这项工作得到了 Ministero dell'Istruzione、dell'Università e della Ricerca - MIUR 项目 Dipartimenti di Eccellenza 2018-2022 和 2023-2027 到神经科学系 Rita Levi Montalcini 的支持;Cavalieri-Ottolenghi 基金会，意大利奥尔巴萨诺。BB 是皮埃蒙特地区 INFRA-P （n.378-35） （2022-2023） 和 PRIN 2020 - 20203AMKTW 的研究员。我们感谢 Fondazione per la Ricerca Biomedica Onlus （FORB） 的支持。出版费得到了Distretto Rotaract 2031的善意捐赠，特别是都灵北东扶轮社的捐赠。我们感谢伊莱恩·米勒（Elaine Miller）校对我们的手稿。

本工作中的动物护理和处理是根据 2010年 9 月 22 日欧盟理事会指令 （2010/63/UE） 进行的;本研究中报告的所有程序均已获得意大利卫生部 （407/2018-PR） 和都灵大学伦理委员会（项目编号 360384）的批准。我们建议按照 Kilkenny 等人最初于 2010 年发表的 ARRIVE 指南进行实验设计20.在开始之前，请确保有必要的材料可用（请参阅 材料表）。在高压灭菌器中对用于制备MOG35-55 乳液的所有玻璃器皿和器皿进行消毒。实验过程的总结如 图1所示。
1. MOG35-55 乳液的制备
注意：为了制备乳剂，需要MOG35-55，不完全弗洛伊德佐剂（IFA）， 结核分枝杆 菌菌株H37Ra（MT）和生理溶液（见 材料表）。
注意：热杀灭的 MT 可以刺激先天免疫反应。避免吸入、摄入和接触皮肤和眼睛，使用适当的个人防护装备，并在引擎盖下的有盖精密天平中称量 MT。
<table border="1" fo:keep-together.within-page="1" fo:keep-with-next.within-page="always"><tbody><tr><td>溶液</td>
			<td>组成</td>
			<td>笔记</td>
		</tr><tr><td>2 mg/mL MOG35-55 肽溶液</td>
			<td>在生理溶液中以 2 mg/mL 浓度稀释的冻干 MOG35-55 肽</td>
			<td>将已经稀释的溶液保存在-80°C。</td>
		</tr><tr><td>5 μg/mL PT 溶液</td>
			<td>冻干的PT在生理溶液中以5μg/mL浓度稀释。</td>
			<td>将已经稀释的溶液保存在-80°C。</td>
		</tr><tr><td>乳剂</td>
			<td>每只待免疫小鼠所需的乳剂总体积为300μL，划分如下：</td>
			<td>为避免改变或污染，请在免疫接种当天准备乳剂。</td>
		</tr><tr><td></td>
			<td>200 μg/小鼠的MOG35-55 ，即100μL的MOG35-55 2 mg/mL溶液。</td>
			<td></td>
		</tr><tr><td></td>
			<td>50 μL生理溶液</td>
			<td></td>
		</tr><tr><td></td>
			<td>150 μL IFA</td>
			<td></td>
		</tr><tr><td></td>
			<td>4 mg/mL MT，即 1.2 mg/小鼠</td>
			<td></td>
		</tr><tr><td>生理溶液</td>
			<td>氯化钠0.9%在蒸馏水中稀释。</td>
			<td></td>
		</tr></tbody></table>表1： 用于免疫程序的溶液的组成。
<ol><li>在玻璃烧杯中制备溶液，首先加入液体成分，最后加入MT。 注意：每只待免疫小鼠所需的乳剂总体积为300μL，如 表1所示。乳液非常粘稠，因此在制备和注射过程中，可能会有一些损失，尤其是在为几只小鼠制备溶液时。我们建议通过高估至少1.5-2倍的免疫小鼠数量来计算所需的最终乳剂体积。</li>
	<li>将烧杯放入冰块中，然后使用带有18G针头的玻璃注射器开始乳化溶液。 注意：乳液也可以使用其他策略制备，例如，通过将两个无气玻璃注射器与三通旋塞阀连接并通过来回推动柱塞来混合溶液21,22。</li>
	<li>乳化溶液至少15分钟;一般来说，30分钟的乳化就足够了。为了检查乳液的质量，在装满水的透明容器中加入一滴乳液：如果液滴保持其结构并保持完整，则乳液已准备就绪。</li>
	<li>将乳液直接放入将用于免疫接种的 1 mL 注射器中，并将其储存在 +4 °C 直至使用，以保持乳液的厚度并避免改变或污染。</li>
</ol>2. 动物选择和免疫
<ol><li>动物选择
	<ol><li>在8-10周龄时选择两性成年C57BL / 6J小鼠，最佳体重为~20g。一定要为不同的实验组选择年龄和性别匹配的小鼠，因为对疾病的易感性可能随年龄和性别而变化。 注意：小鼠在免疫当天的体重应相当，因为本程序针对特定体重范围（17-25g）进行了优化。</li>
		<li>在22±2°C，在12：12光/暗循环下，在45cm x 25 cm x 15 cm聚丙烯小鼠笼中，在标准条件下将同性动物分组饲养（n = 4-5 /笼子），以避免社会隔离。 随意提供食物和水。 注意：最终，为了进一步限制免疫动物病程的潜在变异性，我们还建议形成足够数量的实验组。还有研究 8,23 将免疫接种时间描述为决定 EAE 结果变化的条件。因此，我们建议在所有动物中大约在同一时间进行免疫接种，最好是在每日光/暗周期23的光照时间内。为了限制压力，最好在免疫日之前对动物进行操作，并标记它们以轻松识别它们以进行日常评估，例如，剪耳或标签。</li>
