Atypical Guillain-Barrésyndrome with positive anti-sulfatide,anti-GT1b,and anti-GT1a antibodies:A case report

BACKGROUND The role of diverse antibodies in mediating peripheral nerve injury in Guillain-Barrésyndrome(GBS)is becoming clearer,but positivity for multiple antibodies in one case is uncommon.To our knowledge,this is the first case involving GBS with positive anti-sulfatide,anti-GT1a,and anti-GT1b antibodies.CASE SUMMARY A 20-year-old female patient was admitted to the hospital due to weakness of limbs for 5 d,and deterioration of the weakness and muscle aches for 1 d.The patient's limbs were weak,but the tendon reflexes in the part of the limbs were normal.There was no comorbid peripheral nociception or deep sensory dysfunction.She was diagnosed with GBS and was discharged after receiving intravenous human immunoglobulin pulse therapy.CONCLUSION In this article,the clinical manifestations,neurophysiological examination,and auxiliary examination findings of a GBS patient positive for multiple antibodies were analyzed to improve the identification of the disease by clinical physicians at an early stage.

A Case Report of Recurrent Guillain-Barré Syndrome with Orthostatic Hypotension Syncope as the First Symptom

Guillain⁃Barré syndrome (GBS) is an immune-mediated peripheral neuropathy with acute or subacute onset of flaccid paralysis of the limbs with symmetrical hypesthesia and autonomic nerve involvement [1]. The clinical manifestations of autonomic nerve damage are complex and varied, which may involve extensive or limited autonomic function damage, including abnormalities of the skin, pupil, urinary tract, gastrointestinal tract, cardiovascular system, body temperature, lacrimal and salivary glands, and sexual function, etc. [2], and some patients may even have autonomic nerve damage as the only symptom, which is a variant of GBS and is prone to misdiagnosis or underdiagnosis. Recurrence of GBS is rare, and the manifestations of recurrence are often similar to those of the first symptoms [3], but the patient admitted to our hospital had syncope as the main clinical manifestation of recurrence, which was completely different from that of the first incidence, and syncope is not a common and typical clinical manifestation of GBS, so misdiagnosis is highly likely.

Guillain-Barré综合征患者临床及脑脊液细胞学特点

目的探讨Guillain-Barré综合征(GBS)患者临床及CSF细胞学特点。方法回顾性分析37例GBS患者的临床资料。结果本组患者急性起病33例,亚急性起病4例。临床表现为四肢无力18例(48.6%),双下肢无力16例(43.2%),四肢麻木21例(56.8%),双侧面神经麻痹12例(32.4%),其他颅神经损害5例(13.5%),呼吸肌麻痹3例(8.1%),全自主神经功能障碍及Fisher综合征各1例(5.4%);变异型GBS 6例(16.2%)。腰穿CSF检查示4例(10.8%)患者压力高,11例(29.7%)细胞计数升高,29例(78.4%)蛋白升高,7例(18.9%)免疫球蛋白升高。34例(91.9%)CSF细胞学检查异常,22例(64.7%)患者表现为激活的淋巴细胞反应,12例(35.3%)以激活的单核细胞反应为主。感觉或运动神经传导异常25例(67.6%),F波或H反射异常33例(89.2%)。32例患者给予丙种球蛋白或血浆置换治疗,5例给予糖皮质激素治疗,均有效。结论 GBS多数表现为四肢对称性麻木、无力,部分为变异型。F波、H反射电生理检查早期异常率高。CSF细胞学检查早期以淋巴细胞反应为主,后期以单核细胞反应为主。

