多发性硬化症
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多發性硬化症 (multiple sclerosis ,MS)或多发性脑脊髓硬化症 (multiple cerebrospinal sclerosis[ 8] 中枢神经系统 白质 炎性脱髓鞘病变 自身免疫疾病 ,因病变具有部位(空间)多发和时间多发的特点,且产生许多硬性的胶质瘢痕
多發性硬化症最常侵犯的部位是脑室周围白质、视神经、脊髓、脑干传导束和小脑白质等处。患者腦 或脊髓 中的神經細胞 表面的絕緣物質(即髓鞘 )受到破壞[ 1] [ 5] [ 9] [ 10]
多發性硬化症依损害部位不同而临床表现多样,常见表现有视力下降(複視 、單側視力受損 )、感觉异常或遲鈍、肢体无力、共济失调或協調障礙、大小便障碍等[ 1]
病情多變,病程中常有缓解与复发、继发与进展,也可能初次發病後持續加劇。在每次發作之間,症狀有可能完全消失,但永久性的神經損傷仍然存在,這在病情嚴重的患者特別明顯[ 11]
雖然具體的成因不明,但多發性硬化症的機制可能為髓鞘受到免疫系統破壞 或生成髓鞘的細胞發生問題[ 3] 病毒 感染的刺激而引發自體免疫反應[ 9] [ 12] [ 4]
目前尚無根治多發性硬化症的方法[ 1] [ 9] 物理治療 則能改善患者的功能[ 1] 替代疗法 ,儘管其療效缺乏證據支持[ 13] [ 14] [ 5]
多發性硬化症是最常見的中樞神經系統 免疫疾病 [ 15] [ 6] [ 16] [ 7] [ 17] [ 2] 让-马丁·沙可 首次描述了多發性硬化症,意指大腦白質和脊髓中有許多疤痕(sclerae,可理解為現在所稱的斑塊或病灶)[ 18] [ 19] [ 20]
多發性硬化症主要的症狀 多發性硬化症患者可能出現任何神經學 症狀,其中自主神經 、視覺、運動和感覺問題最常出現[ 5] 感覺喪失 感覺異常 (如刺痛感或麻木等)、肌肉無力、視力模糊 [ 21] 反射增強 、痙攣 或運動困難、無法維持協調與平衡(共济失调 )、發音困難 吞嚥障礙 、視覺問題(如眼球震颤 、視神經炎 複視 )、疲勞 、急性 或慢性疼痛 、膀胱與腸胃蠕動問題等等,思考障礙或情緒問題(如憂鬱症 或情緒不穩 )也很常見。烏托夫現象 萊爾米特徵候 [ 5] 扩展残疾状态量表 多發性硬化症功能複合量表 [ 22] [ 23] [ 24]
約85%的患者一開始僅出現臨床單一症狀 視神經炎 腦幹 相關的症狀,剩下的25%則有超過一種前述的問題[ 4] [ 2] [ 11] [ 2] [ 5] [ 25] 感冒 、流行性感冒 或腸胃炎 )也會增加風險[ 5] 壓力 也可能引起疾病發作[ 26] 接種疫苗 、餵乳 [ 5] [ 27] 烏托夫現象 [ 25]
多發性硬化症的病因未明,但一般相信是由遺傳和環境因素(如感染)共同造成[ 5] [ 28]
多發性硬化症在緯度較高的地區較常出現[ 5] [ 29] 萨米人 、美洲原住民 、加拿大胡特爾人 、紐西蘭毛利人 [ 30] 因纽特人 [ 2] 薩丁尼亞人 [ 2] 西西里人 [ 31] 巴勒斯坦人 和帕西人 [ 30] [ 2] [ 29] [ 2]
多發性硬化症在北歐族群較常見[ 5] [ 2] 維生素D 較少有關[ 32] [ 33] [ 34] [ 35] [ 5] [ 28] [ 5]
六號染色體上的HLA區域。這些區域的改變可能會增加罹患多發性硬化症的機率。 普遍不認為多發性硬化症是一種遺傳 疾病,但一些遺傳變異 可能會增加罹病風險[ 36] [ 37] [ 9] [ 5] [ 9] [ 38] [ 2] [ 39]
