TWI769981B - 補充n-乙醯半胱胺酸及甘胺酸以改善穀胱甘肽含量之益處 - Google Patents
補充n-乙醯半胱胺酸及甘胺酸以改善穀胱甘肽含量之益處 Download PDFInfo
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- TWI769981B TWI769981B TW105116728A TW105116728A TWI769981B TW I769981 B TWI769981 B TW I769981B TW 105116728 A TW105116728 A TW 105116728A TW 105116728 A TW105116728 A TW 105116728A TW I769981 B TWI769981 B TW I769981B
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Abstract
本發明係關於涉及使用甘胺酸及N-乙醯半胱胺酸於與甘胺酸、N-乙醯半胱胺酸及/或穀胱甘肽含量減少相關之各種醫學病況的組合物及方法。
Description
本申請案主張於2015年5月28日申請之美國臨時專利申請案第62/167,433號之優先權,該申請案以全文引用之方式併入本文中。
本發明至少係針對生物化學、細胞生物學、化學、分子生物學及醫學領域。
衰老之自由基理論提出,衰老之生物過程在老年人體內引起氧化壓力之增加。細胞抵抗氧化壓力之潛在損害的能力係由氧化性自由基之產生與細胞可用之抗氧化劑防禦陣列之間的重要平衡決定的。存在多個抗氧化防禦系統且在此等系統中,穀胱甘肽(GSH)為所有抗氧化防禦中含量最豐富的細胞內組分。GSH(一種三肽)係由前驅體胺基酸麩胺酸、半胱胺酸及甘胺酸,在麩胺酸半胱胺酸連接酶(GCL,亦稱作γ-麩胺醯半胱胺酸合成酶,EC 6.3.2.2)及γ-L-麩胺醯基-L-半胱胺酸:甘胺酸連接酶(亦稱作穀胱甘肽合成酶,EC 6.3.2.3)催化下,分兩個步驟合成,且GSH合成在細胞中係重新合成。
穀胱甘肽缺乏已涉及若干人類疾病,包括糖尿病、HIV感染、兒童蛋白質能量營養不良、鐮狀細胞性貧血、感染、諸如帕金森氏病
(Parkinson's disease)之神經病症、肝病及囊腫性纖維化。由若干動物研究(Stohs等人,1984;Farooqui等人,1987;Liu等人,2000)及人類研究(Al-Turk等人,1987;Matsubara等人,1991;Lang等人,1992;Samiec等人,1998;Erden-Inal等人,2002;Loguercio等人,1996)得到之證據表明,穀胱甘肽之濃度亦隨衰老而降低。衰老過程中GSH之缺乏與促氧化轉變增加(Rebrin,2008)導致氧化壓力增加相關聯(Rikans及Hornbrook,1997)。此等變化已涉及諸如白內障(Campisi等人,1999;Castorina等人,1992;Sweeney等人,1998)、年齡相關之黃斑變性(Samiec,1998)、免疫功能改變(Fidelus及Tsan,1987;Furukawa等人,1987)及神經退化性疾病(Liu等人,2004)之衰老性疾病,且在分子層面上涉及DNA損害之增加(Hashimoto等人,2008)。雖然尚未充分瞭解衰老相關穀胱甘肽缺乏的潛在機制,但有跡象表明可能涉及穀胱甘肽合成之擾亂(Toroser及Sohal,2007)。
其他及更多目標、特徵及優點將自以下出於揭示目的而給出的本發明之當前較佳實施例的描述而顯而易知。
本發明之實施例係關於用於治療或預防與細胞內GSH含量減少直接或間接相關之醫學病況或身體狀況,或延緩其發作的方法及/或組合物。本發明之實施例亦係關於用於治療或預防與半胱胺酸及/或甘胺酸之血液或細胞內含量減少直接或間接相關之醫學病況或身體狀況,或延緩其發作的方法及/或組合物。在特定實施例中,使個體中之細胞內GSH含量增加,此後醫學病況或身體狀況由此得以治療、預防,或發作延緩。在某些實施例中,使個體中之C反應蛋白(CRP)含量減少,此後醫學病況或身體狀況由此得以治療、預防,或發作延緩。
在特定實施例中,涵蓋自穀胱甘肽、n-乙醯半胱胺酸及/或甘胺
酸提供益處之方法,且在特定情形中,穀胱甘肽、n-乙醯半胱胺酸及/或甘胺酸各自單獨地及/或共同地具有作用。
在本發明之一個實施例中,存在一種使有需要之個體中之半胱胺酸及甘胺酸(例如,半胱胺醯甘胺酸)(或其功能性衍生物)之血液含量增加以增加細胞內GSH含量的方法。個體可已知具有將得益於GSH含量增加之醫學病況或身體狀況,或個體可懷疑具有將得益於GSH含量增加之醫學病況或身體狀況。在特定實施例中,經受本發明之方法及/或組合物的個體希望預防一或多種不合需要的身體狀況(或其影響,諸如伴隨衰老的影響)或醫學病況。在某些實施例中,出於增加GSH含量之明確目的,向個體提供有效含量之半胱胺酸及甘胺酸或其功能性衍生物以治療、預防醫學病況或身體狀況,或延緩其發作。
在特定實施例中,個體被鑑別為需要治療(或預防或延緩發作)與GSH含量不足相關之醫學病況。
本發明之實施例係關於用於治療或預防與個體之一或多個細胞中之穀胱甘肽含量不足相關之一或多種醫學病況或身體狀況,或延緩其發作的各種方法。在特定實施例中係用於治療或預防與細胞內甘胺酸及/或半胱胺酸濃度不足相關之一或多種醫學病況或身體狀況,或延緩其發作的方法。在特定態樣中,方法由於獨立於GSH恢復甘胺酸及/或半胱胺酸之細胞內濃度的固有益處而允許治療或預防一或多種醫學病症或身體狀況,或延緩其發作。在特定實施例中,該病況或身體狀況包括以下至少一者或多者:肌肉損失(出於任何原因,至少包括肌肉減少症、HIV感染、衰老及/或惡病質、失重之有害影響);器官損害(例如,由糖尿病及胰島素抗性引起且包括糖尿病性腎病);心臟功能及衰竭(例如,預防或改善心臟衰竭及/或改善心臟收縮功能);脂肪肝;癌症預防;用於預防日後發展肥胖症及/或糖尿病之胎兒代謝程式化;妊娠期糖尿病中之母體及胎兒的健康狀況;運動能力及身
體機能;肥胖症;生活品質;壽命;神經退化性疾病;用於預防經歷對比研究或程序或者HIV相關神經病變之個體之腎病的防治;乙醯胺苯酚毒性之預防;非酒精性脂肪變性肝炎;非酒精性脂肪肝疾病(包括伴隨或不伴隨發炎);耳鳴;頭暈;酒精宿醉;聽覺障礙;阿茲海默氏病(Alzheimer's);帕金森氏病;骨質疏鬆、高血壓、動脈粥樣硬化/冠狀動脈疾病,及壓力(諸如由於燒傷或創傷)後之心肌損害;囊腫性纖維化;脂肪肝疾病之非酒精性脂肪肝疾病;炎症;改善記憶及認知;創傷後(例如,手術後、敗血症後,或由事故或身體攻擊引起之鈍挫傷或穿透傷後等)恢復及存活;創傷性腦損傷(包括震盪);改善自一般創傷及手術之恢復;糖尿病預防;前期糖尿病/代謝症候群之治療或預防;等等。
在一個實施例中,存在一種預防及/或治療肌肉減少症、肌肉減少性肥胖症或惡病質之方法。在針對惡病質之特定實施例中,惡病質係由於潛在的醫學病況而存在於個體中,該潛在醫學病況諸如長期生病、患有HIV、患有癌症、患有COPD、原本健康個體之衰老(肌肉減少症)等等。在針對老年HIV病患之特定實施例中,補充本文中涵蓋之組合物使穀胱甘肽增加且引起瘦體重(肌肉)增加及脂肪組織減少。
本發明之特定實施例提供對由低GSH含量(包括在已知富含穀胱甘肽之眼部晶狀體中的低含量)直接或間接導致的眼部病況之預防及/或治療。該等病況包括例如白內障及/或青光眼、老花眼(隨著衰老而喪失近距視力,需要老花眼鏡),或老年性耳聾(隨著衰老而喪失聽力,需要助聽器)。
在特定實施例中,存在一種預防及/或治療任何種類之發炎的方法,且在特定實施例中,該方法涉及減少C反應蛋白(CRP;發炎標記物)或TNF-α之下降(諸如在HIV病患中)。在特定實施例中,炎症與對有害刺激(包括一或多種病原體、受損細胞及/或刺激物)之反應有關。
炎症可為急性或慢性的。在一些狀況下,炎症與諸如衰老、糖尿病、座瘡、哮喘、自體免疫疾病、脂瀉病、***炎、絲球體腎炎、發炎性腸病、***、再灌注損傷、類風濕性關節炎、類肉瘤病、移植排斥、血管炎、間質性膀胱炎、動脈粥樣硬化、過敏、肌病、白血球缺乏、藥物反應(諸如***或搖頭丸(ecstasy))、癌症、抑鬱、肌肉修復等病症相關聯。認識到炎症與免疫力相關聯,且在特定實施例中,存在向接受疫苗之個體提供NAC及甘胺酸以增強對疫苗之免疫反應的方法。
在特定實施例中,本發明之方法預防且緩解/治療粒線體毒性,包括藥物誘發之粒線體毒性。舉例而言,向患有HIV且接受對粒線體功能有害之抗反轉錄病毒HIV藥物治療的個體提供有效量的NAC及甘胺酸以改善粒線體功能。