Guillain-Barré综合征患者中枢神经系统内源性免疫反应与脑脊液蛋白的相关性

目的探讨Guillain-Barré综合征(GBS)患者CNS内源性免疫反应与CSF蛋白的关系及临床意义。方法收集69例GBS患者的临床资料,采用免疫散射比浊法测定CSF和血清免疫球蛋白G(Ig G)、白蛋白水平,计算CSF白蛋白/血清白蛋白(QALB)、Ig G指数、24 h鞘内Ig G合成率。结果 CSF蛋白正常与偏高患者性别、年龄、残疾量表评分、上呼吸道感染、胃肠感染、肺部感染、近期疫苗接种比率差异无统计学意义。CSF蛋白正常患者CSF蛋白、QALB、Ig G、24 h鞘内Ig G合成率均显著低于CSF蛋白异常患者(均P<0.01),Ig G指数差异无统计学意义。24 h鞘内Ig G合成率正常患者CSF蛋白[0.49(10.84)]g/L显著低于偏高患者[0.98(12.97)]g/L(U=205.50,P<0.01)。24 h鞘内Ig G合成率与CSF蛋白呈正相关(r=0.599,P<0.01)。结论 GBS患者CSF蛋白水平随CNS内源性免疫反应增强而增加,24 h鞘内Ig G合成率有助于GBS的病情监测及预后评估。

MBP、IL-16在Guillain-Barré综合征发病中的机制

目的探讨髓鞘碱性蛋白(MBP)和白细胞介素16(IL-16)在Guillain-Barré综合征(GBS)发病过程中的变化。方法用ELISA法检测GBS组(36例)中MBP和IL-16的水平,并与多发性硬化(MS)组(45例)及对照组(33例)相比较。结果GBS、MS和对照组3组中CSFMBP的水平均明显高于SerumMBP的水平(P<0.01),而CSFIL-16的水平均明显低于SerumIL-16的水平(P<0.01)。GBS组CSF中MBP的水平明显高于对照组(P<0.01)但低于MS组(P<0.01),Serum中MBP水平和对照组相比无明显差异但低于MS组(P<0.01)。CSF中的IL-16水平明显高于对照组(P<0.05),但与MS组相比无明显差异,Serum中IL-16的水平低于对照组(P<0.01)但与MS组相比无明显差异。结论GBS发病早期神经根髓鞘的脱失可能更严重,中枢神经系统局部产生的IL-16参与了GBS神经根脱髓鞘的炎症过程。

EGRIS模型预测Guillain-Barré综合征患者呼吸衰竭风险的初步研究

目的探讨EGRIS模型对Guillain-Barré综合征(GBS)患者发生呼吸衰竭的预测价值。方法回顾性分析263例GBS患者的临床资料,按住院期间是否发生呼吸衰竭分为两组。绘制EGRIS预测呼吸衰竭的受试者工作曲线分析(ROC),计算曲线下面积(AUC)、最大约登指数时的评分临界值、灵敏度及特异度。结果本组中28例(10.6%)GBS患者发生呼吸衰竭。EGRIS模型显示了极好的预测能力(AUC=0.892, 95%CI:0.835～0.949,P<0.05);当EGRIS分值为3.5时约登指数最大,灵敏度为75%,特异度为85.1%。结论 EGRIS评分模型简便易行,能够在GBS早期准确识别发生呼吸衰竭的高危患者。

Guillain-Barré综合征患者HLA和TNF基因多态性的研究

目的 :探讨空肠弯曲菌 (Campylobacterjejuni,Cj)感染与Guillain Barr啨综合征 (GBS)的关系 ,以及Cj感染与抗 GM1抗体的关系 ;并进一步研究GBS患者人类白细胞抗原 (Humanleukocyteantigen ,HLA)和肿瘤坏死因子 (tumornecrosisfactor,TNF)基因的多态性。方法 :用ELISA方法检测 80例GBS患者血清中Cj的IgG、IgM、IgA抗体及抗 GM1抗体 ,同时从患者的大便中培养Cj;用改良的PCR 限制性片段长度多态性 (PCR RFLP)结合组间特异性引物法分别测定HLA DRB1和 DQB1基因的多态性 ;用PCR和微卫星方法测定TNFα等位基因的多态性。结果 :GBS患者Cj感染率为 5 1.3% ,抗 GM1抗体检出率为 42 .5 % ;近期Cj感染者抗 GM1抗体检出率 ( 6 3.4% )显著高于未感染者 ( 2 0 .5 % ) (P <0 .0 0 1) ;GBS与HLA DR及 DQ等位基因无明显相关性 (P >0 .0 5 ) ,而与TNFα2等位基因有显著相关性 (P <0 .0 5 )。结论 :Cj感染是GBS的重要诱发因素之一 ,血清中抗 GM1抗体的存在与近期Cj感染有关 ;TNFα2等位基因可能是GBS的易感基因。