目前已發現許多和多發性硬化症有關的基因 ,其中就包括了人類白細胞抗原 (HLA),這是一群在第六染色體上作為主要組織相容性複合體 (MHC)的蛋白質[ 5] 1型糖尿病 和全身性紅斑狼瘡 )有關[ 40] 等位基因 為DR15 DQ6 HLA-C554 和HLA-DRB1 [ 5] 遺傳傾向 全基因組關聯分析 ),科學家已發現其他至少12個HLA基因座以外的基因可能會增加多發性硬化症的罹病率[ 40]
科學家曾提出多種微生物 可能會誘發多發性硬化症,但沒有一種獲得證實[ 9] [ 12] 衛生假說 和盛行假說。衛生假說認為在生命早年暴露於特定的感染源能增強個體的保護力,若長大後才接觸那些病源則會造成疾病[ 5] [ 12] [ 41] [ 12]
多數多發性硬化症的患者腦和腦脊髓液 中含有寡株落條帶 腦脊髓炎 [ 42] 人類皰疹疹病毒 是最可能的感染源[ 43] EB病毒 感染的人罹患多發性硬化症的機率較低,但在成人早年受感染的人比更年輕就被感染的人有更高的罹病風險[ 5] [ 12] [ 12] 麻疹 、腮腺炎 和德國麻疹 [ 5]
目前已知吸菸 是多發性硬化症的一個獨立風險因子[ 32] 疫苗接種 做過因果分析,但多數沒有找到關聯性[ 28] 飲食 和賀爾蒙 攝取)也曾被科學家檢視,但這些因素和多發性硬化症間的關係都較薄弱且缺乏說服力[ 32] 痛風 的比率較低,血中的尿酸 濃度也較低;因此有假說認為尿酸對多發性硬化症有保護作用,但目前對於尿酸扮演的角色仍屬未知[ 44]
多發性硬化症目前認為可能是因自體免疫細胞攻擊神經系統,進而導致髓鞘破壞的疾病。 擁有髓鞘的神經細胞軸突 多發性硬化症發生的三個重要特徵包含出現中樞神經系統 病灶、發炎反應,以及髓鞘破壞 等。關於上述特徵如何出現,以及這些機轉如何導致臨床症狀,目前尚未完全了解[ 5] 膽固醇結晶 [ 45] [ 46] 免疫發炎 [ 9]
多發性硬化症的脫髓鞘現象(Demyelination),Klüver-Barrera 多發性硬化症會造成受侵犯的神經病灶處產生疤痕,並以此得名。本疾病最常進犯視神經 、腦幹 、基底核 、脊髓 ,以及側腦室 周圍的白質 [ 5] 灰質 腦區間的信息。多發性硬化症較少侵犯周邊神經系統 [ 9]
更精確一點來說,多發性硬化症會造成寡突膠質細胞 的喪失。寡突膠質細胞會產生和維持包覆神經纖維的髓鞘 ,幫助動作電位 的傳導[ 5] 軸突 受損退化。髓鞘消失後,神經元的傳導效率會下降[ 9] 再髓鞘化 [ 47] 磁振照影 (MRI)時常會顯示腦部出現十幾個新斑塊。這種現象可能代表患者腦部其實存在有大量的病灶,但因為神經的自癒功能,使患者平時沒有出現明顯症狀。另外,病灶處也會因為神經損傷而導致星狀細胞異常增多 [ 5] 病理特徵 [ 48]
除脫髓鞘現象外,發炎反應 也是多發性硬化症的重要體徵之一。T細胞 在多發性硬化症的發炎反應中扮演重要角色[ 9] 血腦障壁 保護,一旦這層屏障受到破壞,T細胞就會進到中樞神經,將髓鞘視為外來物進行攻擊,這些攻擊自身的淋巴細胞又稱自體反應性淋巴球(autoreactive lymphocytes)[ 5] 細胞激素 和抗體 ,擴大發炎反應。持續擴大的發炎反應可能會導致血腦障壁的瓦解,進而出現一系列神經受損的現象,例如神經水腫 、巨噬細胞 活化、細胞激素釋放,以及出現許多遭受破壞的蛋白質[ 9] [ 5]