在特定實施例中,存在一種預防及/或治療乙醯胺苯酚毒性之方法。特定言之,向打算攝入乙醯胺苯酚或正服用乙醯胺苯酚或具有乙醯胺苯酚毒性之個體提供有效含量的如本文中所涵蓋的一或多種組合物。具有乙醯胺苯酚毒性之個體可為或可不為乙醯胺苯酚的長期使用者。在特定實施例中,個體在服用增加個體中GSH含量之一或多種藥劑的同時,服用乙醯胺苯酚。
在特定實施例中,存在一種改善肌肉效能及恢復(諸如自肌肉壓力,包括與運動相關之肌肉壓力恢復)之方法。在特定實施例中,個體為運動員,但個體可不為運動員。個體可出於娛樂及/或健康目的而參與運動。個體可在運動之前、期間及/或之後(包括運動之前及/或之後的數分鐘、數小時或數天之前及/或之後及之內)服用增加個體中GSH含量的一或多種藥劑。個體可在運動之前、期間及/或之後(包括運動之前及/或之後的數分鐘、數小時或數天之前及/或之後及之內)服用提高個體中半胱胺酸及/或甘胺酸之細胞內含量的一或多種藥劑。
在特定實施例中,提高細胞內NAC及/或甘胺酸增進肌肉效能及/或恢復,與其對GSH之影響無關。運動可屬於任何類型,包括例如有氧(「心肺(cardio)」)運動及/或負重訓練。個體可具有直接或間接與GSH含量減少相關聯之醫學病況或身體狀況。在特定實施例中,個體為患有HIV之老年個體,諸如年齡為50歲或更大的個體。研究表明,接受本文中所涵蓋之組合物的老年HIV病患在2週內雙手的肌肉強度顯著增加。
本發明之實施例包括用於治療、預防非老年個體之加速衰老,或延緩其發作的方法;該加速衰老可歸於任何原因,至少包括如患有HIV感染或暴露於零重力任何時間段之彼等者。在某些實施例中,存在加速衰老(諸如在HIV、失重,或存在年齡相關性缺陷(機能減退、肌肉強度損失、生活品質降低、白內障形成、免疫衰老)情況下所見,諸如通常見於非HIV人員(大約70至80歲),極年輕(50歲或更年輕)的感染HIV之病患)之逆轉。在某一實施例中,存在一種延長個體壽命之方法。在特定實施例中,個體為至少50歲、55歲、60歲、65歲、70歲、75歲、80歲、85歲、90歲或95歲。在本發明之某些實施例中,經提供有效量之甘胺酸及n-乙醯半胱胺酸之個體的壽命得以延長。因此,在本發明之特定實施例中,存在與延長個體壽命相關之方法及組合物。個體可患有或可不患有危及生命之醫學病況。在失重(諸如經歷零重力之個體)的狀況下,可能存在肌肉萎縮及/或骨質減少等。
在某些實施例中,存在個體認知功能之改善,包括不患有可偵測之認知功能障礙的個體或患有可偵測之認知功能障礙的個體(包括歸於任何原因之障礙)之認知功能改善。在特定實施例中,該等方法允許延緩認知功能障礙之發作或強化正常認知功能。認知功能可定義為認識之心理過程,包括諸如意識、感覺、推理及判斷等方面,包括
(但不限於)如經由感覺、推理或直覺得到瞭解者;知識。在特定實施例中,將本文中所涵蓋之組合物提供給個體以改善記憶力,該個體包括具有正常或減退之記憶力之個體。
本發明之實施例包括改善由於任何原因(包括由於惡病質、肌肉減少症、不活動、壓力(包括手術後、敗血症後及創傷後)等)引起之骨胳肌損失的方法。該改善可為肌肉損失之速率或量的減少及/或肌肉損失之逆轉。
在一個實施例中,存在用於預防或治療至少例如經歷對比研究或程序或者患有糖尿病及/或HIV之之腎病的防治。腎病可為對腎臟之損害或腎臟疾病,且腎病可為非發炎性的或發炎性的。腎病之實例包括腎小球中IgA抗體之沈積、鎮痛劑之投與、黃嘌呤氧化酶不足、化學治療藥劑或其他藥物之毒性、長期暴露於鉛或其鹽;全身性紅斑性狼瘡症、創傷、阻塞後尿路病、腎炎;腎病症候群;導致糖尿病性腎病及高血壓性腎病之糖尿病及高血壓(high blood pressure/hypertension)。
在本發明之某些實施例中,本發明係關於與使用甘胺酸及n-乙醯半胱胺酸(NAC)治療及/或預防有需要哺乳動物之適應症相關之組合物及方法。哺乳動物可為任何種類且可包括例如人類、狗、貓、馬、豬、綿羊及山羊。在某些實施例中,本發明係針對涉及哺乳動物之穀胱甘肽轉換受損及/或氧化壓力增加及/或氧化劑損害(包括在衰老或糖尿病情況下之此類穀胱甘肽轉換受損及/或氧化壓力增加及/或氧化劑損害)之一或多種方法及/或組合物。在特定實施例中,本發明係關於具有甘胺酸及n-乙醯半胱胺酸之食物(包括至少膳食補充劑)對有需要之哺乳動物(包括例如衰老或患有糖尿病之哺乳動物)的有益作用。
有需要之哺乳動物可包括需要預防或治療衰老之不利影響、或需要預防或治療糖尿病或由糖尿病引起之併發症、或需要預防或治療
以下一或多者的哺乳動物:血脂異常;胰島素抗性;肥胖症;脂肪酸氧化;糖尿病性血脂異常;糖尿病性微血管併發症(例如,腎病、視網膜病變及/或神經病變);高膽固醇及/或三酸甘油酯含量;脂肪肝疾病;衰老過程中之神經退化性疾病;斯達汀(statin)誘發性肌病。
在一些實施例中,本發明係關於出於任何原因,包括因為合成減少,且在某些實施例中因為例如前驅體胺基酸之不良可用性引起的合成減少而GSH含量降低的個體,例如老年人。低GSH狀態傾向於使個體之氧化壓力增加,如例如藉由氧化損害之血漿標記物所量測。在本發明之某些實施例中,補充NAC及甘胺酸兩者使GSH合成及濃度得到改善,且減少損害之血漿標記物,且在特定態樣中,NAC及甘胺酸之功能性衍生物係有效的。經由增加合成引起的GSH改善可影響至少對代謝健康(包括粒線體燃料代謝、胰島素抗性、身體組成及肌肉強度)之改善。此可藉由以不同形式及前驅體(至少包括N-乙醯半胱胺酸(NAC)、L-甘胺酸、L-甘胺酸乙酯及二肽形式,例如半胱胺醯甘胺酸或n-乙醯半胱胺醯甘胺酸)投與前驅體半胱胺酸及甘胺酸以增加其可用性來實現。在某些實施例中,補充NAC及/或甘胺酸使得至少代謝健康(包括粒線體燃料代謝、胰島素抗性、身體組成及肌肉強度)得到改善,且此改善之發生與GSH無關。
在本發明之一個實施例中,存在可用於減小及/或預防個體之氧化壓力之方法及組合物。在特定實施例中,該等方法及組合物可用於治療及/或預防與氧化壓力相關之醫學病況。在特定實施例中,本發明之方法及組合物可用於治療及/或預防與穀胱甘肽含量減少相關之醫學病況。在本發明之一個特定實施例中,該等方法及組合物可用於治療糖尿病。在本發明之某一態樣中,該等方法及組合物可用於提供給老年人。在特定實例中,本發明提供可用於衰老之方法及組合物。
在某些實施例中,本發明係關於組合物及以下例示性方法:減
小血漿F2-異***素含量之方法;減小血漿F3-異***素及/或F2-異***素含量及/或神經***素(neuroprostane)及/或F4-異***素含量(例如,因為其與腦氧化壓力之標記物有關)之方法;增加GSH產量之方法;增加細胞內GSH濃度之方法;增加肝(且單獨地,例如肌肉)GSH含量之方法;改善胰島素敏感性之方法;增加脂肪氧化之方法;減少體重之方法;治療/預防血脂異常之方法;治療/預防脂肪肝疾病及/或降低肝中過量脂肪含量之方法;減少膽固醇含量之方法;預防肌病(包括斯達汀誘發性肌病)之方法;及/或降低三酸甘油酯含量之方法。
在本發明之一個實施例中,存在主要由甘胺酸及N-乙醯半胱胺酸組成之組合物。在本發明之另一實施例中,存在由甘胺酸及n-乙醯半胱胺酸組成之組合物。
在某些態樣中,存在增加個體中GSH產量之方法,該方法包含向個體提供有效量之甘胺酸及n-乙醯半胱胺酸之步驟。
在本發明之某些實施例中,因為衰老與脂肪氧化減少及肥胖,以及由合成減少引起之穀胱甘肽不足相關聯,所以提供甘胺酸及n-乙醯半胱胺酸恢復穀胱甘肽合成及濃度,且亦改善脂肪氧化、胰島素抗性、肥胖及/或血脂異常。
在特定實施例中,存在一種使用本發明中所涵蓋之組合物來預防及/或治療由酒精攝入引起之宿醉的方法。在特定實施例中,宿醉可直接或間接由GSH儲存耗盡或由乙醛與GSH及/或半胱胺酸相互作用導致其耗盡引起。在一些實施例中,宿醉直接或間接由同類物過量引起,該等同類物包括多種物質,諸如胺、丙酮、乙醛、組胺及鞣酸,且特別是有毒的物質。酒精可為任何種類,包括烈酒(濃或淡烈酒)、啤酒及/或葡萄酒。在特定實施例中,細胞健康的穀胱甘肽含量之恢復防止氧化壓力,抵消乙醛之作用,且防止宿醉或降低其有害影
響。
在特定實施例中,存在使用本文所涵蓋之組合物預防及/或治療個體之多囊卵巢症候群(PCOS)的方法。在特定實施例中,該方法藉由增加雄激素產量以干擾卵巢***能力來直接地或間接地解決影響卵巢之過量胰島素(由任何原因引起)。在一些實施例中,用於預防及/或治療PCOS之方法解決了刺激多囊卵巢產生雄激素之低級炎症。