Guillain-Barré综合征患者B淋巴细胞辅助受体CD l9表达的研究

目的本研究通过检测Guillain-Barre综合征(GBS)患者外周血单个核细胞CD l9蛋白的表达,探讨CD l9与GBS及其严重程度之间的关系。方法利用流式细胞术检测GBS组(36例)和正常对照组(20例)的CD l9蛋白表达,按病程将GBS组分为急性期亚组与恢复期亚组,并分析与疾病严重程度之间的关系。结果与正常对照组221±78个比较,GBS组742±128个B细胞数量显著升高,差异有统计学意义(P<0.01)。与正常对照组62.21±7.85%比较,GBS组83.92±6.23%CD l9+CD20+显著升高,差异有统计学意义(P<0.01)。与恢复期GBS组686±108个比较,急性期GBS组810±124个B细胞数量无明显差异(P>0.05)。与恢复期GBS组87.27±6.04%比较,急性期GBS组81.20+5.25%CD l9+CD20+无明显差异(P>0.05)。与轻症GBS组632+68个比较,重症GBS组797+130个B细胞数量无明显差异(P>0.05)。与轻症GBS组82.53+5.03%比较,重症GBS组85.84+6.77%CD l9+CD20+无明显差异(P>0.05)。结论 CD l9在GBS中表达显著升高,但与病程和病情严重程度无关。

伴低钠血症脑脊液抗Sufatide抗体阳性Guillain-Barré综合征的临床特点(附1例报告)

目的探讨伴低钠血症CSF抗Sufatide抗体阳性Guillain-Barré综合征(GBS)的临床特点及诊疗经验。方法回顾性分析1例伴低钠血症CSF抗Sufatide抗体阳性GBS的临床资料,并通过文献检索总结分析CSF抗Sufatide抗体阳性GBS患者的临床特点。结果文献检索收集2篇文献共2例CSF抗Sulfatide抗体阳性GBS患者的相关资料,结合本例病例共3例患者。患者均为男性,发病时间4~6 d。2例患者表现为四肢无力、剧烈腰背部及肢体疼痛,并出现CSF蛋白-细胞分离现象,使用人体免疫球蛋白治疗效果欠佳。并且本例患者使用人体免疫球蛋白后出现严重性低钠。1例患者表现为多脑神经损害,CSF蛋白轻度升高,使用人体免疫球蛋白后症状改善。结论以四肢无力为主要表现的CSF抗Sufatide抗体阳性GBS患者建议进行血浆置换,以防输注人体免疫球蛋白效果欠佳或导致顽固性低钠加重病情,进而影响预后。

Guillain-Barré综合征患者发生呼吸衰竭的预测量表

Guillain—Barre综合征（GBS）患者发生呼吸衰竭的比例大约占20％，此部分患者预后较差。80％患者发生呼吸衰竭在夜间，需紧急行气管插管，延迟插管则可能增加误吸而发生肺炎的风险，预后差。如果及早发现可能存在呼吸衰竭者，即可明确患者处理的优先级别，及时将这些患者收入监护室。目前已有两个有关GBS的预测研究，