	</ol></li>
	<li>免疫程序 注意：确保该程序由经验丰富的调查员执行，以尽量减少对动物的压力并优化免疫接种。在开始免疫接种之前，请根据机构动物护理和伦理委员会指南选择麻醉方法。我们的实验室使用异氟醚进行短暂麻醉。<ol><li>麻醉小鼠：4%异氟醚用于麻醉诱导，1.5-2%异氟醚用于麻醉维持。等待麻醉有效，并使用前脚脚趾捏住来评估麻醉水平。为防止小鼠在麻醉下出现眼睛干燥，请使用兽医批准的眼药膏。</li>
		<li>在外侧尾静脉中静脉注射PT：用乙醇溶液轻轻塞住小鼠的尾巴，乙醇溶液可作为血管扩张剂，以显示静脉。聚焦于尾部的两条侧静脉之一，并使用装有 30 G 针头的 0.5 mL 注射器注射 500 ng PT（即，100 μL PT 稀释在生理溶液中以 5 μg/mL 的浓度）。</li>
		<li>皮下注射MOG35-55 乳剂：使用带有26G针头的1mL注射器，对先前制备的乳液进行三次皮下注射：两次在侧翼的喙部下方，一次在尾部底部。在每个部位注射的乳剂体积为100μL，每只小鼠中注射的乳剂总体积为300μL。 注意：免疫接种日记录为免疫接种后第 0 天 （dpi）;48小时后（即在2dpi下），有必要进行另一次静脉注射PT，与先前进行的注射相同。可以使用鼠标约束器在没有麻醉的情况下进行注射。这里描述的程序旨在在免疫程序期间诱导和维持小鼠的麻醉，以避免动物可能的不适和运动或小鼠和研究人员的风险。因此，没有外科手术。然而，为了优化实验过程，重要的是在这些步骤中保持适当的无菌条件，并在这些程序后监测小鼠的状况。</li>
		<li>为了验证小鼠是否已从注射中恢复过来，请在手术后将其放入干净的笼子中，并等待它恢复足够的意识以保持胸骨卧位。老鼠完全康复后，将其与其他动物一起放回笼子。</li>
	</ol></li>
</ol>3. EAE跟进
<ol><li>体重和食物摄入量
	<ol><li>使用电子精密天平每天监测动物的体重（BW），因为BW的减少是疾病进展的指标。 注意：根据机构和伦理委员会的动物护理指南，这种减少不应超过一定百分比。通常，如果动物减掉了初始体重的 20% 以上（即以 0 dpi 记录的体重），则应将其作为人道终点的应用而牺牲。安乐死方法包括吸入（例如，5% 异氟烷）的深度不可逆麻醉，然后斩首。</li>
		<li>监测食物摄入量 （FI） - 动物在一天内吃的食物 （g∙day-1∙animal-1），每周至少称量一次特定容器中的食物量，并将经过的天数除以两次连续测量和笼子中的动物数量。 注意：此测量可以估计平均食物摄入量。由于临床疾病体征的出现和积累，包括四肢瘫痪，我们建议当动物不能用后肢站稳并够到食物容器或水瓶时，在笼子的地板上放置一些浇水的食物。为了尽可能精确地评估随访期间的食物摄入量，我们还测量了这种食物的干重，然后再为小鼠润湿。</li>
	</ol></li>
	<li>EAE期间发情周期性的评估
	<ol><li>检查发情周期至少两个周期，评估 McLean 等人 24 描述的阴道细胞学涂片。根据阴道涂片样本中三种主要细胞类型（有核上皮细胞、角化鳞状上皮细胞和白细胞）的存在对发情周期的阶段进行分类，如下所示：<ol><li>根据几乎完全存在的圆形、形成良好的有核上皮细胞簇，将其分类为发情期。</li>
			<li>根据密集堆积的角质化鳞状上皮细胞簇的主要存在分类为发情期。</li>
			<li>根据主要存在小的深色白细胞和少量角质化鳞状上皮细胞，将其分类为中胚层。</li>
			<li>根据高度突出的深色小白细胞和罕见的角质化鳞状上皮细胞以及可能出现的有核上皮细胞，将其归类为发情期。 注意：在评估两性疾病时，重要的是要检查由于发情周期引起的女性变异性。我们建议重点评估发情周期，特别是在免疫接种后第一周和第二周之间（即在EAE的急性期）。先前已经表明，免疫程序会导致发情周期在这一阶段最显着的改变25.此外，重要的是要考虑到，由于后肢麻痹和后肢缺乏张力，当动物达到高临床评分（尤其是 >3）时进行涂片是困难的。</li>
		</ol></li>
	</ol></li>
	<li>临床评分
	<ol><li>让盲法调查员每天评估动物的临床评分。为每只动物分配一个从0到5的评分（见表2），以评估Racke7所描述的疾病过程26。 注意：与体重减轻类似，根据机构和伦理委员会的动物护理指南，人道终点对于临床评分的增加也是必要的。一般来说，如果动物不再能够自主进食（根据我们使用的量表，这通常发生在动物至少达到 4 分时），它应该被牺牲作为人道终点的应用。</li>
	</ol></li>
	<li>通过旋转测试评估电机性能 注意：EAE 进展的评估通常通过每天分配临床评分来进行，该评分由训练有素的盲法研究者完成。然而，对疾病的进展进行更定量和客观的评估可能是有用的。在先前的研究26中，旋转试验用于测量免疫动物的运动性能。正如van den Berg等人27所描述的那样，为了对病程进行更定量和更精确的临床评估，通过旋转试验对运动性能的评估可以支持临床评分评估。详细描述见van den Berg et al.27。<ol><li>让小鼠每天进行旋转训练，从1 dpi开始直到牺牲（即28 dpi）。每个会话由一个 300 秒的会话组成，在此期间，杆速必须从 4 rpm 线性增加到 40 rpm。</li>
