靶標(biāo)解讀IFN-γ

更新時(shí)間：2025-05-19

點(diǎn)擊次數(shù)：852

1、簡(jiǎn)介

干擾素（IFN）多效性細(xì)胞因子家族，根據(jù)受體特異性可分為三型：I型（含IFN-α/β等13個(gè)亞型，通過(guò)IFNAR1/IFNAR2受體傳遞信號(hào)）、II型（僅包含IFN-γ，特異性結(jié)合IFNGR1/IFNGR2受體）及III型（IFN-λ，依賴IL-10R2/IFNLR1受體發(fā)揮作用）^[1-2]。IFN-γ是Ⅱ型干擾素的成員，其基因定位于人類染色體12q15區(qū)域，包含4個(gè)外顯子，其編碼基因在脊椎動(dòng)物中呈現(xiàn)高度保守性（人鼠氨基酸序列同源性約70%）。編碼的成熟蛋白由143個(gè)氨基酸通過(guò)鏈間二硫鍵形成功能性同源二聚體，其受體結(jié)合域中保守的α螺旋結(jié)構(gòu)對(duì)生物活性至關(guān)重要^[3]。

IFN-γ主要由T淋巴細(xì)胞、自然殺傷細(xì)胞（NK）和抗原提呈細(xì)胞（APCs，包括單核細(xì)胞、巨噬細(xì)胞和樹突狀細(xì)胞）分泌^[4-6]。其表達(dá)受先天免疫信號(hào)的嚴(yán)格調(diào)控，APCs通過(guò)分泌IL-12/IL-18激活STAT4/NF-κB通路，一方面趨化NK細(xì)胞向炎癥部位遷移，另一方面直接誘導(dǎo)IFN-γ基因轉(zhuǎn)錄，形成連接病原識(shí)別與適應(yīng)性免疫啟動(dòng)的關(guān)鍵調(diào)控軸^[7-9]。

作為免疫微環(huán)境的核心調(diào)控者，IFN-γ在感染部位呈現(xiàn)爆發(fā)式表達(dá)特征，其通過(guò)激活巨噬細(xì)胞殺菌功能、上調(diào)MHC分子表達(dá)及驅(qū)動(dòng)Th1分化等機(jī)制增強(qiáng)宿主防御^[10]。同時(shí)，該因子在腫瘤免疫中發(fā)揮雙重作用：既可誘導(dǎo)腫瘤細(xì)胞免疫原性死亡，又能促進(jìn)免疫檢查點(diǎn)分子（如PD-L1）表達(dá)形成負(fù)反饋調(diào)控^[11]。這種功能復(fù)雜性與其特殊的信號(hào)級(jí)聯(lián)機(jī)制直接相關(guān)，IFN-γ通過(guò)結(jié)合異源二聚體受體（IFNGR1/IFNGR2），觸發(fā)JAK1/JAK2-STAT1磷酸化級(jí)聯(lián)反應(yīng)，磷酸化STAT1入核后協(xié)同IRF家族蛋白，通過(guò)結(jié)合干擾素刺激反應(yīng)元件（ISRE）啟動(dòng)數(shù)百種干擾素刺激基因（ISGs）轉(zhuǎn)錄，形成級(jí)聯(lián)放大效應(yīng)。

2、功能或作用機(jī)制

1）受體激活與激酶級(jí)聯(lián)

IFN-γ以同源二聚體形式結(jié)合異源二聚體受體IFNGR，誘導(dǎo)受體構(gòu)象變化。此過(guò)程激活受體偶聯(lián)的JAK1（結(jié)合IFNGR2）和JAK2（結(jié)合IFNGR1）酪氨酸激酶，觸發(fā)二者相互磷酸化。活化的JAK1進(jìn)一步磷酸化IFNGR1鏈第440位酪氨酸殘基（Y440），形成兩個(gè)相鄰的STAT1蛋白SH2結(jié)構(gòu)域結(jié)合位點(diǎn)^[12-14]。

2）STAT1磷酸化與復(fù)合物組裝

募集至受體的STAT1分子在其C端Y701位點(diǎn)被JAK激酶磷酸化，激活誘導(dǎo)STAT1同源二聚化并從受體解離，同源二聚體進(jìn)一步激活激活I(lǐng)RF-1（Interferon Regulatory Factor-1，干擾素調(diào)節(jié)因子-1）及IFN-γ激活序列（GAS），以啟動(dòng)后續(xù)的基因轉(zhuǎn)錄調(diào)控，而少部分受體解離的STAT1會(huì)與STAT2及IRF-9形成異源復(fù)合物^[15-17]。其中，STAT1:STAT1:IRF-9復(fù)合物調(diào)控經(jīng)典GAS（IFN-γ-激活序列）響應(yīng)基因；STAT1:STAT2:IRF-9（ISGF3復(fù)合物）：靶向ISRE（干擾素刺激反應(yīng)元件）