在特定實施例中,在疫苗接種之後,向個體提供有效量之甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物以提高免疫力。在特定實施例中,在沒有提供甘胺酸(或其功能性衍生物)及N-乙醯半胱胺酸(或其功能性衍生物)之情況下,當給予個體組合物時,與提供疫苗相比,疫苗接種將引起免疫力的降低。在特定實施例中,使用甘胺酸/NAC校正穀胱甘肽允許提高成功接種疫苗之機會,尤其對於固有免疫細胞具有不良功能之彼等人群(諸如老年人及感染HIV之病患之免疫衰老人群)。該等人群中之疫苗失效率通常較高,且在特定實施例中,甘胺酸/NAC克服此等不足。在特定實施例中,在給予疫苗之前、在給予疫苗的同時及/或在給予疫苗之後向個體給予甘胺酸/NAC。在特定實施例中,個體在給予疫苗之前大約數月、數週或數天接受甘胺酸/NAC。在某些情況下,在給予疫苗之前,將甘胺酸/NAC給予個體,持續1週、2週、3週或4週。在某些實施例中,個體在給予疫苗之後大約數月、數週或數天接受甘胺酸/NAC。在特定實施例中,在給予疫苗之後,將甘胺酸/NAC給予個體,持續1週、2週、3週或4週。在某些實施例中,存在藉由提供有效量之甘胺酸及/或NAC(或其功能性衍生物)來治療個體之聽覺喪失或預防易感個體之聽覺喪失的方法。在特定實施例中,歸因於衰老、喧鬧的雜訊、頭部創傷、感染、疾病、遺傳病況、畸形、其組合等,個體易受聽覺喪失影響。聽覺喪失可為部分或完全的,且可影響一隻或兩隻耳朵。
在某些實施例中,存在用於在有需要之個體中治療創傷性腦損傷(TBI--由TBI引起之急性及慢性病況)及/或震盪或預防創傷性腦損傷(TBI--由TBI引起之急性及慢性病況)及/或震盪之方法。TBI或震盪可為事故、創傷等之結果。在該方法之特定實施例中,在TBI及/或震盪發作之前及/或在其發作之後向個體提供有效量的甘胺酸及/或NAC(或其功能性衍生物)。
在特定實施例中,藉由提供有效量的甘胺酸及/或NAC(或其功能性衍生物)來治療或預防個體之耳毒性(例如,由藥物,例如抗生素、胺基醣苷類、亨氏環利尿劑、鉑基化學治療劑(諸如順鉑)、非類固醇消炎藥引起)、耳鳴、眩暈、頭暈及/或梅尼爾氏病(Meniere's Disease)。在無甘胺酸及/或NAC(或其功能性衍生物)情況下,該病況可為可逆且暫時性的或為不可逆且永久性的。
在某些實施例中,本發明之組合物有益於肝中之脂質代謝。益處可源於穀胱甘肽、n-乙醯半胱胺酸及/或甘胺酸,且在特定實施例中,該等組分中之每一者可單獨地及/或共同地作用。
在本發明之實施例中,將該等方法及/或組合物用於任何哺乳動物,包括人類、馬、狗、貓、山羊、綿羊、牛、豬等中。
在一個實施例中,存在一種治療個體之一或多種醫學病況或身體狀況的方法,該方法包含向個體提供有效量之組合物的步驟,該組合物包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物,其中該醫學病況或身體狀況係選自由以下組成之群:(a)肌肉損失;(b)失重之有害影響;(c)器官損害;(d)心臟功能或衰竭;(e)癌症預防;(f)用於預防日後發展肥胖症及/或糖尿病之胎兒代謝程式化;(g)妊娠期糖尿病中之母體及胎兒的健康狀況;(h)運動能力及身體機能;(i)肥胖症;(j)壽命;(k)肝毒性;(l)神經退化性疾病;(m)腎病之防治;(n)預防乙醯胺苯酚毒性;(o)非酒精性脂肪變性肝炎(NASH);
(p)酒精宿醉;(q)聽覺障礙;(r)阿茲海默氏病;(s)帕金森氏病;(t)骨質疏鬆;(u)高血壓;(v)多囊卵巢症候群(PCOS);(w)動脈粥樣硬化;(x)冠狀動脈疾病;(y)壓力後之心肌損害;(z)疫苗接種後之免疫力不足;(aa)囊腫性纖維化;(bb)創傷性腦損傷;(cc)震盪;(dd)耳毒性;(ee)耳鳴;(ff)眩暈;(gg)頭暈;(hh)梅尼爾氏病;(ii)創傷後恢復及存活;(jj)非酒精性脂肪肝病(NAFLD);(kk)神經認知功能;以及(ll)其組合。
在特定實施例中,甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物係以相同組合物或不同組合物提供給個體。甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物可經口提供給個體。
在特定實施例中,甘胺酸衍生物係選自由以下組成之群:D-烯丙基甘胺酸;N-[雙(甲硫基)亞甲基]甘胺酸甲酯;Boc-烯丙基-Gly-OH(二環己基銨)鹽;Boc-D-Chg-OH;Boc-Chg-OH;(R)-N-Boc-(2'-氯苯基)甘胺酸;Boc-L-環丙基甘胺酸;Boc-L-環丙基甘胺酸;(R)-N-Boc-4-氟苯基甘胺酸;Boc-D-炔丙基甘胺酸;Boc-(S)-3-噻吩基甘胺酸;Boc-(R)-3-噻吩基甘胺酸;D-α-環己基甘胺酸;L-α-環丙基甘胺酸;N-(2-氟苯基)-N-(甲磺醯基)甘胺酸;N-(4-氟苯基)-N-(甲磺醯基)甘胺酸;Fmoc-N-(2,4-二甲氧基苯甲基)-Gly-OH;N-(2-呋喃甲醯基)甘胺酸;L-α-新戊基甘胺酸;D-炔丙基甘胺酸;肌胺酸;Z-α-膦醯基甘胺酸三甲酯,及其混合物。甘胺酸及N-乙醯半胱胺酸可包含於二肽中,諸如N-乙醯半胱胺醯甘胺酸或半胱胺醯甘胺酸。
在一個實施例中,有一種中和或緩和個體之藥物誘發之粒線體功能不全或障礙的方法,其包含向個體提供有效量的包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物之組合物之步驟。在一個特定實施例中,藥物誘發之粒線體功能不全或障礙係由抗病毒
藥物引起,諸如其中抗病毒藥物係用於HIV或肝炎。在一個特定實施例中,該藥物為抗驚厥藥;精神科藥物(抗抑鬱劑;抗精神病藥;巴比妥酸鹽(Barbiturate);焦慮症藥劑);膽固醇藥劑;鎮痛/消炎藥物;抗生素;抗心律不整藥物;類固醇;抗病毒藥物;抗反轉錄病毒藥物;癌症藥劑;糖尿病藥劑;β-阻斷劑;或為免疫接種。該藥物可為丙戊酸鹽(帝拔癲(Depakote));阿米曲替林(Amitriptyline)(依拉維(Elavil));阿莫沙平(Amoxapine);氟西汀(Fluoxetine)(百憂解(Prozac));西它普蘭(Citalopram)(喜普妙(Cipramil));氯丙嗪(Chlorpromazine)(托拉靈(Thorazine));氟非那嗪(Fluphenazine)(氟奮乃靜(Prolixin));氟哌啶醇(Haloperidol)(好度(Haldol));利培酮(Resperidone)(理思必妥(Risperdol));***(Phenobarbital);司可巴比妥(Secobarbital)(速可眠(Seconal));布他比妥(Butalbital)(非歐諾(Fiornal));異戊巴比妥(Ambarbital)(安密妥(Amytal));戊巴比妥(Pentobarbital)(寧必妥(Nembutal));阿普唑侖(Alprazolam)(贊安諾(Xanax));二氮平(Diazepam)(煩寧(Valium)、***(Diastat));斯達汀(Statins);膽酸-消膽胺(cholestyramine);環丙貝特(Ciprofibrate);ASA(阿司匹林(Aspirin));乙醯胺苯酚(泰諾(Tylenol));吲哚美辛(Indomethacin)(消炎痛(Indocin));甲氧萘丙酸(Naproxen)(萘普生(Aleve));雙氯芬酸(Diclofenac);四環素、米諾環素(minocycline);氯黴素(Chloramphenical);胺基醣苷類;利奈唑胺(Linezolid)(彩福適(Zyvox));胺碘酮(Amiodarone);干擾素;齊多夫定(Zidovudine);阿黴素(Doxorubicine)(阿德力黴素(Adriamycin));順鉑;他莫昔芬(Tamoxifen);二甲雙胍(Metformin);或其混合物。
前文已相當廣泛地概述本發明之特徵及技術優勢,以便能更好地理解以下本發明之詳細描述。本發明之其他特徵及優勢將在下文進行描述,其形成本發明之申請專利範圍之主題。應瞭解,本發明之概
念及特定實施例可易於用作修改或設計實現本發明之相同目的之其他結構的基礎。亦應意識到,此類等效結構並未脫離如所附申請專利範圍中所闡述之發明。當結合附圖考慮時,自以下描述將更好地理解咸信為本發明所特有的關於組織及操作方法之新穎特徵,以及其他目標及優勢。然而,應清楚地理解,各附圖僅出於說明及描述之目的而提供,且不意圖限定本發明之界限。
為了更全面地理解本發明,現結合附圖論及以下描述。
圖1說明穀胱甘肽不足與某些身體狀況之間的例示性關係。
圖2展示相比於對照組,老年HIV病患中GSH之分數合成率。
圖3顯示相比於對照組,老年HIV病患之GSH濃度。
圖4展示相比於對照組,老年HIV病患之空腹燃料氧化。
圖5顯示老年HIV病患在口服補充N-乙醯半胱胺酸及甘胺酸之前及之後的C反應蛋白含量。