Guillain-Barré综合征患者脑脊液蛋白水平与疾病严重性及预后的关系

目的总结Guillain-Barré综合征(GBS)患者CSF蛋白细胞分离现象(AD-CSF)的特点,分析GBS患者CSF蛋白水平与疾病严重性和预后的关系,探讨其临床意义。方法回顾性收集2007年1月至2016年10月在济宁医学院附属医院住院的206例GBS患者的一般临床资料(性别、年龄、前驱感染和电生理分类)、CSF细胞数和蛋白水平、高峰期及12个月后残疾评分(GDS),比较发病后≤7d、8~14d、15~21d、≥22d患者AD-CSF的阳性率。利用Pearson相关及Spearman相关分析电生理正常组、脱髓鞘型组、轴索型组、不能分型组患者CSF蛋白水平与高峰期及12个月后GDS的关系。结果患者发病第3周时腰穿的AD-CSF阳性率最高(85.7%),与其他时间点相比,差异有统计学意义(均P<0.001)。电生理正常组CSF蛋白水平与高峰期GDS呈正相关(r=0.707,P=0.003),与12个月后GDS无相关性;脱髓鞘型组CSF蛋白水平与高峰期及12个月后GDS均呈正相关(r=0.495,P=0.019;r=0.770,P<0.001)。回归分析表明,CSF蛋白水平是脱髓鞘型GBS患者高峰期GDS以及12个月后更高GDS的预测因子。结论GBS患者AD-CSF的阳性率与腰穿的时间密切相关;CSF蛋白水平可作为脱髓鞘型GBS高峰期疾病更重以及预后不良的预测因子。

ROC曲线在评价髓鞘碱性蛋白早期诊断Guillain-Barré综合征中的应用

目的运用受试者工作特征(ROC)曲线评价脑脊液(CSF)及血清(Serum)中髓鞘碱性蛋白(MBP)早期诊断Guillain-Barré综合征(GBS)的价值。方法用ELISA法检测GBS组(36例)中MBP的水平并和对照组(33例)相比较。运用ROC曲线评价CSF及Serum中MBP诊断GBS的敏感性及特异性。结果GBS组CSF中MBP的水平明显高于对照组(P<0.01),Serum中MBP水平和对照组相比差异无统计学意义。CSF MBP诊断GBS的ROC曲线下面积(AUC)为0.804±0.056,最佳分界值为0.65pg/mL。以CSF MBP≥0.65pg/mL来预测GBS,敏感性为80.6%,特异性为78.8%。Serum MBP ROC曲线的AUC为0.548±0.070,最佳分界值为0.20pg/mL。以Serum MBP≥0.20pg/mL来预测GBS,敏感性为44.4%,特异性为69.7%。两条曲线AUC的差异有统计学意义(P<0.01)。结论CSF MBP水平对诊断早期GBS有一定的准确性,可以作为早期诊断GBS较为敏感的指标。

Guillain-Barré综合征预后的评估及其预测因素

Guillain-Barre综合征（ GBS）是一种免疫介导的急性多发性周围神经病，年发病率约（1．1～1．8）／100000[1]。 GBS呈单向性病程，但患者的神经功能缺损程度和预后存在明显的个体差异，一些患者仅有轻度瘫痪，数周之内即自愈，而有些发病急、进展快、病情重，出现脑神经、呼吸肌以及四肢瘫痪，需长期机器辅助通气和卧床。仍有约20％的GBS患者死于并发症或遗留重度残疾[2]。如何对GBS患者的预后进行评估，识别可能预后不良的患者，给予更有效的治疗，对改善GBS患者的预后具有重要意义[2，3]。现对GBS患者预后的评估方法及其相关预测因素综述如下。

