基。
較佳之ALA衍生物可列舉R1為甲醯基、乙醯基、丙醯基、丁醯基等之化合物。又,較佳之ALA衍生物可列舉上述R2為甲基、乙基、丙基、丁基、戊基等之化合物。又,較佳之ALA衍生物可列舉上述R1與R2之組合為(甲醯基與甲基)、(乙醯基與甲基)、(丙醯基與甲基)、(丁醯基與甲基)、(甲醯基與乙基)、(乙醯基與乙基)、(丙醯基與乙基)、(丁醯基與乙基)之各組合之化合物。
ALA類中作為ALA或其衍生物之鹽可列舉藥理學上容許之酸加成鹽、金屬鹽、銨鹽、有機胺加成鹽等。酸加成鹽可例示例如鹽酸鹽、氫溴酸鹽、氫碘酸鹽、磷酸鹽、硝酸鹽、硫酸鹽等各無機酸鹽,甲酸鹽、乙酸鹽、丙酸鹽、甲苯磺酸鹽、琥珀酸鹽、草酸鹽、乳酸鹽、酒石酸鹽、乙醇酸鹽、甲磺酸鹽、丁酸鹽、戊酸鹽、檸檬酸鹽、富馬酸鹽、馬來酸鹽、蘋果酸鹽等各有機酸加成鹽。金屬鹽可例示鋰鹽、鈉鹽、鉀鹽等各鹼金屬鹽,鎂、鈣鹽等各鹼土類金屬鹽,鋁、鋅等各金屬鹽。銨鹽可例示銨鹽、四 甲基銨鹽等烷基銨鹽等。有機胺鹽可例示三乙基胺鹽、哌啶鹽、嗎啉鹽、甲苯胺鹽等各鹽。又,該等鹽亦可於使用時作成溶液使用。
以上之ALA類中,最理想者為ALA及ALA甲酯、ALA乙酯、ALA丙酯、ALA丁酯、ALA戊酯等各種酯類及該等之鹽酸鹽、磷酸鹽、硫酸鹽。又可例示ALA鹽酸鹽、ALA磷酸鹽特別好。
上述ALA類例如可藉由化學合成、藉由微生物生產、藉由酵素生產等公知之方法製造。又,上述ALA類亦可形成水合物或溶劑合物,亦可將ALA類單獨或2種以上適當組合使用。
將上述ALA類調製成水溶液時,為了防止ALA類分解,需留意水溶液不成為鹼性。於已成為鹼性時,藉由除去氧可防止分解。
本發明之醫藥組成物於一實施形態中,可另含有一種或二種以上之含有金屬之化合物。相關之含有金屬之化合物之金屬部分可列舉鐵、鎂、鋅、鎳、釩、鈷、銅、鉻、鉬。較佳之實施形態為含有金屬之化合物之金屬部分為鐵、鎂或鋅,更好為鐵。
可於本發明中使用之鐵化合物可為有機鹽,亦可為無機鹽。無機鹽可列舉氯化鐵、三氧化二鐵、硫酸鐵、焦磷酸亞鐵。有機鹽可列舉羥基羧酸鹽等羧酸鹽、檸檬酸亞鐵、檸檬酸鐵鈉、檸檬酸亞鐵鈉(SFC)、檸檬酸鐵銨等檸檬酸鹽或焦磷酸鐵、血紅素鐵、右旋糖酐鐵、乳酸鐵、 葡萄糖酸亞鐵、二伸乙基三胺五乙酸鐵鈉、二伸乙基三胺五乙酸鐵銨、乙二胺四乙酸鐵鈉、乙二胺五乙酸鐵銨、二羧甲基麩胺酸鐵鈉、二羧甲基麩胺酸鐵銨、富馬酸亞鐵、乙酸鐵、草酸鐵、琥珀酸亞鐵、琥珀酸檸檬酸鐵鈉等有機酸鹽或二伸乙基三胺鐵、乳鐵蛋白鐵、運鐵蛋白鐵、鐵葉綠酸鈉、鐵蛋白鐵、含糖氧化鐵、甘胺酸亞鐵硫酸鹽。
可於本發明中使用之鎂化合物可列舉檸檬酸鎂、苯甲酸鎂、乙酸鎂、氧化鎂、氯化鎂、氫氧化鎂、碳酸鎂、硫酸鎂、矽酸鎂、硝酸鎂、二伸乙基三胺五乙酸鎂二銨、乙二胺四乙酸鎂二鈉、鎂原紫質。
可於本發明中使用之鋅化合物可列舉氯化鋅、氧化鋅、硝酸鋅、碳酸鋅、硫酸鋅、二伸乙基三胺五乙酸鋅二銨、乙二胺四乙酸鋅二鈉、鋅原紫質、含鋅酵母。
對象之含有金屬之化合物之投予量,對於對象之ALA之投予量只要莫耳比為0至100倍即可,較好為0.01倍至10倍,更好為0.1倍至8倍。
本發明醫藥組成物中含有之ALA類及含有金屬之化合物,即使作為含有ALA類及含有金屬之化合物之組成物,雖可各自單獨投予,惟,即使於各自單獨投予之情況,較好為同時投予,此處,同時係指不僅是同時進行,即使不是同時,為了可發揮投予ALA類及含有金屬之化合物之加成效果,較好兩者之間無相當的間隔地進行可發揮相乘效果。