圖6展示接受N-乙醯半胱胺酸及甘胺酸之小鼠的壽命。
如本說明書中所使用,「一個(種)(a/an)」可意謂一或多個(種)。當與詞語「包含」結合使用時,如本文在申請專利範圍中所使用,詞語「一個(種)(a/an)」可意謂一或多個(種)。如本文中所使用,「另一個(種)」可意謂至少第二個(種)或更多個(種)。
如本文中所使用,術語「糖尿病之併發症」在特定實施例中係指例如糖尿病性腎病、神經病變、視網膜病變、糖尿病性肥胖症、糖尿病性血脂異常、心血管代謝症候群及其組合。
如本文所使用,術語「有效量」係指改善個體之醫學病況之至少一種症狀所需要的甘胺酸及n-乙醯半胱胺酸(或其功能性衍生物)的
量;在特定實施例中,醫學病況直接地或間接地因為穀胱甘肽含量不足而出現在個體中。在特定實施例中,有效量係指用以增加個體中穀胱甘肽含量之甘胺酸及n-乙醯半胱胺酸的量。
如本文所使用,術語「年老的」係指年齡在至少60歲以上之個體。
如本文所使用,術語「氧化壓力」係指個體或個體之細胞或組織中活性氧物質之產生與使活性中間物解毒或容易地修復生物系統中所造成之損害之能力之間的不平衡狀態。藉由使用持續輸入代謝能量之方法來維持細胞內的天然還原環境,且此正常氧化還原狀態之擾亂可經由產生例如損害諸如蛋白質、脂質及/或DNA之細胞組分的自由基及過氧化物而產生有毒作用。
本發明之實施例包括增加半胱胺酸及甘胺酸(例如,半胱胺醯甘胺酸)之血液含量以增加細胞內GSH、半胱胺酸及/或甘胺酸含量及/或減少CRP含量之方法。在一些實施例中,作用機制涉及半胱胺酸及/或甘胺酸但與GSH無關。
在本發明之某些實施例中,存在用於治療直接或間接由個體中GSH含量不足引起之醫學病況的方法及組合物。該個體可為任何年齡或健康狀況,但在特定實施例中,該個體為年老的,易受直接或間接與GSH含量不足相關聯之特定醫學病況或身體狀況影響,或具有直接或間接與GSH含量不足相關聯之醫學病況或身體狀況。在此狀況下,遞送至個體之組合物至少包括甘胺酸及n-乙醯半胱胺酸,尤其作為前驅體胺基酸以促進個體中穀胱甘肽含量升高。舉例而言,可量測紅血球GSH或肌肉活組織檢查來量測細胞內GSH含量。細胞內GSH量測分析法為此項技術中已知的(Rahman等人,2007)。
在特定實施例中,直接或間接由半胱胺酸、甘胺酸及/或GSH含
量減少引起之一或多種醫學病況可使用有效量之甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物來進行治療或預防。在特定實施例中,該醫學病況或身體狀況為以下一或多種:(a)肌肉損失;(b)失重之有害影響;(c)器官損害;(d)心臟功能或衰竭;(e)癌症預防;(f)用於預防日後發展肥胖症及/或糖尿病之胎兒代謝程式化;(g)妊娠期糖尿病中之母體及胎兒的健康狀況;(h)運動能力及身體機能;(i)肥胖症;(j)壽命;(k)肝毒性;(l)神經退化性疾病;(m)腎病之防治;(n)預防乙醯胺苯酚毒性;(o)非酒精性脂肪變性肝炎;(p)酒精宿醉;(q)聽覺障礙;(r)阿茲海默氏病;(s)帕金森氏病;(t)骨質疏鬆;(u)高血壓;(v)多囊卵巢症候群(PCOS);(w)動脈粥樣硬化;(x)冠狀動脈疾病;(y)壓力後之心肌損害;(z)疫苗接種後之免疫力不足;(aa)囊腫性纖維化;(bb)創傷性腦損傷;(cc)震盪;(dd)耳毒性;(ee)耳鳴;(ff)眩暈;(gg)頭暈;(hh)梅尼爾氏病;(ii)創傷後(例如,手術後、敗血症後或歸因於事故或身體攻擊之鈍挫傷或穿透傷後等)恢復及存活;(jj)非酒精性脂肪肝疾病(NAFLD);以及(kk)其組合。個體可被診斷患有該(等)病況,或可被懷疑患有該(等)病況,或可易患上該(等)病況。可使用除本發明之方法外的一或多種其他療法來治療該個體。
在特定實施例中,出於提高GSH、半胱胺酸及/或甘胺酸之細胞內含量的明確目的,且由於確定個體罹患直接或間接與該等含量相關之病況,向個體提供有效量的如本文中所描述之組合物。在特定情況下,本發明之方法包括該(等)醫學病況之診斷。
在特定實施例中,本發明係針對用於治療、預防直接或間接與細胞內GSH含量減少相關之醫學病況或身體狀況,或延緩其發作之醫藥組合物。在特定實施例中,該等組合物由或基本上由甘胺酸(或其
功能性衍生物)及N-乙醯半胱胺酸(或其功能性衍生物)組成,或包含甘胺酸(或其功能性衍生物)及N-乙醯半胱胺酸(或其功能性衍生物)。甘胺酸之功能性衍生物定義為本身或與N-乙醯半胱胺酸(或其功能性衍生物)結合以在個體中有效增加細胞內GSH含量之甘胺酸衍生物。N-乙醯半胱胺酸之功能性衍生物定義為本身或與甘胺酸(或其功能性衍生物)結合以在個體中有效增加細胞內GSH含量之N-乙醯半胱胺酸衍生物。在特定實施例中,可使用「半胱胺酸」衍生物,亦即,其本身或與甘胺酸結合而對個體有效的半胱胺酸之功能性衍生物。
甘胺酸組分及N-乙醯半胱胺酸組分可一起或單獨地提供。在特定實施例中,該組合物包含N-乙醯半胱胺醯甘胺酸;半胱胺醯甘胺酸及其所有形式,例如L-半胱胺醯甘胺酸;等等。甘胺酸衍生物之實例至少包括D-烯丙基甘胺酸;N-[雙(甲硫基)亞甲基]甘胺酸甲酯;Boc-烯丙基-Gly-OH(二環己基銨)鹽;Boc-D-Chg-OH;Boc-Chg-OH;(R)-N-Boc-(2'-氯苯基)甘胺酸;Boc-L-環丙基甘胺酸;Boc-L-環丙基甘胺酸;(R)-N-Boc-4-氟苯基甘胺酸;Boc-D-炔丙基甘胺酸;Boc-(S)-3-噻吩基甘胺酸;Boc-(R)-3-噻吩基甘胺酸;D-α-環己基甘胺酸;L-α-環丙基甘胺酸;N-(2-氟苯基)-N-(甲磺醯基)甘胺酸;N-(4-氟苯基)-N-(甲磺醯基)甘胺酸;Fmoc-N-(2,4-二甲氧基苯甲基)-Gly-OH;N-(2-呋喃甲醯基)甘胺酸;L-α-新戊基甘胺酸;D-炔丙基甘胺酸;肌胺酸;Z-α-膦醯基甘胺酸三甲酯;等等。
在特定實施例中,該等醫藥組合物包含N-乙醯半胱胺酸(NAC)、L-甘胺酸、L-甘胺酸乙酯,及/或二肽形式,例如半胱胺醯甘胺酸。
在特定實施例中,在特定時間段內,甘胺酸係以1.33mmol/kg/d投與且NAC係以0.83mmol/kg/d投與。舉例而言,治療持續時間可持續一或多天、1週、2週、3週、一個月、兩個月、三個月、四個月、五個月、六個月、一年、兩年、五年、十年、十五年、二十年、二十
五年、三十年等。在某些情況下,治療持續個體之餘生。在特定實施例中,投藥直至醫學病況無可偵測之症狀殘留。在特定實施例中,投藥直到至少一種症狀發生可偵測之改善,且在其他情況下,持續投藥以保持改善。
在本發明係關於使用本發明之化合物進行治療之情況下,視需要,可經由任何可接受之投藥模式,在合適醫藥賦形劑存在下投與本發明之化合物。視需要,該等化合物可包含於醫藥學上可接受的賦形劑中,該賦形劑可被視作在投與動物時不會產生不良反應、過敏反應及/或其他不當反應之分子實體及/或組合物。其包括任何及/或所有溶劑、分散介質、包衣、抗細菌劑及/或抗真菌劑、等張劑及/或吸收延遲劑,及/或其類似物。此類介質及/或試劑用於醫藥活性物質之用途係此項技術中熟知的。除非任何習知介質及/或試劑與活性成分不相容,否則考慮將其用於治療性組合物中。
因此,投藥可例如經靜脈內、局部、皮下、經皮、肌內、經口、關節內、非經腸、腹膜、鼻內、膀胱內或藉由吸入進行。因此,適合的投藥部位包括(但不限於)皮膚、支氣管、腸胃、肛門、***、眼、膀胱以及耳。調配物可呈固體、半固體、冷凍粉或液體劑型之形式,諸如錠劑、丸劑、膠囊、粉劑、溶液、懸浮液、乳液、栓劑、保留灌腸劑、乳膏、軟膏、洗劑、氣霧劑或其類似物,較佳地為適合於簡單地投與精確劑量之單位劑型。
該等組合物通常包括習知的醫藥載劑或賦形劑且可另外包括其他藥劑、載劑、佐劑及其類似物。較佳地,該等組合物將為約5重量%至75重量%一或多種本發明之化合物,且剩餘部分由合適的醫藥賦形劑組成。適當的賦形劑可藉由此項技術中熟知之方法,針對特定組成及投藥途徑定製,例如,REMINGTON'S PHARMACEUTICAL SCIENCES,第18版,Mack Publishing Co.,Easton,Pa.(1990)。
對於經口投藥,該等賦形劑包括醫藥級甘露醇、乳糖、澱粉、硬脂酸鎂、糖精鈉、滑石、纖維素、葡萄糖、明膠、蔗糖、碳酸鎂及其類似物。組合物可呈溶液、懸浮液、錠劑、丸劑、膠囊、粉劑、緩釋調配物之形式,及其類似形式。
在一些實施例中,醫藥組合物呈丸劑、錠劑或膠囊之形式,且因此,組合物除生物活性綴合物之外,亦可含有以下任一者:稀釋劑,諸如乳糖、蔗糖、磷酸二鈣及其類似物;崩解劑,諸如澱粉或其衍生物;潤滑劑,諸如硬脂酸鎂及其類似物;以及黏合劑,諸如澱粉、***膠、聚乙烯吡咯啶酮、明膠、纖維素及其衍生物。