血腦障壁 是中樞神經系統血管外一層防止血液中的物質進入腦脊髓的屏障,同時也能阻擋T細胞進入。但如果中樞神經遭到病毒或細菌感染時,血腦障壁的通透性會增大。感染消退後,血腦障壁會自行修復,但當初跑進來的T細胞會殘留在腦中[ 9] 钆 是一種沒有辦法穿透正常血腦障壁的元素,因此钆增強磁振造影(gadolinium-enhanced MRI)可以用於檢測血腦障壁瓦解與否[ 49]
圖中患者每月進行核磁共振掃描追蹤,可以看到腦中隨時間不斷出現散在型的病灶。 多發性硬化症的核磁共振(MRI)影像 臨床症狀是診斷多發性硬化症的重要依據,配合醫學影像 和醫學檢驗可以輔助診斷[ 4] [ 5] [ 50] 麥克唐納診斷標準 [ 16] 舒馬克 波色診斷標準 [ 51] 泛視神經脊髓疾病 [ 52]
若患者有多次特異性較高的事件發作,可能直接透過臨床證據即可診斷多發性硬化症。但若僅有發作過一次,則必須進行其他測試來輔助診斷。最常見的工具有神經影像學 、腦脊髓液分析,以及誘發電位測試 。核磁共振 影像可以顯示腦部喊脊隨脫髓鞘的區域,以及斑塊等病灶。靜脈輸注含钆 的顯影劑 [ 53] [ 54] 腰椎穿刺 採檢取得。技術員會將腦脊液進行電泳 ,檢視電泳膠片上是否帶有IgG的寡克隆條帶 [ 53] [ 55] 視神經 和感覺神經 對於刺激的敏感度也會下降,這些現象可以透過視神經和感覺神經的誘發電位 偵測而得[ 56]
上述的診斷方式皆屬於非侵入性的診斷方式[ 5] 遺體解剖 和病灶的組織活檢 才能確診[ 53] [ 57] [ 58]
截至2013年為止,美國國家多發性硬化症學會 國際多發性硬化症聯合會 [ 59] [ 60] [ 61]
臨床單一症候群 復發緩解型多發性硬化症(Relapsing-remitting MS,RRMS)
原發進行性多發性硬化症(Primary progressive MS,PPMS)
續發進行性多發性硬化症(Secondary progressive MS,SPMS) 復發緩解型(RRMS)多發性硬化症中最常見的一型,占所有首次發作病患的80%左右。此類患者在單次發作後,會進入數月到數年的緩解期 後遺症 ,且發作時間越久,發生後遺症的機會越大[ 5] [ 4] [ 62] [ 5] 惡性多發性硬化症 [ 63] [ 5] [ 64] [ 64]
原發進行性多發性硬化症(PPMS)約占多發性硬化症患者的10–20%,此類患者在初始發作後,症狀即會不斷惡化,完全不會緩解或改善[ 11] [ 4] [ 65] [ 5] [ 66]
續發進行性(SPMS)常以RRMS作為初始表現,約有65%初始診斷為RRMS的病患為SPMS。此類型的特點是在每次發作之後,神經功能都會有所減退,且之間沒有明顯的緩解期[ 5] [ 11] [ 11] [ 67]
除了上述四種類型之外,還有多種疑似多發性硬化症的亞型也已被描述,這些亞型被統稱為特發性發炎性脫髓鞘病 視神經脊髓炎 瀰漫性脫髓鞘硬化症 同心圓性硬化症 馬爾堡多發性硬化症 [ 68] [ 5]
雖然目前無法治癒多發性硬化症,但部分療法已被證實能有效控制疾病。治療的目標為恢復患者的功能、預防再次發作和失能。一般會建議有發作過一次並有兩處以上MRI病灶的患者開始使用藥物介入[ 69] 副作用 。人們也不斷嘗試另類療法 ,即便這些療法的效果缺乏證據支持[ 13]
在患者症狀發作時,通常會靜脈注射 高劑量類固醇 (如甲基培尼皮質醇 )[ 5] [ 70] [ 71] 血漿置換術 治療[ 5]