		<li>登记动物的分数。当鼠标无法保持平衡并从设备上掉下来时，它会掉在地上并触发传感器，并记录时间。因此，性能被评分为下降的延迟。</li>
	</ol></li>
</ol>
<table border="1" fo:keep-together.within-page="1" fo:keep-with-next.within-page="always"><tbody><tr><td>年级</td>
			<td colspan="2">临床体征</td>
			<td colspan="3">描述</td>
		</tr><tr><td>0</td>
			<td colspan="2">健康</td>
			<td colspan="3">无观察到的临床体征。动物表现出正常的音调和尾巴的移动。它走路不会绊倒。</td>
		</tr><tr><td>0.5</td>
			<td colspan="2">闸门受损</td>
			<td colspan="3">动物在烤架上行走时绊倒。</td>
		</tr><tr><td>1</td>
			<td colspan="2">跛行的尾巴</td>
			<td colspan="3">当动物被尾巴的根部捡起时，尾巴会下垂（松弛的尾巴）。</td>
		</tr><tr><td>1.5</td>
			<td colspan="2">跛行的尾巴和受损的门</td>
			<td colspan="3">这只动物的尾巴松弛，在烤架上行走时会绊倒。</td>
		</tr><tr><td>2</td>
			<td colspan="2">共济失调</td>
			<td colspan="3">一旦动物被翻过来，它就很难站起来。</td>
		</tr><tr><td>2.5</td>
			<td colspan="2">共济失调和后肢麻痹</td>
			<td colspan="3">动物展示一旦仰卧就无法站立，并且失去了一只后肢的音调。</td>
		</tr><tr><td>3</td>
			<td colspan="2">后肢瘫痪</td>
			<td colspan="3">动物失去双后肢的音调。</td>
		</tr><tr><td>3.5</td>
			<td colspan="2">后肢瘫痪和/或前肢麻痹</td>
			<td colspan="3">动物失去后肢和部分前肢的音调。事实上，它显示了前肢抓握的力量丧失。</td>
		</tr><tr><td>4</td>
			<td colspan="2">四肢麻痹</td>
			<td colspan="3">动物完全失去了四肢的音调。</td>
		</tr><tr><td>4.5</td>
			<td colspan="2">四肢麻痹和体温降低</td>
			<td colspan="3">动物完全失去了四肢的音调，并且体温下降（很冷）。</td>
		</tr><tr><td>5</td>
			<td colspan="2">垂死或死亡</td>
			<td colspan="3">动物正在死亡（它对任何刺激没有反应）或死亡。</td>
		</tr></tbody></table>表2： 用于评估 EAE 进展的临床评分系统。
4. 脊髓水平 EAE 诱导的组织病理学体征的评估
注意：在这里，我们简要报告了牺牲动物并收集脊髓进行组织病理学分析的程序;有关详细说明，请参阅这些参考文献10、26、28、29。
<ol><li>固定和组织取样 注：有关详细说明，请参阅这些参考文献10,26。<ol><li>在疾病的慢性期以28 dpi处死动物。<ol><li>通过深度不可逆麻醉（腹膜内注射唑拉西泮和替他明80mg / kg /甲苯噻嗪10mg / kg）麻醉小鼠。</li>
			<li>用生理盐水溶液经心灌注小鼠，然后用4%多聚甲醛（PFA）溶液灌注。 注意： 使用 PFA 时要注意：因为它有毒，请使用适当的个人防护设备避免吸入、摄入和接触皮肤和眼睛。称量粉末，制备溶液，并在罩下进行灌注。</li>
		</ol></li>
		<li>从脊柱上取下脊髓30.</li>
		<li>将脊髓储存在4%PFA溶液中24小时。</li>
		<li>在0.01M盐水磷酸盐缓冲液（PBS）中进行多次洗涤。</li>
		<li>将脊髓嵌入石蜡块30.</li>
	</ol></li>
	<li>组织学程序 注：有关详细说明，请参阅Montarolo et al.10。<ol><li>使用切片机切割10μm厚的横脊髓切片，并将它们收集在明胶涂层的载玻片上。定向切片平面以匹配对应于小鼠脊髓图谱31的横截面的图纸。</li>
		<li>执行第32 节的脱蜡。</li>
		<li>用苏木精和曙红32 染色切片。</li>
		<li>脱水部分32.</li>
		<li>用安装介质覆盖这些部分，并在化学罩下在室温下干燥。 注意：苏木精-伊红染色可以检测血管周围炎症浸润（PvIIs）26的存在，这被评估为疾病的征兆28。</li>
	</ol></li>
	<li>脊髓切片的定量分析
	<ol><li>使用连接到具有 20 倍物镜29 的数码相机的光学显微镜获取染色切片的图像。</li>
		<li>分析采集的图像以获得PvIIs的数量，表示为每mm2的浸润数。 注意：对于采集图像的分析，利用图像分析软件很有用。本研究中提出的神经病理学发现在每只小鼠 （n = 8/组） 的 10 个完整的脊髓横截面中量化，代表整个脊髓水平。</li>
	</ol></li>
</ol>