本發明中之ALA類及含有金屬之化合物之 投予路徑並無特別限制,可全身投予,亦可局部投予。投予路徑可列舉例如包含舌下投予之經口投予、吸入投予、藉由導管對於標的組織或臓器直接投予、包含點滴之静脈內投予、藉由貼付劑等之經皮投予、栓劑或藉由使用經鼻胃管、經鼻腸管、胃造口管或腸造口管之強制經腸營養法投予等非經口投予等。又,如上所述,可將ALA類及含有金屬之化合物從不同之路徑投予。
本發明中使用之ALA類、含有金屬之化合物或將該等組合之調配劑之劑型可對應上述投予路徑適當決定,並無特別限制,可列舉注射劑、點滴劑、錠劑、膠囊劑、細粒劑、散劑、液劑、溶解於糖漿等之水劑、貼附劑、栓劑等。
本發明相關之醫藥組成物必要時可加入其他之藥效成分、營養劑、載體等其他任意成分。任意成分可添加例如結晶性纖維素、明膠、乳糖、澱粉、硬脂酸鎂、滑石、植物性及動物性脂肪、油脂、膠、聚伸烷基二醇等藥學上容許之通常之載體、黏合劑、安定化劑、溶劑、分散劑、增量劑、賦形劑、稀釋劑、pH緩衝劑、崩解劑、可溶化劑、溶解補助劑、等張劑等各種調劑用調配成分。
於對象投予本發明醫藥組成物之頻率或投予期間可由業者(例如醫師)考慮對象之症狀或狀態等適當決定。
於本說明書中使用之用語除去經特別定義者,為用於說明特定實施態樣,本發明不只限於此。
於本說明書中使用之「包含」之用語為文理上可明白地有不同理解之情況除外,為表示所敍述之事項(部材、步驟、要素、數字等)存在,未排除該等以外之事項(部材、步驟、要素、數字等)存在。
不同之定義為無限,此處使用之所有用語(包含技術用語及科學用語)具有與本發明所屬技術之業者充分理解之相同意思。此處使用之用語只要不是有明示不同之定義,都可作為具有與本說明書及於相關技術領域相同意思來解釋,而不是於理想化或過度形式的意思來解釋。
於以下,參照實施例對本發明加以詳細說明。惟,本發明可藉由種種態樣具體化,不只限於此處所記載之實施例。
實施例1(藉由ALA之1次排尿量等之增加效果)
實驗群
實驗大鼠使用12週齡之雄性SHR(自發性高血壓大鼠(spontaneously hypertension rats),藉由下述ALA之投予條件,將實驗群分為I至III群。於實驗群II,於實驗開始日經口投予ALA及檸檬酸亞鐵鈉。ALA之投予量為10mg/kg體重,檸檬酸亞鐵鈉為15.7mg/kg體重。另一方面,於實驗群III,ALA之投予量為100mg/kg體重,檸檬酸亞鐵鈉為157mg/kg體重。又,於對照群I,只投予與 ALA同量之生理食鹽水替代ALA及檸檬酸亞鐵鈉。
ALA投予條件
於對照群I,從實驗開始日(12週齡)至第6週(18週齡),每日經口投予生理食鹽水。
於實驗群II及III,從實驗開始日(12週齡)至第6週(18週齡),每日經口投予ALA及檸檬酸亞鐵鈉。
排尿動態測定法
對於各實驗群,藉由代謝籠實施排尿動態測定。具體而言,於12週齡(ALA投予前)時及於18週齡(ALA投予後)時實施測定,測定1次之排尿量、24小時之排尿量、飲水量。此處,藉由代謝籠之測定方法採用以Yono人等生活科學(Yono et al.,Life Sci.,)2007 June 27;81(3):218-222為基礎之方法(小鼠排尿機能之無麻醉/無拘束/晝夜連續測定法)。又,因為與體重/血壓/心跳有關,於排尿動態測定前另測定排尿量及飲水量。再者,排尿動態測定,時亦測定相關之總排尿次數。
結果
結果表示於第1圖至第3圖。第1圖表示於各實驗群1次排尿量之結果,縱軸表示排尿量,橫軸表示有無投予ALA。如第1圖所示,與對照群相比,確認藉由投予ALA,1次排尿量增加(約3成左右)。
又,第2圖表示於各實驗群24小時排尿量之結果,縱軸表示排尿量,橫軸表示有無投予ALA。如第2圖所示,與對照群相比,確認藉由投予ALA,24小時之排尿量增加。