3）核轉(zhuǎn)位與基因轉(zhuǎn)錄調(diào)控

磷酸化Stat1同源二聚體與ISGF3復(fù)合物轉(zhuǎn)位入核，分別結(jié)合靶基因啟動(dòng)子區(qū)的GAS和ISRE元件^[18]。IRF-1作為次級(jí)轉(zhuǎn)錄因子，進(jìn)一步擴(kuò)大調(diào)控網(wǎng)絡(luò)。此過(guò)程激活包括ICAM-1（細(xì)胞間黏附分子）、iNOS（誘導(dǎo)型一氧化氮合酶）及IRF家族成員在內(nèi)的多種干擾素調(diào)控基因，形成多層級(jí)轉(zhuǎn)錄放大效應(yīng)。

3、臨床應(yīng)用

1）抗感染

IFN-γ作為一種重要的免疫調(diào)節(jié)因子，在抗感染過(guò)程中發(fā)揮著關(guān)鍵作用。它通過(guò)激活巨噬細(xì)胞，增強(qiáng)其吞噬和殺傷能力，促進(jìn)抗原提呈，從而提高機(jī)體對(duì)病原體的清除效率^[20]。此外，IFN-γ還能誘導(dǎo)產(chǎn)生抗菌肽和其他具有直接殺菌作用的分子，進(jìn)一步加強(qiáng)宿主防御功能。

2）抗腫瘤

IFN-γ在腫瘤免疫監(jiān)視中占據(jù)核心地位，能夠直接抑制腫瘤細(xì)胞增殖，并通過(guò)多種途徑增強(qiáng)機(jī)體的抗腫瘤免疫反應(yīng)。IFN-γ可以上調(diào)MHC I類分子表達(dá)，使腫瘤細(xì)胞更容易被識(shí)別；刺激NK細(xì)胞、T細(xì)胞等效應(yīng)細(xì)胞的活性；誘導(dǎo)免疫檢查點(diǎn)分子如PD-L1的表達(dá)，進(jìn)而調(diào)節(jié)腫瘤微環(huán)境中的免疫平衡^[11,21-22]。

3）自身免疫性疾病

過(guò)度活躍的IFN-γ信號(hào)可能導(dǎo)致自身免疫性疾病的發(fā)生和發(fā)展，如系統(tǒng)性紅斑狼瘡（SLE）、多發(fā)性硬化癥（MS）等^[23-24]。針對(duì)IFN-γ信號(hào)通路的關(guān)鍵節(jié)點(diǎn)進(jìn)行干預(yù)，如使用單克隆抗體阻斷IFN-γ與其受體結(jié)合，或設(shè)計(jì)小分子化合物抑制下游信號(hào)傳導(dǎo)，可有效控制病情進(jìn)展，減少并發(fā)癥。

4）移植排斥反應(yīng)

術(shù)后，供體與受體之間的HLA（Human Leukocyte Antigen，人類白細(xì)胞抗原）差異是引發(fā)急性排斥反應(yīng)的主要原因。IFN-γ在此過(guò)程中扮演重要角色，它能增強(qiáng)移植物特異性T細(xì)胞的活化，加劇局部炎癥反應(yīng)，最終導(dǎo)致移植物功能喪失。IFN-γ抑制藥物可下調(diào)移植排斥介導(dǎo)的免疫應(yīng)答。此外，IL-10等具有抗炎效果的細(xì)胞因子，可以作為潛在的治療策略，減輕IFN-γ帶來(lái)的不利影響^[25]。

5）神經(jīng)退行性疾病

IFN-γ在神經(jīng)退行性疾病如阿爾茨海默?。ˋD）、帕金森?。≒D）中顯示出復(fù)雜的雙重作用。一方面，適度的IFN-γ水平有助于清除β-淀粉樣蛋白沉積物，減緩疾病進(jìn)程；另一方面，過(guò)量的IFN-γ可能會(huì)加重神經(jīng)炎癥，損害神經(jīng)元結(jié)構(gòu)與功能^[26]。針對(duì)IFN-γ在神經(jīng)退行性疾病中的復(fù)雜角色，未來(lái)的研究需要更加細(xì)致地解析其調(diào)控網(wǎng)絡(luò)，以期找到既能利用其有益效應(yīng)又能避免不良后果的治療方案。

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