小鼠实验性自身免疫性脑脊髓炎的诱导和评价

<ol>
	<li>Thompson, A. J., Baranzini, S. E., Geurts, J., Hemmer, B., Ciccarelli, O. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Multiple+sclerosis.">Multiple sclerosis.</a> Lancet. 391 (10130), 1622-1636 (2018).</li><li>Gold, S. M., Willing, A., Leypoldt, F., Paul, F., Friese, M. A. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Sex+differences+in+autoimmune+disorders+of+the+central+nervous+system.">Sex differences in autoimmune disorders of the central nervous system.</a> Semin immunopathol. 41 (2), 177-188 (2019).</li><li>Smith, P. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Animal+models+of+multiple+sclerosis.">Animal models of multiple sclerosis.</a> Curr Protoc. 1 (6), 185 (2021).</li><li>Procaccini, C., De Rosa, V., Pucino, V., Formisano, L., Matarese, G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Animal+models+of+Multiple+Sclerosis.">Animal models of Multiple Sclerosis.</a> Eur J Pharmacol. 759, 182-191 (2015).</li><li>Torre-Fuentes, L., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Experimental+models+of+demyelination+and+remyelination.">Experimental models of demyelination and remyelination.</a> Neurologia. 35 (1), 32-39 (2020).</li><li>Kipp, M., Nyamoya, S., Hochstrasser, T., Amor, S. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Multiple+sclerosis+animal+models:+a+clinical+and+histopathological+perspective.">Multiple sclerosis animal models: a clinical and histopathological perspective.</a> Brain Pathol. 27 (2), 123-137 (2017).</li><li>Racke, M. K. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Experimental+autoimmune+encephalomyelitis+(EAE).">Experimental autoimmune encephalomyelitis (EAE).</a> Curr Protoc Neurosci. , (2001).</li><li>Constantinescu, C. S., Farooqi, N., O'Brien, K., Gran, B. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Experimental+autoimmune+encephalomyelitis+(EAE)+as+a+model+for+multiple+sclerosis+(MS).">Experimental autoimmune encephalomyelitis (EAE) as a model for multiple sclerosis (MS).</a> Br J Pharmacol. 164 (4), 1079-1106 (2011).</li><li>Montarolo, F., Perga, S., Martire, S., Bertolotto, A. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Nurr1+reduction+influences+the+onset+of+chronic+EAE+in+mice.">Nurr1 reduction influences the onset of chronic EAE in mice.</a> Inflamm Res. 64 (11), 841-844 (2015).</li><li>Montarolo, F., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Effects+of+isoxazolo-pyridinone+7e,+a+potent+activator+of+the+Nurr1+signaling+pathway,+on+experimental+autoimmune+encephalomyelitis+in+mice.">Effects of isoxazolo-pyridinone 7e, a potent activator of the Nurr1 signaling pathway, on experimental autoimmune encephalomyelitis in mice.</a> PLoS One. 9 (9), 108791 (2014).</li><li>Furlan, C., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Analysis+of+the+gadolinium+retention+in+the+experimental+autoimmune+encephalomyelitis+(EAE)+murine+model+of+multiple+sclerosis.">Analysis of the gadolinium retention in the experimental autoimmune encephalomyelitis (EAE) murine model of multiple sclerosis.</a> J Trace Elem Med Biol. 68, 126831 (2021).</li><li>Desole, C., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Engineering,+characterization,+and+biological+evaluation+of+an+antibody+targeting+the+HGF+receptor.">Engineering, characterization, and biological evaluation of an antibody targeting the HGF receptor.</a> Front Immunol. 12, 775151 (2021).</li><li>Voskuhl, R. R., MacKenzie-Graham, A. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Chronic+experimental+autoimmune+encephalomyelitis+is+an+excellent+model+to+study+neuroaxonal+degeneration+in+multiple+sclerosis.">Chronic experimental autoimmune encephalomyelitis is an excellent model to study neuroaxonal degeneration in multiple sclerosis.</a> Front Mol Neurosci. 15, 1024058 (2022).</li><li>McCombe, P. A., Greer, J. M. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Effects+of+biological+sex+and+pregnancy+in+experimental+autoimmune+encephalomyelitis:+It's+complicated.">Effects of biological sex and pregnancy in experimental autoimmune encephalomyelitis: It's complicated.</a> Front Immunol. 13, 1059833 (2022).</li><li>Ascherio, A., Munger, K. L. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Epidemiology+of+multiple+sclerosis:+from+risk+factors+to+prevention-an+update.">Epidemiology of multiple sclerosis: from risk factors to prevention-an update.</a> Semin Neurol. 36 (2), 103-114 (2016).</li><li>Spence, R. D., Voskuhl, R. R. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Neuroprotective+effects+of+estrogens+and+androgens+in+CNS+inflammation+and+neurodegeneration.">Neuroprotective effects of estrogens and androgens in CNS inflammation and neurodegeneration.</a> Front Neuroendocrinol. 33 (1), 105-115 (2012).</li><li>Laffont, S., Garnier, L., L&#233;lu, K., Gu&#233;ry, J. -. C. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Estrogen-mediated+protection+of+experimental+autoimmune+encephalomyelitis:+Lessons+from+the+dissection+of+estrogen+receptor-signaling+in+vivo.">Estrogen-mediated protection of experimental autoimmune encephalomyelitis: Lessons from the dissection of estrogen receptor-signaling in vivo.</a> Biomed J. 38 (3), 194-205 (2015).</li><li>Avila, M., Bansal, A., Culberson, J., Peiris, A. N. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=The+role+of+sex+hormones+in+multiple+sclerosis.">The role of sex hormones in multiple sclerosis.</a> Eur Neurol. 80 (1-2), 93-99 (2018).</li><li>Collongues, N., Patte-Mensah, C., De Seze, J., Mensah-Nyagan, A. -. G., Derfuss, T. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Testosterone+and+estrogen+in+multiple+sclerosis:+from+pathophysiology+to+therapeutics.">Testosterone and estrogen in multiple sclerosis: from pathophysiology to therapeutics.</a> Expert Rev Neurother. 18 (6), 515-522 (2018).</li><li>Kilkenny, C., Browne, W. J., Cuthill, I. C., Emerson, M., Altman, D. G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Improving+bioscience+research+reporting:+the+ARRIVE+guidelines+for+reporting+animal+research.">Improving bioscience research reporting: the ARRIVE guidelines for reporting animal research.</a> PLoS Biol. 8 (6), 1000412 (2010).</li><li>Shaw, M. K., Zhao, X., Tse, H. Y. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Overcoming+unresponsiveness+in+experimental+autoimmune+encephalomyelitis+(EAE)+resistant+mouse+strains+by+adoptive+transfer+and+antigenic+challenge.">Overcoming unresponsiveness in experimental autoimmune encephalomyelitis (EAE) resistant mouse strains by adoptive transfer and antigenic challenge.</a> J Vis Exp. (62), e3778 (2012).</li><li>Bittner, S., Afzali, A. M., Wiendl, H., Meuth, S. G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Myelin+oligodendrocyte+glycoprotein+(MOG35-55)+induced+experimental+autoimmune+encephalomyelitis+(EAE)+in+C57BL/6+mice.">Myelin oligodendrocyte glycoprotein (MOG35-55) induced experimental autoimmune encephalomyelitis (EAE) in C57BL/6 mice.</a> J Vis Exp. (86), (2014).</li><li>Downton, P., Early, J. O., Gibbs, J. E. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Circadian+rhythms+in+adaptive+immunity.">Circadian rhythms in adaptive immunity.</a> Immunology. 161 (4), 268-277 (2020).</li><li>McLean, A. C., Valenzuela, N., Fai, S., Bennett, S. A. L. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Performing+vaginal+lavage,+crystal+violet+staining,+and+vaginal+cytological+evaluation+for+mouse+estrous+cycle+staging+identification.">Performing vaginal lavage, crystal violet staining, and vaginal cytological evaluation for mouse estrous cycle staging identification.</a> J Vis Exp. (67), e4389 (2012).</li><li>Rahn, E. J., Iannitti, T., Donahue, R. R., Taylor, B. K. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Sex+differences+in+a+mouse+model+of+multiple+sclerosis:+neuropathic+pain+behavior+in+females+but+not+males+and+protection+from+neurological+deficits+during+proestrus.">Sex differences in a mouse model of multiple sclerosis: neuropathic pain behavior in females but not males and protection from neurological deficits during proestrus.</a> Biol Sex Differ. 5 (1), 4 (2014).</li><li>Bonaldo, B., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Effects+of+perinatal+exposure+to+bisphenol+A+or+S+in+EAE+model+of+multiple+sclerosis.">Effects of perinatal exposure to bisphenol A or S in EAE model of multiple sclerosis.</a> Cell Tissue Res. 392 (2), 467-480 (2023).</li><li>vanden Berg, R., Laman, J. D., van Meurs, M., Hintzen, R. Q., Hoogenraad, C. C. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Rotarod+motor+performance+and+advanced+spinal+cord+lesion+image+analysis+refine+assessment+of+neurodegeneration+in+experimental+autoimmune+encephalomyelitis.">Rotarod motor performance and advanced spinal cord lesion image analysis refine assessment of neurodegeneration in experimental autoimmune encephalomyelitis.</a> J Neurosci Methods. 262, 66-76 (2016).</li><li>Bolton, C., Smith, P. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Defining+and+regulating+acute+inflammatory+lesion+formation+during+the+pathogenesis+of+multiple+sclerosis+and+experimental+autoimmune+encephalomyelitis.">Defining and regulating acute inflammatory lesion formation during the pathogenesis of multiple sclerosis and experimental autoimmune encephalomyelitis.</a> CNS Neurol Disord Drug Targets. 14 (7), 915-935 (2015).</li><li>Glaser, J. R., Glaser, E. M. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Neuron+imaging+with+Neurolucida--a+PC-based+system+for+image+combining+microscopy.">Neuron imaging with Neurolucida--a PC-based system for image combining microscopy.</a> Comput Med Imaging Graph. 14 (5), 307-317 (1990).</li><li>Kennedy, H. S., Puth, F., Van Hoy, M., Le Pichon, C. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=A+method+for+removing+the+brain+and+spinal+cord+as+one+unit+from+adult+mice+and+rats.">A method for removing the brain and spinal cord as one unit from adult mice and rats.</a> Lab Anim (NY). 40 (2), 53-57 (2011).</li><li>Watson, C., Paxinos, G., Kayalioglu, G., Heise, C., Watson, C., Paxinos, G., Kayalioglu, G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Chapter+16+-+Atlas+of+the+mouse+spinal+cord.">Chapter 16 - Atlas of the mouse spinal cord.</a> The Spinal. , 308-379 (2009).</li><li>Khan, A., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Suppression+of+TRPV1/TRPM8/P2Y+nociceptors+by+withametelin+via+downregulating+MAPK+signaling+in+mouse+model+of+vincristine-induced+neuropathic+pain.">Suppression of TRPV1/TRPM8/P2Y nociceptors by withametelin via downregulating MAPK signaling in mouse model of vincristine-induced neuropathic pain.</a> Int J Mol Sci. 22 (11), 6084 (2021).</li><li>Bergamaschi, R. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Prognostic+factors+in+multiple+sclerosis.">Prognostic factors in multiple sclerosis.</a> Int Rev Neurobiol. 79, 423-447 (2007).</li><li>Harbo, H. F., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Genes+in+the+HLA+class+I+region+may+contribute+to+the+HLA+class+II-associated+genetic+susceptibility+to+multiple+sclerosis.">Genes in the HLA class I region may contribute to the HLA class II-associated genetic susceptibility to multiple sclerosis.</a> Tissue Antigens. 63 (3), 237-247 (2004).</li><li>Ryan, L., Mills, K. H. G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Sex+differences+regulate+immune+responses+in+experimental+autoimmune+encephalomyelitis+and+multiple+sclerosis.">Sex differences regulate immune responses in experimental autoimmune encephalomyelitis and multiple sclerosis.</a> Eur J Immunol. 52 (1), 24-33 (2022).</li><li>Lasrado, N., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Mechanisms+of+sex+hormones+in+autoimmunity:+focus+on+EAE.">Mechanisms of sex hormones in autoimmunity: focus on EAE.</a> Biol Sex Differ. 11 (1), 50 (2020).</li><li>Hofstetter, H. H., Shive, C. L., Forsthuber, T. G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Pertussis+toxin+modulates+the+immune+response+to+neuroantigens+injected+in+incomplete+Freund's+adjuvant:+induction+of+Th1+cells+and+experimental+autoimmune+encephalomyelitis+in+the+presence+of+high+frequencies+of+Th2+cells.">Pertussis toxin modulates the immune response to neuroantigens injected in incomplete Freund's adjuvant: induction of Th1 cells and experimental autoimmune encephalomyelitis in the presence of high frequencies of Th2 cells.</a> J Immunol. 169 (1), 117-125 (2002).</li><li>Maria, Z., Turner, E., Agasing, A., Kumar, G., Axtell, R. C. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Pertussis+toxin+inhibits+encephalitogenic+T-cell+infiltration+and+promotes+a+B-cell-driven+disease+during+Th17-EAE.">Pertussis toxin inhibits encephalitogenic T-cell infiltration and promotes a B-cell-driven disease during Th17-EAE.</a> Int J Mol Sci. 22 (6), 2924 (2021).</li><li>Krementsov, D. N., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Studies+in+experimental+autoimmune+encephalomyelitis+do+not+support+developmental+bisphenol+a+exposure+as+an+environmental+factor+in+increasing+multiple+sclerosis+risk.">Studies in experimental autoimmune encephalomyelitis do not support developmental bisphenol a exposure as an environmental factor in increasing multiple sclerosis risk.</a> Toxicol Sci. 135 (1), 91-102 (2013).</li><li>Kummari, E., Nichols, J. M., Yang, E. -. J., Kaplan, B. L. F. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Neuroinflammation+and+B-cell+phenotypes+in+cervical+and+lumbosacral+regions+of+the+spinal+cord+in+experimental+autoimmune+encephalomyelitis+in+the+absence+of+pertussis+toxin.">Neuroinflammation and B-cell phenotypes in cervical and lumbosacral regions of the spinal cord in experimental autoimmune encephalomyelitis in the absence of pertussis toxin.</a> Neuroimmunomodulation. 26 (4), 198-207 (2019).</li><li>Huntemann, N., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=An+optimized+and+validated+protocol+for+inducing+chronic+experimental+autoimmune+encephalomyelitis+in+C57BL/6J+mice.">An optimized and validated protocol for inducing chronic experimental autoimmune encephalomyelitis in C57BL/6J mice.</a> J Neurosci Methods. 367, 109443 (2022).</li></ol>