截至2019年,已有11種藥物核准用於復發緩解型多發性硬化症的疾病調節,這些药物分別為干擾素β-1a 干擾素β-1b 醋酸格拉替雷 (glatiramer acetate)、米托蒽醌 (mitoxantrone)、那他珠單抗 芬戈莫德 特立氟胺 [ 72] [ 73] 富馬酸二甲酯 (dimethyl fumarate)[ 74] 阿侖單抗 [ 75] [ 76] 奥美珠单抗 [ 77] 西普尼莫德 [ 78]
截至2012年,藥物治療的成本效益仍然未明[ 79] 美国食品药品监督管理局 (FDA)核准奥美珠单抗 CD20 人源化 單株抗體 [ 80] [ 81] 第四期臨床試驗 [ 82]
減少發作次數對於復發緩解型的病程有一定的效果[ 72] [ 4] [ 83] [ 84] [ 85] [ 86] [ 4] [ 83] [ 4] 干擾素 治療可以減少病人進展為多發性硬化症的機率[ 5] [ 87] [ 88]
截至2017年,儘管利妥昔單抗 (rituximab)尚未核准用於多發性硬化症的治療,但臨床上仍常用於治療 復發緩解型多發性硬化症[ 89]
2017年以前,利妥昔單抗 (rituximab)廣泛被作為原發進行性多發性硬化症的仿單標示外治療[ 89] 美國食品藥品監督管理局 (FDA)核准了奥美珠单抗 [ 80] [ 81] 第四期 [ 82]
截至2011年 (2011-Missing required parameter 1=month ! ) [update] 米托蒽醌 (mitoxantrone)是唯一一種核准用於治療續發進行性多發性硬化症的藥物[ 90] [ 91] [ 92]
注射格拉替美後引發的局部紅腫 干擾素及格拉替美(glatiramer)等疾病調節劑最常見的副作用之一是注射處紅腫(皮下注射90%機率,肌肉注射33%機率)。且注射一段時間後,注射處的脂肪組織會崩解,形成一個明顯的凹痕,此現象稱為脂萎縮 [ 93] 類似流行性感冒的症狀 [ 94] [ 95] 肝損傷 [ 96] 米托蒽醌 則有可能造成心臟收縮問題 (12%)、不孕 ,以及急性骨髓性白血病 (0.8%)等問題[ 91] [ 97] 进行性多灶性白质脑病 (PML,1/600人)[ 4] [ 98]
芬戈莫德 高血壓 、心率下降 、黃斑部水腫 、肝指數上升,或淋巴球減少 [ 88] [ 72] 致畸性 都曾有報導[ 88] 富馬酸二甲酯 的常見副作用為潮紅和腸胃道副作用[ 74] [ 88] 白血球數量減少 ,但目前試驗並無伺機性感染的報導[ 99] [ 100] [ 101]
藥物和神經復健 [ 102] 科際合作 來改善病人的生活品質。由於多發性硬化症的病程及醫療涉及多項醫學專科,因此難以界定所謂的「核心團隊」[ 5] [ 103] [ 104] [ 105] [ 106] [ 107] [ 108] 認知行為療法 則顯示對於多發性硬化症造成的疲憊症狀有所助益[ 109]
超過50%的多發性硬化症患者會尋求替代醫療 (此比率依替代醫療的定義而有差異),但替代醫療的療效通常證據薄弱或缺乏證據支持[ 13] [ 110] [ 13] [ 111] [ 112] [ 113] 瑜珈 等放鬆技巧 [ 13] 草藥 (包括医用大麻 )[ 13] [ 114] [ 115] 高壓氧治療 [ 116] 自行吞下鉤蟲 區域反射療法 、针灸 [ 13] [ 117] 正念療法 [ 118] [ 13]
血管外科醫師保羅·贊博尼 慢性腦脊髓靜脈回流不足 [ 119] [ 120] [ 119]
多發性硬化症2012年的失能調整生命年 (每十萬人) 32-68
68-75
77-77
77-88
88-105
106-118
119-119
120-148
151-462
470-910