配方中之活性化合物可調配成栓劑,該栓劑包含例如約0.5%至約50%之本發明化合物安置於聚乙二醇(PEG)載劑(例如,PEG 1000[96%]及PEG 4000[4%])中。
可藉由將化合物(約0.5%至約20%)及視情況選用之醫藥佐劑溶解或分散於載劑,諸如生理鹽水溶液(例如,0.9%w/v氯化鈉)、右旋糖水溶液、甘油、乙醇及其類似物中,以形成溶液或懸浮液(例如,用於靜脈內投藥),由此製備液體組合物。活性化合物亦可調配成保留灌腸劑。
必要時,待投與之組合物亦可含有微量無毒輔助物質,諸如潤濕劑或乳化劑、pH緩衝劑(諸如醋酸鈉、脫水山梨醇單月桂酸酯或三乙醇胺油酸酯)。
對於局部投藥,組合物係以任何合適的形式投與,諸如洗劑或經皮貼片。對於藉由吸入遞送,組合物可以乾粉(例如Inhale Therapeutics)或液體形式經由噴霧器遞送。
熟習此項技術者已知或易於瞭解用於製備該等劑型之方法;例如,參見Remington's Pharmaceutical Sciences,同前述,及類似出版物。當根據本發明之教示投與時,在任何情況下,待投與之組合物均
將含有呈醫藥有效量的一定量前藥及/或一或多種活性化合物以減輕所治療之病況。
一般而言,本發明之化合物係以治療有效量(亦即,足以實現治療之劑量)投與,該有效量將取決於所治療之個體及病況而變化。通常,治療有效的日劑量為每天每公斤體重0.1mg至100mg藥物。大部分病況對每天每公斤體重在約1mg與30mg之間,或對於70kg個體在每天約70mg與2100mg之間之總投藥劑量起反應。
綴合物之穩定性可進一步藉由化學改變進行控制,該等化學改變包括多肽鏈中之D胺基酸殘基以及其他肽模擬物部分。另外,綴合物之穩定性亦可藉由非天然碳水化合物殘基增強。
甘胺酸及N-乙醯半胱胺酸組分可以特定比率進行調配。在某些實施例中,該調配物包含的組分可例如呈以下例示性比率:1:1、1:2、1:3、1:4、1:5、1:6、1:7、1:8、1:9、1:10、1:12、1:15、1:20、1:25、1:30、1:35、1:40、1:45、1:50、1:55、1:60、1:65、1:70、1:75、1:80、1:85、1:90、1:95、1:100、1:150、1:200、1:300、1:400、1:500、1:600、1:750、1:1000、1:10,000等等。在特定實施例中,調配物包含的組分可例如以調配物計呈以下百分比(各自具有相同或不同百分比):1%、2%、3%、4%、5%、6%、7%、8%、9%、10%、12%、15%、20%、25%、30%、40%、45%、50%、55%、60%、65%、70%、75%、80%、85%、90%、95%、97%或99%。
甘胺酸(或功能性衍生物)及N-乙醯半胱胺酸(或功能性衍生物)可以同一組合物或不同組合物遞送。在分別提供甘胺酸(或功能性衍生物)及N-乙醯半胱胺酸(或功能性衍生物)之實施例中,用於其分別遞送之方案可為任何合適的種類。在特定實施例中,在N-乙醯半胱胺酸之前、與N-乙醯半胱胺酸同時或在N-乙醯半胱胺酸之後,將甘胺酸提供給個體。分別遞送可涵蓋在不同時間以相同投藥途徑遞送,或可為不
同投藥途徑。
替代地,本發明之治療可以在另一治療之前、之後或兩者間隔數分鐘至數週進行。在將創造性組合物與另一藥劑分別提供給個體的實施例中,通常應確保在每一次遞送之時間之間未經過較長時間段,以使得創造性組合物及另一藥劑仍能夠對細胞發揮有利的組合作用。在此等情況下,預期可在彼此間隔約12小時至24小時內,更佳在彼此間隔約6小時至12小時內遞送兩種形式。然而,在一些情況下,可能需要顯著地延長治療時段,其中各別投藥之間相差若干天(2天、3天、4天、5天、6天或7天)至若干週(1週、2週、3週、4週、5週、6週、7週或8週)。
可使用各種組合,例如,其中本發明之治療為「A」,且用於如本文所描述之本發明之醫學病況,諸如糖尿病治療(僅舉例而言)的第二藥劑為「B」:
考慮到分子之毒性(若存在),將遵循用於藥物投與之通用方案向病患投與本發明之創造性組合物。預期視需要將重複治療週期。亦預期各種標準療法以及手術干預可與所描述之療法組合應用。
與本發明之組合物相關的治療套組構成本發明之另一態樣。該等套組通常將在合適的容器構件中含有本發明之創造性組合物。該套組可具有含有創造性組合物之單一容器構件,或其可具有用於創造性組合物及可包括在該等套組內之其他試劑的不同容器構件。
套組中之組分可以一或多種液體溶液或一或多種乾粉形式提
供。當以液體溶液形式提供該等組分時,該液體溶液為水性溶液或非水性溶液,其中無菌水性溶液或非水係溶液尤佳。當試劑或組分係以乾粉形式提供時,該粉末可藉由添加合適溶劑而復原。設想溶劑亦可提供在另一容器構件中。
容器構件通常將包括至少一個小瓶、試管、燒瓶、瓶、注射器,或可將組合物置放於其中且較佳地適當等分該組合物的其他容器構件。在提供第二藥劑的情況下,套組通常將另含有第二小瓶或可將此藥劑置放於其中的其他容器。本發明之套組通常亦包括用於容納緊密限制之該等藥劑容器之構件以用於商業銷售。該等容器可包括例如將所需小瓶保持在其中之射出模製或吹塑模製之塑料容器。
在本發明之套組中,甘胺酸(或其功能性衍生物)及N-乙醯半胱胺酸(或其功能性衍生物)可分別提供或以混合物一起提供。
包括以下實例以顯示本發明之較佳實施例。熟習此項技術者應瞭解,以下實例中所揭示之技術呈現本發明人發現的較佳用於實施本發明的技術,且因此可視為構成其較佳實施方式。然而,根據本發明,熟習此項技術者應瞭解,在不背離本發明之精神及範疇的情況下可對所揭示之特定實施例作出許多改變且仍獲得相同或類似結果。
老年人超重或發展肥胖症之風險最高。加之在此人群中肌肉質量之佔有率減小,老年人發展『肌肉減少性肥胖症』表型,伴隨肌肉強度降低及生活品質降低,但尚未充分瞭解其潛在機制且缺乏有效治療。在人類及嚙齒動物中進行之轉化研究已發現,在衰老過程中含量最豐富之內源性抗氧化劑穀胱甘肽(GSH)的不足與粒線體功能不全有關,且在一些實施例中,此提供了有關老年人肌肉減少性肥胖症發展
之機制解釋。老年人GSH不足係由其前驅體胺基酸半胱胺酸及甘胺酸之有限可用性導致合成減少而引起。短期補充此等胺基酸足以校正其自身不足,且亦足以恢復細胞內GSH合成及濃度。與空腹的健康年輕人對照組相比,GSH不足之老年人在空腹時粒線體脂肪酸氧化嚴重減少(此可促進脂肪儲存)且碳水化合物氧化增加(此可促成肌肉損耗)。因為在空腹狀態下粒線體燃料優先選擇脂肪酸而非葡萄糖,所以此在空腹燃料優先選擇中之異常反轉表明粒線體能量之減弱。有趣地是,該等老年人經2週半胱胺酸及甘胺酸前驅體補充而恢復GSH合成,使得空腹粒線體脂肪酸及碳水化合物氧化完全恢復至在年輕人對照組中所見之水準。基於該等資料,認為粒線體脂肪酸氧化減少迫使燃料氧化轉變成葡萄糖以滿足能量需求。因為在空腹狀態下,葡萄糖係由葡萄糖新生(其中肌肉蛋白為重要貢獻者)提供,所以此將導致肌肉蛋白質(且因此肌肉質量)之損失,以及半胱胺酸及甘胺酸(已知的葡萄糖新生胺基酸)之不足,從而進一步加大GSH之不足。肌肉質量之損失又將導致肌肉強度減弱。補充半胱胺酸及甘胺酸可校正GSH之不足且破壞此下降(negative spiral)以校正粒線體脂肪酸氧化(且因此降低總體脂肪),降低碳水化合物氧化(且因此避免肌肉蛋白損失以增加瘦體重)且增加肌肉強度。對於此考慮之支持來自在經歷生物學衰老之HIV病患中之研究,其中用半胱胺酸及甘胺酸補充(以與老年人研究相同之劑量及持續時間使用)來改善GSH不足係與空腹粒線體燃料氧化之恢復、總體脂肪質量減少3.5lb、瘦體重增加1.9lh及在2週時間內在慣用手及非慣用手肌肉強度之顯著增加相關。
肌肉減少症為與衰老相關之骨胳肌質量、品質及強度的退化性損失。肌肉減少症亦可繼發於不使用及零重力或失重。惡病質係以體
重減輕、肌肉萎縮無力及疲乏為特徵且伴隨一系列慢性疾病,包括癌症、HIVAIDS、COPD、退化性神經病症(諸如多發性硬化)、充血性心臟病、肺結核及腎病的複雜代謝消耗症候群。肌肉減少症可伴隨脂肪質量之增加(亦即肌肉減少性肥胖症),且惡病質可伴隨或不伴隨脂肪質量之減少。
該等病況代表藉由提供半胱胺酸加甘胺酸以提高哺乳動物細胞內GSH且改善肌肉健康來預防及治療的原則目標。在感染HIV之老年病患中,藉由投與GSH前驅體半胱胺酸及甘胺酸來改善GSH與粒線體燃料氧化之生理模式改善、較低之總體脂肪、腰圍及胰島素抗性,及較高去脂體重及肌肉強度相關,表明該方法可預防及逆轉肌肉減少症、肌肉減少性肥胖症及惡病質。