作者在本文的研究、作者身份和/或出版方面没有任何利益冲突需要声明。

我们描述的 MOG35-55 诱导的 EAE 方案导致 C57BL/6J 小鼠慢性 MS的发展 7,8,13。在这些具有代表性的结果中，我们报告说，接受免疫程序的男女动物都患上了慢性形式的疾病（即，它们在疾病发作后没有完全恢复，它们积累了缺陷，并且在慢性期保持CS至少为1.5）。
即使许多研究报告该模型1...

An erratum was issued for:&#160;<a href="https://www.jove.com/t/65778">Modeling Multiple Sclerosis in the Two Sexes: MOG35-55-Induced Experimental Autoimmune Encephalomyelitis</a>. The Authors section was updated. An additional affiliation (School of Pharmacy, Pharmacology Unit, University of Camerino) was added for author Antonino Casile.

An erratum was issued for:&#160;<a href="https://www.jove.com/t/65778">Modeling Multiple Sclerosis in the Two Sexes: MOG35-55-Induced Experimental Autoimmune Encephalomyelitis</a>. The Authors section was updated.

Erratum: Modeling Multiple Sclerosis in the Two Sexes: MOG35-55-Induced Experimental Autoimmune Encephalomyelitis

多发性硬化症（MS）是一种影响中枢神经系统（CNS）的慢性自身免疫性炎症性疾病。它显示存在炎症细胞的血管周围浸润、脱髓鞘、轴突缺失和胶质增生1。其病因尚不清楚，其临床方面、影像学和病理学特征表明该疾病具有显著的异质性2。
由于其病因和复杂性未知，目前尚无动物模型概括人类多发性硬化症中显示的所有临床和放射学特征 3,4。然而，采用各种动物模型来研究 MS 3,4 的不同方面。在这些模型中，疾病的发生通常是非常人为的，并且人类和小鼠之间临床症状发作的时间范围不同。例如，在人类中，在临床表现出现之前，疾病的病理生理过程多年未被发现。相反，实验者可以在 MS 诱导后的数周甚至数天内检测到动物模型的症状 4.
三种基本动物模型产生多发性硬化症特征的脱髓鞘特征：病毒诱导的特征（例如，泰勒氏鼠脑脊髓炎病毒）、毒性物质诱导的特征（例如铜酮、溶血卵磷脂）以及实验性自身免疫性脑脊髓炎 （EAE） 的不同变体5。每个模型都有助于研究疾病的某些特定方面，但没有一个模型可以复制MS6的所有特征。因此，考虑到具体的实验需求和要解决的科学问题，选择正确的模型至关重要。
由于针对髓鞘衍生抗原的免疫程序，EAE是通过触发易感小鼠对中枢神经系统成分的自身免疫反应来诱导的。广泛的免疫病理学和神经病理学机制之间的相互作用导致免疫小鼠中 MS 的主要病理特征（即炎症、脱髓鞘、轴突丢失和神经胶质增生）的发展 7,8。小鼠在免疫接种后第二周左右开始出现临床症状，通常表现出从尾巴到肢体和前肢的上行麻痹。临床评分（即疾病相关缺陷积累的量化）通常使用 5 分制7 进行评估。
蛋白质或肽的主动免疫或脑致癌 T 细胞的被动转移可用于在具有不同遗传背景的小鼠（例如 SJL/J、C57BL/6 和非肥胖糖尿病 （NOD） 小鼠）中诱导 EAE。髓鞘蛋白脂质蛋白 （PLP）、髓鞘碱性蛋白 （MBP） 和髓鞘少突胶质细胞糖蛋白 （MOG） 是通常产生免疫原的自身中枢神经系统蛋白的例子。特别是，用免疫显性 PLP 表位 （PLP139−151） 免疫的 SJL/J 小鼠发展为复发缓解 （RR） 病程，而用免疫显性 MOG35-55 肽免疫的 C57BL/6J 小鼠表现出慢性性质的 EAE 1。尽管存在一些局限性，例如提供有关 MS 进展、B 细胞在疾病中的作用、由内而外的机制或研究髓鞘再生的困难的信息很少，但 EAE 模型为理解自身免疫和神经炎症过程做出了巨大贡献，增加了 MS 领域的知识，从而允许开发针对这种疾病的新治疗方法4，6.
在本研究中，我们专注于一种特殊形式的活性 EAE，即髓鞘少突胶质细胞糖蛋白肽 35-55 （MOG35-55） 诱导的形式9、10、11、12。MOG35-55 诱导的 EAE 模拟了一种慢性 MS 形式。免疫后，小鼠在免疫后第一周内经历无症状阶段，然后疾病通常在免疫后的第二周出现，而在免疫后的第三周和第四周之间，疾病变成慢性的，不可能从累积的缺陷中完全恢复7,8,13.有趣的是，在文献中的大多数研究中，男性和女性在发病率、发病、病程或进展方面没有观察到差异14，即使比较男性和女性疾病的研究较少。
相比之下，在人类中，已知这些参数具有强烈的性别二态性 2。多发性硬化症影响女性多于男性;然而，男性通常会患上更具侵袭性的疾病2。这一证据表明，性腺激素起着重要而复杂的作用15;然而，性激素在病理学中的作用和作用机制仍不清楚。此外，来自动物模型的数据支持雌激素和雄激素都以性别特异性的方式对病理学的不同区域产生积极影响的观点16,17。
一些研究还表明黄体酮具有神经保护、早髓鞘和抗炎作用18 ，尽管 MS 患者的证据很少18，但神经活性类固醇（即神经系统 从头 合成的类固醇，如孕烯醇酮、四氢孕酮和二氢孕酮）也可能影响病理过程19.总的来说，这些数据支持这样一种观点，即外周和中枢神经系统内部产生的性激素在疾病发生和进展中具有重要的性别特异性作用。因此，在本工作中，我们敦促收集雄性和雌性动物的单独数据。
从组织病理学的角度来看，脊髓白质是该模型中 CNS 损伤的主要部位，其特征是单核炎症浸润和脱髓鞘的多灶性汇合区域8。因此，在描述该方案在C57BL / 6J小鼠中诱导MOG35-55诱导的EAE时，我们将考虑两性的疾病结果，并提供一些关于脊髓的组织病理学见解。