多發性硬化症的病程取決於疾病的亞型、個人的性別與年齡、最初的症狀和患者失能 的程度。女性、復發緩解型、一開始有視神經炎或感覺症狀、最初幾年較少發作、較早發病的患者有較好的預後[ 14] [ 121]
發病後的平均預期餘命為30年,較未得病的群體少了5到10年[ 5] [ 121] [ 5] 自殺 率也較高,對肢體障礙的患者而言感染和其他併發症的風險則特別高[ 5]
約有80%的多發性硬化症患者一開始是以臨床單一症候群表現。若核磁共振掃描發現未進犯的神經區域有異常的影像學變化,在未來兩年內有50%的機率會發生脫髓鞘疾病,20年內的機率甚至高達八成[ 122] [ 123]
2012年多發性硬化症造成的死亡率(每百萬人) 0-0
1-1
2-2
3–5
6–12
13–25
多發性硬化症是最常見的中樞神經 自體免疫疾病[ 15] [ 16] [ 2] [ 124] [ 16] [ 2] [ 16]
多發性硬化症的發生率似乎正在上升,但這或許可以用診斷技術的進步來解釋[ 2] [ 41] [ 12] [ 28] [ 32]
多發性硬化症常在成年發生,特別是25到35歲,但在少數的情形下也可發生在孩童或大於50歲的人身上[ 16] [ 2] [ 65] [ 5] [ 29] [ 16] [ 5] [ 65]
凱斯威爾對多發性硬化症患者腦幹 級脊髓 病灶的描繪。繪於1838年。 英國病理學家 羅伯特·凱斯威爾 讓·克呂維耶 [ 125] [ 5] 喬治·愛德華·林德弗雷奇 [ 126] [ 127]
1868年,法國神經學家 讓-馬丁·沙可 (1825–1893)在回顧過去文獻,加上自己的臨床和病理觀察後,首次建立多發性硬化症此一診斷[ 125]
在沙可建立診斷的同時,他也嘗試首度建立多發性硬化症的診斷標準,並提出著名的「沙可三重症」(Charcot's triad)[ 註 1] 眼球震顫 、意向性顫抖 電報式語言 [ 128] [ 18] [ 19]
自此,沙可三重症成為多發性硬化症的標準診斷依據,直到1965年舒馬克 [ 128] 波色診斷標準 麥克唐納診斷標準
到了20世紀,關於此病症病理機轉的理論開始有些進展,到了1990年代之後更發展出了數項治療[ 5] [ 129] [ 130]
一名具有步行困難的女性患者的連續拍攝影像。埃德沃德·迈布里奇 攝,1887年。 在沙可建立此診斷之前,相關診斷無法進行。下列病例在重新回顧分析後,可能也是多發性硬化症的患者。
11世紀左右,有一名居住於冰島 的年輕女性哈朵拉(Halldora)突然失去視力和運動功能,在祈禱之後的七天奇蹟似地恢復。斯希丹 的聖李維娜 荷蘭 修女 ,她可能是目前已知最古老的可診斷病例之一。聖李維娜從16歲到她53歲病逝之間的歲月裡,身受間歇性疼痛、下肢無力、視力喪失等症狀所苦,而上述症狀都是典型多發性硬化症的症狀[ 131] 維京人 的假說[ 132]
英國國王喬治三世 的孫子,奧古斯特·弗德里克·德斯特 薩塞克斯公爵 奧古斯都·腓特烈 和茉蕊夫人 短暫性視覺喪失 陰莖不舉 等等,到了1844年他開始使用輪椅輔助他的行動。儘管疾病纏身,德斯特仍然維持樂觀的態度面對人生。他從1822年到1846年的日記至今仍留存於世,紀載了他22年於疾病共生的生活。詳實的病程紀載,使他幾乎可以直接確診為多發性硬化症[ 133] [ 134]
英國日記作家布魯斯·弗雷德里克·卡明斯(Bruce Frederick Cummings,1889–1919)以筆名 「W·N·P·巴貝利昂 [ 134] 鬱人日誌 The Journal of a Disappointed Man )為書名集結出版[ 135]