多種藥物誘導粒線體毒性及/或肝毒性,包括例如乙醯胺苯酚及抗反轉錄病毒劑。引起粒線體毒性之某些藥物至少包括抗驚厥藥、精神科藥物(抗抑鬱劑、抗精神病藥、巴比妥酸鹽及焦慮症藥劑)、膽固醇藥劑、鎮痛/消炎藥物、抗生素、抗心律不整藥、類固醇、抗病毒藥劑、抗反轉錄病毒藥劑、癌症藥劑、糖尿病藥劑、β-阻斷劑及免疫接種。特定藥物包括丙戊酸鹽、阿米曲替林、阿莫沙平、氟西汀、西它普蘭、氯丙嗪、氟非那嗪、氟哌啶醇、利培酮、***、司可巴比妥、布他比妥、異戊巴比妥、戊巴比妥、阿普唑侖、二氮平、斯達汀、膽酸-消膽胺、環丙貝特、非諾貝特(fenofibrate)、阿司匹林、乙醯胺苯酚、吲哚美辛、萘普生、雙氯芬酸、四環素、米諾環素、氯黴素、替諾福韋(tenofovir)、地瑞那韋(darunavir)、利巴韋林(ribavirin)、特拉匹韋(telaprevir)、胺基醣苷類、利奈唑胺、胺碘酮、干擾素、齊多夫定、阿黴素、順鉑、他莫昔芬及二甲雙胍。
在特定實施例中,將NAC及/或甘胺酸提供給個體以預防、治療或減小粒線體毒性及/或肝毒性之不利影響。在特定實施例中,使用本發明之方法治療與氧化壓力及/或GSH不足有關的其他毒性。
在特定實施例中,存在用於預防及治療乙醯胺苯酚毒性(諸如在肝毒性之情況下)之方法。在藥物開發期間及許多現有藥物之使用中,肝毒性為嚴重問題。舉例而言,在美國,乙醯胺苯酚用藥過量為當前引起急性肝衰竭之最常見病因。肝粒線體為藥物毒性之重要目標,此係直接或間接經由反應性代謝物之形成引起。乙醯胺苯酚(泰諾、撲熱息痛(paracetamol)、N-乙醯基-對胺基苯酚;APAP)係廣泛使用的非處方鎮痛劑及解熱劑。其亦常與多種處方***中之氫可酮(hydrocodone)、丙氧吩(propoxyphene)、可待因(codeine)及羥考酮(oxycodone)組合使用。在治療劑量下,乙醯胺苯酚具有類似於阿司匹林及布洛芬之鎮痛及解熱作用,但其具有很窄的治療窗。乙醯胺苯酚為引起急性肝衰竭之主要原因,即使劑量在所建議之範圍內。其引起每年對中毒控制中心及醫院入院之數萬次呼叫,以及數百例死亡。飲酒及禁食(由疾病、食慾不振或營養不良引起)大大提高由乙醯胺苯酚引起之肝損傷之風險。
諸如老年、飲酒及禁食(由例如疾病、食慾不振或營養不良引起)之情形且甚至乙醯胺苯酚之代謝物自身藉由減少穀胱甘肽(一種幫助肝解除乙醯胺苯酚毒性的抗氧化劑)之含量而大大提高肝損傷之風險。即使在標準劑量下,乙醯胺苯酚在人體中之代謝亦釋放少量有毒物質,即N-乙醯基-苯醌亞胺(或NAPQI)。在過量劑量下,形成更大量之此毒素。在乙醯胺苯酚之安全劑量與危險劑量之間存在精細的界限,此意謂劑量即使略微高於4公克/天之最大建議劑量亦會引起肝損傷。
在肝中使用最佳的細胞內穀胱甘肽濃度係針對乙醯胺苯酚毒性
之合理預防及治療方法。投與N-乙醯半胱胺酸經由其維持肝中穀胱甘肽儲量之能力而被用作由乙醯胺苯酚用藥過量引起之肝毒性之主要治療方法。在特定實施例中,在乙醯胺苯酚之前、之時及/或之後使用NAC/甘胺酸提高肝GSH含量減輕乙醯胺苯酚之有毒作用,甚至是在規定量下。
本發明之方法及/或組合物可提供給個體以藉由增強運動之作用,自劇烈運動恢復,或逆轉在其他年輕、身體健康個體(諸如宇航員(零重力)、馬拉松選手、消防員、優秀運動員等)中由加速衰老及肌肉損失之非疾病狀況引起之瘦肌肉質量損失來改善體能,預防肌肉質量損失。此外,持久活動尤其會增加氧化壓力,此在細胞內GSH已經不足之老年運動員中特別值得關注。因此,在特定實施例中,本發明之方法預防及/或治療運動之氧化壓力。
在老齡小鼠之飼料中補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸足以提高抗氧化劑穀胱甘肽之含量。在該等老齡小鼠中穀胱甘肽之恢復使得粒線體燃料氧化顯著改善。因為該等有益變化可用於影響壽命,所以測試在小鼠飼料中補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸是否延長其壽命。該研究如下進行:60週齡小鼠分2組(7隻小鼠,每組有2隻雌性小鼠及5隻雄性小鼠)進行研究,且兩組在性別、年齡及重量上均匹配。使一組任意進食常規餵料,而第二組餵食額外含有半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸之飲食。然而,兩種飲食之飼料成分匹配以使得其每公克飼料中具有相同量的卡路里及蛋白氮,亦即,兩種飲食為等熱量及等氮的。監測飼料重量顯示在兩組中飼料消
耗量相似。使動物自由獲取其各別飲食及水且記錄下壽命作為主要結果量度。結果顯示,接受補充半胱胺酸及甘胺酸之飲食的小鼠平均存活超過34週,此表示壽命延長35%(圖6)。
據報導,感染HIV且年齡在50歲以上之病患與非HIV老年病患相比具有加速之功能減退及較低肌肉質量、減弱之肌肉強度及功能限制,但未完全瞭解引起此等缺陷之根本機制且缺乏有效療法。認識到此點,疾病控制中心(Center for Disease Control)已提出HIV病患之『老齡』截止點開始於50歲。
在本發明之特定實施例中,感染HIV之老年病患之功能減退與粒線體功能減弱有關。粒線體依賴於抗氧化劑來防禦活性氧物質及氧化壓力之損害。已知在HIV病患中穀胱甘肽(GSH)不足,穀胱甘肽為含量最豐富的內源性細胞內抗氧化劑及粒線體抗氧化防禦之關鍵組分。對於導致老年HIV病患中GSH不足之機制,其發生係因為由GSH兩種前驅體胺基酸,即半胱胺酸及甘胺酸之不足所引起的GSH合成嚴重減少。經口膳食補充半胱胺酸及甘胺酸兩週校正該等胺基酸之不足,增加GSH合成,改善細胞內GSH濃度且降低ROS含量及氧化損害。在生理條件下,在空腹狀態下選擇之燃料為脂肪酸(FA),而非葡萄糖。GSH不足的老年HIV病患具有嚴重減少的空腹FA氧化及較高的空腹葡萄糖氧化,從而表明粒線體缺陷。改善GSH濃度使得增加之空腹粒線體FA氧化急劇增加且使葡萄糖氧化減少。該等變化與去脂體重及肌肉強度顯著增加相關。有趣地是,當GSH含量增加時,該等病患之肌肉強度顯著增加,而在GSH不足狀態下其肌肉強度相當於80歲非HIV人群之肌肉強度,隨著GSH增加,其肌肉強度增加至70歲人群之肌肉強度。有效地,該等老年HIV病患在GSH改善之2週時間中變得『年
輕』10歲。
吾人可研究GSH不足是否導致老年HIV病患之肌肉質量、強度、功能限制及生活品質損失,且測試補充半胱胺酸及甘胺酸以校正GSH不足是否會逆轉該等缺陷。舉例而言,吾人可對年齡為50歲至60歲的10位老年HIV病患及10位非HIV對照(年齡、性別及BMI均匹配)進行開放標記研究。基於公佈的資料,需要的樣本量為8位個體且吾人可研究10位個體以計入20%的耗損。可在基線時研究所有個體,且僅HIV個體可在接受半胱胺酸加甘胺酸12週之後再次進行研究。吾人可測試與非HIV對照組相比,老年HIV病患之GSH不足是否與空腹粒線體燃料氧化減少及肌肉蛋白質損失相關,及補充半胱胺酸加甘胺酸是否可逆轉該等缺陷。
在針對老年HIV病患之特定實施例中,GSH不足導致缺乏空腹粒線體燃料氧化、提高之葡萄糖氧化及肌肉蛋白損失,且GSH恢復可逆轉該等缺陷。儘管不受理論限制,但GSH不足導致空腹粒線體NEFA氧化減少,迫使轉換為葡萄糖氧化以實現能量需求。因為在空腹狀態下葡萄糖係由主要來自肌肉蛋白之葡萄糖新生提供,此導致肌肉損失以及半胱胺酸及甘胺酸不足(圖1)。補充半胱胺酸加甘胺酸以校正GSH不足將恢復空腹粒線體FA氧化且降低葡萄糖氧化,由此減少朝向葡萄糖新生之肌肉蛋白損耗且藉此增加肌肉質量。出於此等考慮,吾人可量測肌肉GSH、半胱胺酸及甘胺酸含量(HPLC)、空腹NEFA及葡萄糖氧化(量熱法)、肌肉蛋白損耗(穩定同位素研究)、肌肉質量(DEXA,全身鉀及氮掃描)。
吾人可測試與非HIV對照組相比,老年HIV病患之GSH不足是否與肌肉質量、肌肉強度及功能降低相關,及GSH恢復是否使肌肉強度及功能恢復至相配之非HIV對照組程度。在特定實施例中,老年HIV病患之GSH不足為肌肉強度及功能損失之基礎,且GSH恢復可改善強
度及功能至相配非HIV組之程度。在此等考慮下,吾人可量測強度(諸如藉由肌力測定法測定前臂握力)及功能(諸如6分鐘步行)。
老年HIV病患具有減少的粒線體氧化以及肌肉蛋白損失,但其根本機制未知。因為預期>50%的HIV病患到2015年為老年(年齡>50歲)病患,所以由該等缺陷引起之併發症將顯著增加人類負擔及保健成本。本發明預防及逆轉老年HIV病患之肌肉損失、增加肌肉強度、改善功能及生活品質,且降低日益增加之老年HIV病患群體之保健成本。在特定實施例中,GSH不足為老年HIV病患中肌肉損失之新穎且重要的風險因素,且吾人可提供基於補充半胱胺酸加甘胺酸之療法以校正GSH不足且逆轉肌肉損失。在特定實施例中,可增加肌肉質量及力量、運動能力並改善生活品質。本發明之實施例使用半胱胺酸加甘胺酸提供新穎、簡單、安全、有效且便宜的營養策略以校正老年HIV病患之GSH不足。