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			<td>18 G x 1 &#189;&#8220; 1.2 x 40 mm needle for the glass syringe&#160;</td>
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			<td>Digital camera connected to the optical microscope</td>
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			<td>Electronic precision balance</td>
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			<td>Mod. Kern-440-47N, resolution 0.1 g</td>
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			<td>Eosin Y</td>
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			<td>Glassware (i.e., becker to prepare the emulsion)</td>
			<td>VWR</td>
			<td>213-1170, 213-1172</td>
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			<td>Hematoxylin (Mayer&#8217;s)</td>
			<td>Sigma-Aldrich</td>
			<td>MHS32</td>
			<td>Filter before using it.&#160;</td>
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			<td>Image analysis Software</td>
			<td>Fiji</td>
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			<td>Incomplete Freund&#8217;s adjuvant (IFA)</td>
			<td>Sigma-Aldrich</td>
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			<td>Store at +4 &#176;C.&#160;</td>
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			<td>Isoflurane</td>
			<td>Wellona Pharma</td>
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			<td>This drug is used as inhalational anaesthetic.</td>
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			<td>Male and female C57BL/6J mice</td>
			<td>Jackson Laboratory, Envigo</td>
			<td></td>
			<td>Age 8-10 weeks, optimal body weight of ~20 g.&#160;</td>
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			<td>Microtome</td>
			<td>Leica HistoCore BIOCUT R</td>
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			<td>Merck</td>
			<td>107961</td>
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			<td>Ugo Basile&#160;</td>
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			<td>Mycobacterium tuberculosis (MT), strain H37Ra&#160;</td>
			<td>Difco Laboratories Inc.&#160;</td>
			<td>231141</td>
			<td>Store at +4 &#176;C.</td>
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			<td>Myelin oligodendrocyte glycoprotein peptide 35-55 (MOG35-55)</td>
			<td>Espikem</td>
			<td>EPK1</td>
			<td>Store at -80 &#176;C diluted (2 mg/mL) in physiological solution; prepare it on the day of the immunization to avoid, as much as possible, alterations or contaminations.&#160;</td>
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			<td>Optical microscope</td>
			<td>NIKON eclipse 90i</td>
			<td></td>
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			<td>Paraformaldehyde (PFA)</td>
			<td>Sigma-Aldrich</td>
			<td>158127</td>
			<td>Store at +4 &#176;C once diluted (4%) in phosphate buffer.&#160;</td>
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			<td>Pertussis toxin (PT)</td>
			<td>Duotech&#160;</td>
			<td>PT.181</td>
			<td>Store at -80&#176;C diluted (concentration 5 &#181;g/mL) in physiological solution&#160;</td>
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			<td>Physiological solution (sodium chloride 0.9% solution)</td>
			<td>B. Eurospital</td>
			<td>A 032182038</td>
			<td>Store at +4 &#176;C once opened.</td>
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			<td>Saline phosphate buffer (PBS)</td>
			<td>Thermo Scientific</td>
			<td>J61196.AP</td>
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			<td>Software for image acquisition</td>
			<td>&#160;NIS-Element AR 2.10</td>
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			<td>Syringes U-100 0.5 mL with 30 G x 5/16&#8221; (0.30 x 8 mm) in fixed needle</td>
			<td>&#160;Nipro</td>
			<td>SYMS-0.5U100-3008B-EC</td>
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			<td>Syringes U-100 1 mL with 26G x &#189;&#8221; (0.45 x 12.7 mm) in needle</td>
			<td>PIC</td>
			<td>20,71,26,03,00,354</td>
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			<td>Vet ointment for eyes</td>
			<td>Lacrilube, Lacrigel Europhta</td>
			<td></td>
			<td></td>
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			<td>Xylazine</td>
			<td>Rompun</td>
			<td></td>
			<td>This mixture of drug is used as injectable anaesthetic and sedative.&#160;</td>
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			<td>Zolazepam and Tiletamine</td>
			<td>Zoletil&#160; 100</td>
			<td></td>
			<td>This drug is used as injectable anaesthetic, sedative, muscle relaxer, and analgesic</td>
		</tr>
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modeling multiple sclerosis in the two sexes: mog35-55-induced experimental autoimmune encephalomyelitis

多发性硬化症（MS）是一种影响中枢神经系统（CNS）的慢性自身免疫性炎症性疾病。它的特点是两性患病率不同，影响的女性多于男性，结果也不同，男性比女性更具侵略性。此外，多发性硬化症在临床方面、影像学和病理学特征方面具有高度异质性。因此，有必要利用实验动物模型，以尽可能多地研究病理学的各个方面。实验性自身免疫性脑脊髓炎 （EAE） 是小鼠中最常用的 MS 模型之一，模拟了不同的疾病特征，从免疫系统的激活到中枢神经系统损伤。在这里，我们描述了使用髓鞘少突胶质细胞糖蛋白肽35-55（MOG35-55）免疫在雄性和雌性C57BL / 6J小鼠中诱导EAE的方案，这导致慢性疾病的发展。我们还报告了免疫接种后28天（28 dpi）对这些小鼠的每日临床评分和运动表现的评估。最后，我们说明了中枢神经系统水平的一些基本组织学分析，重点关注脊髓作为疾病诱导损伤的主要部位。

Multiple Sclerosis (MS) is a chronic autoimmune inflammatory disease affecting the central nervous system (CNS). It shows the presence of perivascular infiltration of inflammatory cells, demyelination, axonal loss, and gliosis1. Its etiology remains unknown, and its clinical aspects, radiographic, and pathological features suggest remarkable heterogeneity in the disease2.
Due to its unknown etiology and complexity, at present, no animal model recapitulates all the clinical and radiological features displayed in human MS3,4. However, various animal models are employed to study different aspects of MS3,4. In these models, disease initiation is typically extremely artificial, and the timeframe of the onset of clinical signs is different between humans and mice. For example, in humans, the pathophysiological processes underlying the disease are undetected for years before the onset of clinical manifestations. Conversely, the experimenters can detect symptoms in animal models within weeks or even days after MS induction4.
Three basic animal models produce the features of demyelination that are characteristic of MS: those that are virus-induced (e.g., Theiler&#39;s murine encephalomyelitis virus), those that are induced by toxic agents (e.g., cuprizone, lysolecithin), and the different variants of experimental autoimmune encephalomyelitis (EAE)5. Each model helps study some specific facets of the disease but none replicates all the features of MS6. Thus, it is critical to choose the correct model considering the specific experimental needs and the scientific questions to be addressed.
Thanks to immunization procedures against myelin-derived antigens, EAE is induced by triggering an autoimmune response to CNS components in susceptible mice. The interplay between a wide range of immunopathological and neuropathological mechanisms causes the development of principal pathological traits of MS (i.e., inflammation, demyelination, axonal loss, and gliosis) in the immunized mice7,8. Mice begin to show clinical symptoms around the second week after immunization and generally show ascending paralysis from the tail to the limb and forelimb. The clinical score (i.e., quantification of the accumulation of disease-related deficits) is generally assessed using a 5-point scale7.
Active immunization with protein or peptide or passive transfer of encephalitogenic T cells can be used to induce EAE in mice with different genetic backgrounds (e.g., SJL/J, C57BL/6, and non-obese-diabetic (NOD) mice). Myelin proteolipid protein (PLP), myelin basic protein (MBP), and myelin oligodendrocyte glycoprotein (MOG) are examples of self-CNS proteins from which immunogens are usually produced. Particularly, SJL/J mice immunized with the immunodominant epitope of PLP (PLP139&#8722;151) develop a relapsing-remitting (RR) disease course, while C57BL/6J mice immunized with the immunodominant MOG35-55 peptide show EAE of a chronic nature1. Despite some limitations, such as providing very little information about MS progression, the role of B cells in the disease, the inside-out mechanisms, or difficulties in studying remyelination, the EAE models have hugely contributed to the understanding of autoimmune and neuroinflammatory processes, increasing the knowledge in the MS field and thus allowing the development of novel therapeutic approaches for this disease4,6.
In the present work, we focused on a particular form of active EAE, the myelin oligodendrocyte glycoprotein peptide 35-55 (MOG35-55)-induced form9,10,11,12. The MOG35-55-induced EAE models a chronic form of MS. After immunization, the mice undergo an asymptomatic phase within the first week after immunization, then the disease typically arises during the second week after immunization, while between the third and fourth weeks after immunization, the disease becomes chronic, with no possibility of full recovery from the accumulated deficits7,8,13. Interestingly, no differences between males and females in incidence, disease onset, course, or progression are observed in most of the studies present in the literature14, even if fewer studies compare the disease in males and females.
In contrast, in humans, these parameters are known to be strongly sexually dimorphic2. MS affects more women than men; however, men generally develop a more aggressive form of the disease2. This evidence has suggested an essential, as well as complex, role of the gonadal hormones15; nevertheless, the role and the mechanism of action of sex hormones in the pathology remain unclear. Moreover, data from animal models support the idea that both estrogens and androgens exert positive effects on different tracts of the pathology in a sex-specific manner16,17.
Some studies also suggest neuroprotective, promyelinating, and anti-inflammatory effects of progesterone18 and, although evidence in MS patients is scarce18, neuroactive steroids (i.e., de novo synthetized steroids by the nervous system, such as pregnenolone, tetrahydroprogesterone, and dihydroprogesterone) might also affect the pathological course19. Collectively, these data support the idea that sex hormones produced both peripherally and inside the CNS have an important and sex-specific role in disease onset and progression. Therefore, in the present work, we urge the collection of separate data from both male and female animals.
From the histopathological point of view, the white matter of the spinal cord serves as the principal site of CNS injury in this model, which is characterized by multifocal, confluent regions of mononuclear inflammatory infiltration and demyelination8. Thus, in describing this protocol for the induction of MOG35-55-induced EAE in C57BL/6J mice, we will take into account the disease outcome in the two sexes and provide some histopathological insights regarding the spinal cords.