阿侖單抗 為多發性硬化症找尋更有效、更安全,及更方便的藥物治療仍是目前研究重點。其他研究方向包含神經保護 [ 20]
自21世紀以來,有多種口服藥物已經核准上市,用藥也逐漸普及[ 136] ozanimod 拉喹莫德 雌三醇 。拉喹莫德於2012年8月宣布進行治療多發性硬化症的臨床試驗,目前已在進行第三期試驗,但其二期試驗並未顯示顯著效果[ 137] 干擾素β-1a 聚乙二醇高分子修飾 [ 138] [ 139] 性激素 ,後被發現可能可以治療復發緩解型多發性硬化症,目前已進入第二期試驗[ 140] [ 141]
單株抗體 的高度選擇性使其成為研究重點之一。截至2012年,已有多種單抗顯示可能有潛力對抗多發性硬化症,如阿侖單抗 達利珠單抗 利妥昔單抗 (rituximab)、奥美珠单抗 奧法木單抗 CD20 [ 101] 美国食品药品监督管理局 (FDA)已於2017年3月核准奥美珠单抗 [ 80] [ 136] JC病毒 進行性多灶性白質腦病 (PML)[ 136] [ 136] [ 136]
聯合療法 是指同時使用多種藥物進行治療的策略,其發展與創新也是目前的研究焦點之一。若加入另一種藥物能夠提升治療效果的總和,則這樣的作用稱為協同作用。目前已有多種臨床試驗測試聯合療法的效果,但目前為止仍尚未發展出足夠有效的聯合療法[ 142]
疾病初期的神經保護及神經再生的研究也是目前的研究重點之一,如幹細胞療法 等等[ 143] [ 136]
多發性硬化症目前尚屬於一種類似症狀集合而成的表現。有些譜系的患者擁有特殊的自體抗體,日後可能透過對於這些自體抗體的研究,將疾病進行更精確的分類。
視神經脊髓炎 AQP4 [ 144]
後來又發現擁有抗MOG 馬爾堡多發性硬化症 急性瀰漫性腦脊髓炎 另一種疾病光譜 [ 144]
抗神經束蛋白 蘭氏節 會遭到破壞,此類疾病主要以周邊神經脫髓鞘疾病表現,但可能出現於慢性原發進行性多發性硬化症或合併中樞神經推髓鞘症狀 [ 145]
除了上述幾種自體抗體之外,另有四種脫髓鞘疾病於多發性硬化者患者中發現,代表此疾病現在仍為一個異質性相當高的診斷,有待更精確的分類和分型[ 146]
經梯度回聲相位波序(Gradient-echo phase sequence)處理的腦部核磁共振檢查顯示腦白質中有鐵質沉積(綠色方框中由紅色箭頭標示處)[ 147] 雖然可以預期近期內多發性硬化症的診斷標準不會改變,但科學家仍持續在尋找能幫助診斷和預測疾病活性的生物標記分子 [ 136] [ 148]
目前沒有任何檢驗能預測多發性硬化症的預後,一些有潛力的分子包括白介素-6 、一氧化氮 與一氧化氮合成酶 、骨橋蛋白 和胎球蛋白 神經絲 tau蛋白 和N-乙醯天門冬胺酸 [ 148]
正子斷層造影 (PET)和核磁共振成像 (MRI)等神經影像技術的進步帶來了更好的診斷力和預後預測能力,雖然這些進步要實際應用到臨床上往往需要數十年的時間[ 136] 磁矩轉移 擴散磁振造影 (DWI)和功能性核磁共振成像 (fMRI)。這些技術相較於現有的技術有更高的專一性,但仍缺乏標準化的檢驗流程和常模數值。還有一些仍在開發中的技術,例如能量測周邊巨噬細胞、發炎或神經失能的程度的顯影劑,以及能測量鐵沈積量或大腦灌流量的技術[ 149] 放射性追蹤劑 能觀測特定生物反應的變化,例如腦組織發炎、皮質病灶、細胞凋亡 或再髓鞘化(remylienation)[ 150] Kir4.1 [ 151]
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