在特定實施例中,在患有HIV之老年病患中,GSH不足引起空腹粒線體燃料氧化之減少,肌肉質量、強度及功能之損失,且導致功能減退加速。吾人可使用創新的基於穩定同位素示蹤劑之方案、量熱法、DXA、全身鉀及氮掃描法、肌力測定法及功能測試以量測在全身層面(NEFA及葡萄糖氧化及肌肉損失)及組織層面(肌肉GSH及蛋白質損失)上之結果。吾人顯示因為補充半胱胺酸及甘胺酸而得到益處。本發明之實施例使用半胱胺酸加甘胺酸來提供新穎、簡單、安全、有效且便宜的營養策略以校正老年HIV病患之粒線體燃料氧化之缺陷;肌肉蛋白、肌肉質量及強度之損失;以及生活品質。
HIV及GSH不足:在年輕(年齡為30歲至40歲;n=10)及老年(年齡為50歲至60歲;n=20)HIV病患中量測RBC-GSH含量且在所有病患中發現較低的GSH,但年齡與甚至更低的GSH濃度(P<0.0001)顯著相關。進一步分析顯示,55歲HIV病患具有與70歲非HIV人群類似的
GSH含量。
老年HIV病患中之GSH動力學(圖2、圖3):在8位GSH不足之老年HIV病患(約55歲)中研究補充半胱胺酸加甘胺酸作為GSH前驅體之前及之後的GSH動力學。結果與過去GSH充足之非HIV對照組(n=8)相比顯示,在藉由補充改善之老年HIV病患中存在嚴重半胱胺酸及甘胺酸細胞內不足。如所示,HIV個體在補充前具有58%的較低GSH-FSR含量及57%的較低GSH含量(與對照組相比)。補充後,GSH-FSR(其中FSR為分數合成率)及GSH含量分別增加120%及53%。
老年HIV個體中之空腹燃料氧化(圖4):在空腹16小時之後,與非HIV對照組相比,GSH不足之老年HIV個體具有顯著較低的NEFA氧化及較高的碳水化合物(CARB)氧化。恢復GSH合成使NEFA氧化增加46%且使碳水化合物氧化降低49%。(*=p<0.05;Φ=p<0.01)。
GSH改善增加去脂體重及強度:GSH改善使去脂體重有0.9kg之顯著增加(p=0.003)且使兩個前臂之肌肉強度顯著增加(p<0.01)。
因此,老年HIV病患具有GSH不足係因為合成減少(由其前驅體半胱胺酸及甘胺酸之可用性減小),且其與粒線體燃料氧化減少、肌肉質量及強度損失相關。補充半胱胺酸及甘胺酸2週使GSH含量增加。在特定實施例中,對老年HIV病患持續補充超過12週使GSH濃度完全恢復且逆轉肌肉損失及功能減退。
C反應蛋白(CRP)為在血漿中發現之急性期蛋白,且由肝合成。CRP含量響應於炎症而上升,且因此其被視作與炎症增加相關之病況的生物標記物。CRP亦經鑑別為心血管疾病之生物標記物,其含量>3μg/ml被視為不合需要,且含量<1μg/ml最佳。較高的CRP亦與糖尿病、HIV及衰老相關。降低CRP含量之干預有限。在稱為斯達汀之藥
劑種類中有效降低膽固醇的藥劑可降低CRP含量。
具有穀胱甘肽不足之老年HIV病患具有較高的CRP含量,且當使用經口膳食補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸來增加穀胱甘肽含量時,CRP含量顯著下降(p<0.05)(圖5)。
某些藥物因為其作用機制導致粒線體功能不全或障礙而引起毒性。在某些實施例中,存在藉由向個體提供有效量的組合物來中和或緩和藥物誘發之粒線體功能不全或障礙之方法,該組合物包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物。由藥物引起之毒性可屬於引起粒線體功能不全或障礙之任何類型,但在特定實施例中,該藥物為抗病毒藥物,諸如HIV藥物、肝炎藥物等。在某些實施例中,治療前或治療後的GSH耗乏亦可引起或加劇藥物毒性。
引起粒線體毒性之藥物至少包括抗驚厥藥;影響精神之藥物(抗抑鬱劑;抗精神病藥;巴比妥酸鹽;焦慮症藥劑);膽固醇藥劑;鎮痛/消炎藥物;抗生素;抗心律不整藥物;類固醇;抗病毒藥物;抗反轉錄病毒藥物;癌症藥劑;糖尿病藥劑;β-阻斷劑;以及免疫接種。
在特定情況下,該藥物為丙戊酸鹽(帝拔癲);阿米曲替林(依拉維);阿莫沙平;氟西汀(百憂解);西它普蘭(喜普妙);氯丙嗪(托拉靈);氟非那嗪(氟奮乃靜);氟哌啶醇(好度);利培酮(理思必妥);***;司可巴比妥(速可眠);布他比妥(非歐諾);異戊巴比妥(安密妥);戊巴比妥(寧必妥);阿普唑侖(贊安諾);二氮平(煩寧、***);斯達汀;膽酸-消膽胺;環丙貝特;ASA(阿司匹林);乙醯胺苯酚(泰諾);吲哚美辛(消炎痛);甲氧萘丙酸(萘普生);雙氯芬酸;四環素、米諾環素;氯黴素;胺基醣苷類;利奈唑胺(彩福適);胺碘
酮;干擾素;齊多夫定;阿黴素(阿德力黴素);順鉑;他莫昔芬;二甲雙胍;cystuc;或其混合物。
在個體需要服用已知或懷疑由於粒線體功能障礙或GSH減少而具有藥物毒性之藥劑之情形下,亦可向個體提供包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物之組合物。在特定情況下,在向個體給予甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或其功能性衍生物的同時及/或之前及/或之後向個體給予具有粒線體毒性之藥物。
1.HIV及TNF-α:8位HIV病患在補充半胱胺酸及甘胺酸以增加GSH濃度之前及補充2週之後進行血漿TNF-α濃度之量測。資料顯示,TNF-α自34.6±7.5減少至27.8±4.7(p=0.00049)。
2.神經認知資料:3位HIV病患在補充半胱胺酸及甘胺酸以增加GSH濃度之前及12週之後進行神經認知評估之量測。資料顯示神經認知功能之改善,如下文所示:連線測試(綜合指標)38±3至45±5
MAE III 30±5至45±4
MOCA(蒙特利爾認知評估(Montreal Cognitive Assessment))76±8至86±6
3.心臟舒張功能不良之改善:將雄性小鼠(30至35個月大)分2組進行研究,一個組餵食普通飲食(對照組-CON)且另一組之飼料補充有半胱胺酸加甘胺酸(NacGly)。比較在進食之前及進食七週之後(每一組中n=4)主動脈流出量、經二尖瓣口血流、主動脈僵硬度之非侵入性量測值以及針對左心室及心房解剖結構及功能之超音心動描記量測。與無變化之對照組相比,
NacGly小鼠顯示經二尖瓣口血流參數之顯著改善。NacGly小鼠亦顯著改善等容舒張時間(對照組23.1+2.5毫秒對NacGly 19.2+0.7毫秒,p<0.05)、等容收縮時間(對照組26.3+4.6毫秒對NacGly 13.9+0.3毫秒,p<0.05)、早期峰值充盈速度(對照組67+4cm/sec對NacGly 78+5cm/sec,p<0.05)。此研究之結論為膳食補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸改善老齡小鼠的舒張功能。
4.HIV病患之肝臟脂肪:在對1位個體補充半胱胺酸及甘胺酸之前及補充12週之後藉由MRI研究肝臟脂肪含量。結果顯示如下:藉由MRI測定之肝臟脂肪
右前葉(%)
右後葉(%)
基線(補充之前)
7.0+/-0.9%
8.5+/-1.2%
隨訪(補充之後)
5.0+/-1.1%
6.0+/-1.2%
5.糖尿病小鼠之肝臟脂肪:在暴露於不受控制之嚴重糖尿病1年之後研究兩組小鼠。自誘發糖尿病開始,一個組(治療組)接受半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸補充,而另一(對照)組接受與第一組等氮及等熱量之對照飼料。組織學評價顯示在接受等氮/等熱量飲食之對照組中脂肪肝發病率為95%至100%,而食用半胱胺酸/甘胺酸飲食之治療組僅具有2%至5%的脂肪肝發病率。肝臟脂肪之定量在經治療小鼠中顯示明顯較低的量。
6.肌肉蛋白分解:在對3位老年HIV病患補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸之前及補充12週之後使用示蹤劑3-甲基組胺酸來
研究肌肉蛋白分解情況。結果顯示肌纖維蛋白分解顯著下降。此等資料表明在衰老時使用半胱胺酸及甘胺酸改善穀胱甘肽含量可減少肌肉分解且對抗肌肉減少。
肌纖維肌肉蛋白分解速率:
補充之前:203±59mg/kgLBM/h
補充之後:137±15mg/kgLBM/h
在小鼠研究中,n-乙醯半胱胺酸及甘胺酸之作用改善老齡小鼠的粒線體功能及肌肉強度,且在特定實施例中,此改善經由穀胱甘肽進行。在一些實施例中,n-乙醯半胱胺酸及甘胺酸之補充減少小鼠之肝臟脂肪。
在特定態樣中,對HIV病患補充n-乙醯半胱胺酸及甘胺酸改善感染HIV之病患的輕度神經認知缺陷,改善肌肉強度及運動能力;及/或使穀胱甘肽恢復至年齡匹配之對照組程度。