另,第3圖表示於各實驗群24小時飲水量之結果,縱軸表示飲水量,橫軸表示有無投予ALA。從第3圖明瞭,確認藉由投予ALA,飲水量增加。
此處,通常於膀胱過動之情況與未罹患膀胱過動之情況相比,膀胱之容量無差異。因此,於膀胱過動模型大鼠,從確認1次排尿量、24小時排尿量、飲水量增加,認為ALA作用於膀胱血流調整,有助於膀胱之貯尿容量的增加。因此,為了確認藉由ALA膀胱血流之變化,實施膀胱內壓的測定。
實施例2(藉由ALA之排尿期間延長效果)
膀胱內壓測定法
於上述排尿動態測定法之後,以下述之步驟實施膀胱內壓測定法。又,膀胱內壓測定為確認排尿肌之過動狀態,確立作為膀胱過動之檢査手法。
(1)將18週齡雄性SHR/Hos大鼠及Wistar/ST大鼠藉由胺基甲酸酯(1.0g/kg,i.p.)全身麻醉。
(2)將各大鼠放倒,將四肢以膠帶固定後進行開腹,擠壓膀胱使排尿。為了防止乾燥,蓋上生理食鹽水脫脂綿放 置30分鐘。
(3)於各大鼠之膀胱插入膀胱內壓測定用之導管。
此處,導管連接三方活栓,一端連接於注射泵,將生理食鹽水以一定之速度(12mL/小時)持續注入膀胱內。另一端連接於壓力轉換器,以壓力放大器進行監控器增幅,藉由PowerLab系統放入個人電腦記錄之。
(*PowerLab(16ch高速PowerLab系統):PowerLab/16SP model ML 795,ADI(AD Instruments),USA)
(4)之後注入生理食鹽水,放置約30分鐘至安定。
(5)邊看波形邊採取1次之尿至1.5mL管子中,測定尿之重量。
(6)採取各大鼠之殘尿測定量。
(7)將相同之間隔、高度之高峰連續採取6次(約1小時)。
結果
結果表示於第4圖及第5圖。第4圖中,(a)表示對照群I之結果,(b)表示實驗群II之結果,(c)表示實驗群III之結果。於各圖,縱軸表示膀胱內壓,橫軸表示時間(秒)。又,第5圖為將第4圖表示之圖以排尿間隔(秒)為基礎使變形。如第4及5圖所示,藉由投予ALA,與未投予ALA之群相比,確認排尿間隔的延長。從該結果認為藉由投予ALA,因膀胱過動而萎縮之膀胱被擴張,認為藉由此使膀胱中之貯尿容量增加。
實施例3(藉由ALA之膀胱血流改善效果)
方法
於上述膀胱內壓測定後,以下述之步驟實施測定膀胱血流(氫廓清法)。
(1)於各大鼠之前胸部下面埋入為參照電極之氯化銀盤。
(2)於膀胱壁內刺入線型白金電極(於膀胱壁之3個地方各採取3次之數值)。
(3)使用UH-METER測定血流。
具體而言,將氫彈打開至0.3L/min,使用漏斗將100%氫直接吸引。給予氫至達到高峰為止,藉由PowerLab系統測定氫廓清曲線。將氫廓清曲線開始下降之時點作為0秒,記錄約180秒。
(4)藉由迴歸曲線算出血流量。
*迴歸曲線藉由Y=B-A尋求半衰期(T1/2)。
血流量=69.3/T1/2(mL/min/100g)
(*PowerLab(16ch高速PowerLab系統):PowerLab/16SP model ML 795,ADI(AD Instruments),USA)
結果
結果表示於第6圖。於第6圖,縱軸表示膀胱血流量,橫軸表示各實驗群。從第6圖明瞭藉由投予ALA,確認依 賴ALA之投予量,膀胱血流有增加之傾向。合併第4圖及第5圖之結果可說藉由膀胱血流的增加,使因膀胱過動導致萎縮之膀胱擴張。其結果為確認藉由投予ALA改善膀胱過動。
實施例4(藉由投予ALA之膀胱過動之改善作用機序的驗證)