作者聚焦：创建与雄性和雌性小鼠相关的多功能实验性自身免疫性脑脊髓炎模型 

两性多发性硬化症建模：MOG35-55 诱导的实验性自身免疫性脑脊髓炎

Our research focuses on the experimental autoimmune encephalomyelitis, or EAE model, which can significantly announce the understanding of peripheral immune-mediated mechanism and evaluate neuroinflammatory and partially delineating processes. This model has also been widely used to develop and test a wide range of therapeutics drugs. Due to the unknown etiology and complexity of multiple sclerosis, no animal model currently recapitulates all the clinical and radiological features displayed in humans.Thus, it is quite challenging for the researchers to select the animal model most fitting for a specific experimental question. EAE is a widely used model of multiple sclerosis. However, to do several issue, only some studies performing this model considered both sexes.With our protocol, we want a light possibility of including both sexes in the study conducted in this model. Specifically, our protocol proposed a clinical evaluation based of two methods:the clinical score assessment and the rotator test, leading a more quantitative, less subjective and more precise clinical assessment of the disease course. Even though this model does not entirely reproduce the sexual dimorphism of multiple sclerosis, it has potential advantages.The combination of the induction with other possible risk factor, especially the environmental ones, can end in understanding specific effects of such factors and identifying the specific role in some sexually dimorphic aspect of the disease.

免疫接种后的EAE随访 评估如下。
体重和食物摄入量 双因素方差分析（ANOVA）（性别和时间作为自变量）显示，两性EAE动物的BW均有所下降，尤其是在诱导后第二周内（F（1,57）= 4.952，p < 0.001; 图2A）。然而，BW中的性二态性始终保持不变（图2A）。就 BW 的百分比而言 （F（1,5...

Watch this Scientific Journal Video about Creating a Versatile Experimental Autoimmune Encephalomyelitis Model Relevant for Both Male and Female Mice at JoVE.com

实验性自身免疫性脑脊髓炎是多发性硬化症使用最广泛的小鼠模型之一。在目前的方案中，两性的C57BL / 6J小鼠都用髓鞘少突胶质细胞糖蛋白肽免疫，主要导致尾巴和四肢的上行麻痹。在这里，我们讨论EAE诱导和评估的协议。

Multiple Sclerosis (MS) is a chronic autoimmune inflammatory disease affecting the central nervous system (CNS). It is characterized by different ...

我们的研究重点是实验性自身免疫性脑脊髓炎或EAE模型，该模型可以显着宣布对外周免疫介导机制的理解，并评估神经炎症和部分描述过程。该模型也被广泛用于开发和测试各种治疗药物。由于多发性硬化症的病因和复杂性不明，目前尚无动物模型概括人类表现出的所有临床和放射学特征。因此，对于研究人员来说，选择最适合特定实验问题的动物模型是相当具有挑战性的。EAE是一种广泛使用的多发性硬化症模型。然而，为了解决几个问题，只有一些执行该模型的研究考虑了两性。通过我们的协议，我们希望在该模型中进行的研究中包括两性的可能性很小。具体而言，我们的方案提出了基于临床评分评估和旋转器测试两种方法的临床评估，从而对病程进行更定量、更少主观和更精确的临床评估。尽管该模型不能完全再现多发性硬化症的性别二态性，但它具有潜在的优势。诱导与其他可能的危险因素，特别是环境因素的结合，可以最终了解这些因素的具体影响，并确定在疾病的某些性别二态性方面的具体作用。

modeling-multiple-sclerosis-two-sexes-mog35-55-induced-experimental

Research

JoVE Journal

Neuroscience

Modeling Multiple Sclerosis in the Two Sexes: MOG35-55-Induced Experimental Autoimmune Encephalomyelitis

739 次观看.  Neuroscience Institute Cavalieri Ottolenghi (NICO). 我们的研究重点是实验性自身免疫性脑脊髓炎或EAE模型，该模型可以显着宣布对外周免疫介导机制的理解，并评估神经炎症和部分描述过程。该模型也被广泛用于开发和测试各种治疗药物。由于多发性硬化症的病因和复杂性不明，目前尚无动物模型概括人类表现出的所有临床和放射学特征。因此，对于研究人员来说，选择最适合特定实验问题的动物模型是相当具有挑战?...