在某些實施例中,在對老年人正在進行之研究中,補充n-乙醯半胱胺酸及甘胺酸在至少4週內改善認知缺陷。
據報導,感染HIV之病患因生理功能減退而加速衰老。據報導,HIV病患亦具有顯著的認知功能障礙。為評價補充半胱胺酸及甘胺酸之影響,研究8位HIV病患在補充半胱胺酸(如n-乙醯半胱胺酸)及甘胺酸之前及補充12週之後的情況,且比較對照組為年齡、性別及BMI相配之8位呈HIV陰性的人。結果量測包括生理功能(步行速度)及神經認知功能(連線測試及MAEIII)。
結果顯示,與非HIV對照組相比,感染HIV之病患具有明顯較慢
的步行速度(1.3±0.1m/s對1.06±0.04m/s,p<0.001),以及如藉由連線測試A(34.6±3.6秒對62.6±6.1秒,p<0.01)及連線測試B(53.8±7.2秒對117.5±5.0秒,p<0.01),以及藉由多語失語檢查III(41.0±3.5字對28.9±3.2字,p<0.01)所量測的明顯認知障礙。與補充前之水準相比,在補充12週之後,HIV病患之步行速度恢復(1.06±0.04m/s對1.30±0.04m/s,p<0.01)至與HIV陰性對照組類似且相當的水準,表明補充半胱胺酸及甘胺酸可使HIV病患之加速衰老逆轉。如由連線測試A(62.6±6.1秒對46.4±4.4秒,p<0.01)及連線測試B(117.5±5.0秒對69.8±5.4秒,p<0.01),以及MAE III(28.9±3.2字對34.6±2.0字,p<0.01)之評分改善所見的認知功能之顯著提高(補充前之水準對比補充後之水準)進一步支持此結果。
結論:補充半胱胺酸及甘胺酸使HIV病患之穀胱甘肽不足逆轉,且使功能衰退及認知功能逆轉。總體而言,該等資料支持補充半胱胺酸及甘胺酸使感染HIV之病患之加速衰老逆轉的指示。
本說明書中所提及之所有專利及出版物均指示熟習本發明所屬領域之技術者的水準。本文中所有專利及出版物皆以引用之方式併入,其引用程度就如同具體且單獨地指示每一個別出版物以全文引用之方式併入。
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儘管已詳細描述本發明及其優勢,但應理解,在不脫離如由申請專利範圍所界定之本發明的情況下,可在本文中進行各種變化、替代及變更。此外,本申請案之範疇不意欲侷限於說明書中所描述之製程、機器、製造、物質組合物、構件、方法及步驟之特定實施例。吾人自揭示內容將易於瞭解,可使用目前現有的或日後將開發的實質上執行與本文中所描述之相應實施例相同之功能或實質上實現與本文中所描述之相應實施例相同之結果的製程、機器、製造、物質組合物、構件、方法或步驟。因此,該等申請專利範圍意欲將此等製程、機器、製造、物質組合物、構件、方法或步驟包括在其範疇內。
Claims (6)
- 一種包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或甘胺酸及N-乙醯半胱胺酸之二肽之組合的用途,其係用於製造用以治療一或多種與細胞內穀胱甘肽(GSH)含量減少直接或間接相關之醫學病況或身體狀況之醫藥品,其中該醫學病況或身體狀況選自由以下組成之群:(a)肌肉損失;(b)失重之有害影響;(c)骨質疏鬆;(d)高血壓;(e)多囊卵巢症候群(PCOS);(f)冠狀動脈疾病;(g)壓力後之心肌損害;(h)疫苗接種後之免疫力不足;(i)耳毒性(j)頭暈(dizziness);(k)其組合,其中該甘胺酸衍生物係選自由以下組成之群:D-烯丙基甘胺酸;N-[雙(甲硫基)亞甲基]甘胺酸甲酯;Boc-烯丙基-Gly-OH(二環己基銨)鹽;Boc-D-Chg-OH;Boc-Chg-OH;(R)-N-Boc-(2'-氯苯基)甘胺酸;Boc-L-環丙基甘胺酸;(R)-N-Boc-4-氟苯基甘胺酸;Boc-D-炔丙基甘胺酸;Boc-(S)-3-噻吩基甘胺酸;Boc-(R)-3-噻吩基甘胺酸;D-α-環己基甘胺酸;L-α-環丙基甘胺酸;N-(2-氟苯基)-N-(甲磺醯基)甘胺酸;N-(4-氟苯基)-N-(甲磺醯基)甘胺酸;Fmoc-N-(2,4-二甲氧基苯甲基)-Gly-OH;N-(2-呋喃甲醯基) 甘胺酸;L-α-新戊基甘胺酸;D-炔丙基甘胺酸;肌胺酸;Z-α-膦醯基甘胺酸三甲酯,及其混合物。
- 如請求項1之用途,其中該甘胺酸或其功能性衍生物及該N-乙醯半胱胺酸係提供於同一組合物中。
- 如請求項1之用途,其中該甘胺酸或其功能性衍生物及該N-乙醯半胱胺酸係提供於不同組合物中。
- 如請求項1之用途,其中該甘胺酸或其功能性衍生物及該N-乙醯半胱胺酸係提供用於經口投與。
- 如請求項1之用途,其中該二肽包含N-乙醯半胱胺醯甘胺酸或半胱胺醯甘胺酸。
- 一種包含甘胺酸或其功能性衍生物及N-乙醯半胱胺酸或甘胺酸及N-乙醯半胱胺酸之二肽之組合的用途,其係用於製造用以中和或緩和與細胞內GSH含量減少直接或間接相關之藥物誘發之粒線體功能不全或障礙的醫藥品,及其中該甘胺酸衍生物係選自由以下組成之群:D-烯丙基甘胺酸;N-[雙(甲硫基)亞甲基]甘胺酸甲酯;Boc-烯丙基-Gly-OH(二環己基銨)鹽;Boc-D-Chg-OH;Boc-Chg-OH;(R)-N-Boc-(2'-氯苯基)甘胺酸;Boc-L-環丙基甘胺酸;(R)-N-Boc-4-氟苯基甘胺酸;Boc-D-炔丙基甘胺酸;Boc-(S)-3-噻吩基甘胺酸;Boc-(R)-3-噻吩基甘胺酸;D-α-環己基甘胺酸;L-α-環丙基甘胺酸;N-(2-氟苯基)-N-(甲磺醯基)甘胺酸;N-(4-氟苯基)-N-(甲磺醯基)甘胺酸;Fmoc-N-(2,4-二甲氧基苯甲基)-Gly-OH;N-(2-呋喃甲醯基)甘胺酸;L-α-新戊基甘胺酸;D-炔丙基甘胺酸;肌胺酸;Z-α-膦醯基甘胺酸三甲酯,及其混合物,及其中該藥物誘發之粒線體功能不全或障礙係由用於肝炎之抗病毒藥物引起,或 其中該藥物為抗驚厥藥;精神科藥物(psychotropic)(抗抑鬱劑;抗精神病藥;巴比妥酸鹽;焦慮症藥劑);膽固醇藥劑;鎮痛/消炎藥物;抗生素;抗心律不整藥物;類固醇;抗病毒藥物;癌症藥劑;糖尿病藥劑;β-阻斷劑;或為免疫接種(immunization),或其中該藥物為丙戊酸鹽(帝拔癲(Depakote));阿米曲替林(Amitriptyline)(依拉維(Elavil));阿莫沙平(Amoxapine);氟西汀(Fluoxetine)(百憂解(Prozac));西它普蘭(Citalopram)(喜普妙(Cipramil));氯丙嗪(Chlorpromazine)(托拉靈(Thorazine));氟非那嗪(Fluphenazine)(氟奮乃靜(Prolixin));氟哌啶醇(Haloperidol)(好度(Haldol));利培酮(Resperidone)(理思必妥(Risperdol));***(Phenobarbital);司可巴比妥(Secobarbital)(速可眠(Seconal));布他比妥(Butalbital)(非歐諾(Fiornal));異戊巴比妥(Ambarbital)(安密妥(Amytal));戊巴比妥(Pentobarbital)(寧必妥(Nembutal));阿普唑侖(Alprazolam)(贊安諾(Xanax));二氮平(Diazepam)(煩寧(Valium)、***(Diastat));膽酸-消膽胺(cholestyramine);環丙貝特(Ciprofibrate);ASA(阿司匹林(Aspirin));乙醯胺苯酚(泰諾(Tylenol));吲哚美辛(Indomethacin)(消炎痛(Indocin));甲氧萘丙酸(Naproxen)(萘普生(Aleve));雙氯芬酸(Diclofenac);四環素、米諾環素(minocycline);氯黴素(Chloramphenical);胺基醣苷類;利奈唑胺(Linezolid)(彩福適(Zyvox));胺碘酮(Amiodarone);干擾素;齊多夫定(Zidovudine);阿黴素(Doxorubicine)(阿德力黴素(Adriamycin));順鉑;他莫昔芬(Tamoxifen);二甲雙胍(Metformin);或其混合物。
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| US20140288177A1 (en) * | 2008-12-18 | 2014-09-25 | Baylor College Of Medicine | Increasing Glutathione Levels for Therapy |
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