為了更詳細的驗證根據上述實施例驗證之藉由投予ALA膀胱過動之改善作用機序,進行對於投予ALA與膀胱血管內皮障礙及氧化壓力之關係之檢討。使用VEGF(血管內皮生長子(Vascular Endothelial Growth Factor))作為對象之膀胱血管內皮障礙之標識,使用MDA(丙二醛(Malondialdehyde))、NGF(神經生長因子(Nerve Growth Factor))及Nrf2(核內呼吸因子2(Nuclear Respiratory Factor 2))作為氧化壓力標識。
1.VEGF之測定
對於在對象投予ALA與VEGF表現量之變化進行檢討。VEGF為血管內皮增殖因子,作為膀胱血管內皮障礙之標識使用。
實驗群之準備
實驗群及對照群之準備以與實施例1記載之方法相同之方法及條件進行。
大鼠膀胱組織試樣之調整
將實驗群及對照群之膀胱組織以下述之步驟處理,作為試樣使用。
1.將100mg之組織以1xPBS洗淨。
2.以1xPBS 500μl均質化。
3.於-20℃保存一晚。
4.進行凍結融解將細胞膜破壞,於4℃離心分離5000G,5分鐘
5.分注之,於-20℃或-80℃保存。
6.融解後再進行一次離心分離,於分析中使用。
VEGF之測定
使用Rat VEGF ELISA kit(CUSABIO CSB-E04757r),根據製造業者提供之計劃書進行ELISA分析。
結果
測定結果表示於第7圖。如第7圖所示,於實驗群(ALA投予群),與對照群比較,於膀胱組織中VEGF表現量顯著降低。
2.MDA之測定
對於在對象投予ALA與MDA表現量之變化進行檢討。MDA為脂質過氧化分解生成物之一種,已知為脂質過氧化 之主要標識。
實驗群之準備
實驗群及對照群之準備以與實施例1記載之方法相同之方法及條件進行。
大鼠膀胱組織之試樣調整
將實驗群及對照群之膀胱組織以下述之步驟處理,作為試樣使用。
1.以冷分析緩衝液(cold assay buffer)400μl生物搗碎(Biomasher)。
2.於4℃以15000rpm進行離心分離5分鐘。離心分離後於上清液加入緩衝液300μl,以on ice保存。
3.校正蛋白質濃度。
MDA之測定
使用丙二醛(MDA)分析kit(NWK-MDA01),根據製造業者提供之計劃書進行ELISA分析。
結果
測定結果表示於第8圖。如第8圖所示,於實驗群(ALA投予群),與對照群比較,於膀胱組織中MDA表現量顯著降低。
3.NGF之測定
對於在對象投予ALA與NGF表現量之變化進行檢討。由於膀胱內NGF若增加,則排尿反射亢進,其結果導致膀胱過動,NGF作為下部尿路機能障礙標識使用。
實驗群之準備
實驗群及對照群之準備以與實施例1記載之方法相同之方法及條件進行。
調整大鼠膀胱組織之試樣
將實驗群及對照群之膀胱組織以下述之步驟處理,作為試樣使用。
1.將100mg之組織以1xPBS洗淨。
2.以1xPBS 1mL均質化。
3.於-20℃保存一晚。
4.進行凍結融解將細胞膜破壞,於4℃離心分離5000G,5分鐘
5.分注之,於-20℃或-80℃保存。
6.融解後再進行一次離心分離,於分析中使用。
NGF之測定
使用Rat MGF ELISA kit(CUSABIO CSB-E24685r),根據製造業者提供之計劃書進行ELISA分析。
結果
測定結果表示於第9圖。如第9圖所示,於實驗群(ALA投予群),與對照群比較,於膀胱組織中NGF表現量顯著降低。
4.Nrf2之測定
對於在對象投予ALA與Nrf2表現量之變化進行檢討。Nrf2為調節抗氧化酵素或解毒代謝酵素之表現,調控氧化壓力之轉錄因子之一,作為氧化壓力標識使用。
實驗群之準備
實驗群及對照群之準備以與實施例1記載之方法相同之方法及條件進行。
調整大鼠膀胱組織之試樣
將實驗群及對照群之膀胱組織以下述之步驟處理,作為試樣使用。
1.以PBS清洗多餘之血液。
2.測定重量。
3.於On Ice,於生物搗碎器中放入PBS600μl,將組織絞碎。
4.進行超音波處理或凍結融解(-20℃/室溫)3次。
5.以5000G進行離心分離5分鐘。
6.將上清液移至新的試管(測定蛋白質濃度)。
Nrf2之測定
使用Rat NFE2L2/NRF2 ELISA kit(LSBio LS-F12145),根據製造業者提供之計劃書進行ELISA分析。
結果
測定結果表示於第10圖。如第10圖所示,於實驗群(ALA投予群),與對照群比較,膀胱組織中Nrf2表現量顯著降低。
考察
如上述之結果,於投予ALA之大鼠之膀胱組織,與對照群比較,VEGF、MDA、NGF、Nrf2之表現量顯著降低。由於VEGF與膀胱血管內皮障礙有關,MDA、NGF及Nrf2與組織之氧化壓力有關,藉由投予ALA,膀胱之血流獲得改善之結果,減輕膀胱組織之組織障礙或氧化壓力,暗示有抑制排尿肌過動之作用機序。
Claims (11)
- 一種醫藥組成物,為用於膀胱過動之預防或治療用之醫藥組成物,含有下述式(I)表示之化合物或其鹽 R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)式中,R 1表示氫原子或醯基,R 2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基。
- 如申請專利範圍第1項所述之醫藥組成物,其中,上述膀胱過動為呈現頻尿症狀之膀胱過動。
- 如申請專利範圍第1項或第2項所述之醫藥組成物,其中,R 1為由氫原子、碳數1至8之烷醯基及碳數7至14之芳醯基所構成之群組選擇者,R 2為由氫原子、直鏈或支鏈狀之碳數1至8之烷基、碳數3至8之環烷基、碳數6至14之芳基及碳數7至15之芳烷基所構成之群組選擇者。
- 如申請專利範圍第3項所述之醫藥組成物,其中,R 1及R 2為氫原子。
- 如申請專利範圍第1項至第4項中任一項所述之醫藥組成物,該醫藥組成物另含有一種或二種以上之含有金屬之化合物。
- 如申請專利範圍第5項所述之醫藥組成物,其中,該含有金屬之化合物為含有鐵、鎂、鋅、鎳、釩、銅、鉻、鉬或鈷之化合物。
- 如申請專利範圍第5項所述之醫藥組成物,其中,該含 有金屬之化合物為含有鐵、鎂或鋅之化合物。
- 如申請專利範圍第5項所述之醫藥組成物,其中,該含有金屬之化合物為含有鐵之化合物。
- 如申請專利範圍第8項所述之醫藥組成物,其中,上述含有鐵之化合物為檸檬酸亞鐵鈉。
- 一種下述式(I)表示之化合物或其鹽之用途,其係用於製造膀胱過動之預防劑或治療劑, R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)式中,R 1表示氫原子或醯基,R 2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基。
- 一種預防或治療膀胱過動之方法,該方法包含對於對象投予治療上有效量之下述式(I)表示之化合物或其鹽之步驟 R 1 -NHCH 2 COCH 2 CH 2 COOR 2 (I)式中,R 1表示氫原子或醯基,R 2表示氫原子、直鏈或支鏈狀烷基、環烷基、芳基或芳烷基。
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