血浆纤维蛋白原、中性粒细胞/淋巴细胞比值评估Guillain-Barrés综合征严重程度的预测价值

目的探索血浆纤维蛋白原(FIB)及中性粒细胞/淋巴细胞比值(NLR)对Guillain-Barrés综合征(GBS)疾病严重程度的预测价值。方法选取蚌埠医学院第一附属医院2016年1月至2020年12月收治的109例GBS患者,根据住院免疫治疗前休斯功能分级量表(HFGS)分为轻度组66例及中重度组43例,比较两组年龄、性别、前驱感染史类型、发病至免疫治疗时间、免疫治疗前HFGS评分、血浆白蛋白、三酰甘油、C反应蛋白(CRP)、FIB、NLR等指标的差异。结果轻度组与中重度组之间年龄、白蛋白、三酰甘油、CRP、FIB、D-二聚体、中性粒细胞计数、淋巴细胞计数、NLR及血小板/淋巴细胞比值差异均有统计学意义(均P<0.05)。通过多因素Logstic回归分析血浆FIB和NLR水平是影响GBS患者疾病严重程度的独立危险因素(OR=10.78,P<0.05;OR=2.23,P<0.05)。ROC曲线显示,血浆FIB预测中重度GBS的曲线下面积是0.912,最佳截断点是3.61,灵敏度及特异性分别是90.7%、77.3%;NLR预测中重度GBS的曲线下面积是0.856,最佳截断点是4.11,灵敏度及特异性分别是72.1%、90.9%。Spearman相关分析结果显示,血浆FIB、NLR与免疫治疗前HFGS评分呈正相关(r=0.610,P<0.05;r=0.549,P<0.05)。结论血浆FIB、NLR对评估GBS疾病严重程度有良好的预测价值。

Guillain-Barré syndrome in a patient with multiple myeloma after bortezomib therapy: A case report

BACKGROUND Bortezomib is a first-line drug approved for patients with multiple myeloma (MM) and has significantly increased their overall survival. However, bortezomib-induced peripheral neuropathy (PN) remains a significant side effect that has led to its discontinuation in some patients. Guillain-Barré syndrome (GBS) is recognized as an immune-mediated PN characterized by the involvement of multiple nerve roots and peripheral nerves and albuminocytologic dissociation in cerebrospinal fluid (CSF) tests. Intravenous immunoglobulin (IVIG) and plasmapheresis are effective. CASE SUMMARY A 45-year-old man diagnosed with stage III MM (λ type) was treated with bortezomib and dexamethasone. Fourteen days after the second course, he complained of intense burning sensation in the lower limbs and hands, loss of tactile sensation, and pain in the distal area of both thighs and in the distal part of both wrist joints. Neurological examination revealed absence of knee and ankle reflexes. CSF examination revealed albuminocytologic dissociation. Nerve conduction studies indicated sensory nerve action potential amplitudes, conduction velocity decrease, and F wave latency prolongation. He was diagnosed as MM complicated with GBS. Subsequently, he was treated with high-dose IVIG (400 mg/kg/d for five days). His symptoms fully resolved without relapse at the 6-month follow-up. CONCLUSION Our case highlights the differential diagnosis and management of complications after bortezomib treatment in MM.

Guillain-Barrésyndrome following hepatitis E

Guillain-Barrésyndrome(GBS)is often triggered by a preceding bacterial or viral infection.Occasionally,it has been observed in association with acute hepatitis A,B and C,and three cases have been previously described in India in which GBS was associated with acute hepatitis E.A molecular mimicry mechanism is supposed to be involved in the pathogenesis of GBS triggered by infectious agents,although the nature of the shared epitopes has not been characterized in most instances,including that in the case of hepatotropic viruses.We report a case of GBS following acute hepatitis E in a European individual.The presence of antiganglioside GM2 antibodies in this patient suggested molecular mimicry involving ganglioside GM2 in the pathogenesis of GBS associated with hepatitis E.

急性Guillain-Barré综合征外周血TNF-α及sIL-2R的变化及发病机制探讨

目的 探讨肿瘤坏死因子(tumor necrosis factor-α,TNF-α)及可溶性白介素2受体(solubleinterleukln-2 receptor,sIL-2R)在急性 Guillain-Barre综合征(Guillain-Barre syndrome,GBS)免疫发病机制中的作用。方法 采用双抗体夹心 ELISA法,对30例急性GBS患者外周血TNF-α及sIL-2R水平进行检测,并与24例其他神经系统疾病患者及正常对照组进行比较。结果 急性CBS患者外周血TNF-α及SIL-2R水平明显升高,与正常对照组及其他神经系统疾病组比较差异有显著性意义(P<0.01);且外周血TNF-α水平的明显增高与GBS的病情进展有关。结论 急性GBS患者有多种细胞因子异常,TNF-α、SIL-2R可能参与了急性GBS的免疫发病机制过程。

Severe lumbar spinal stenosis combined with Guillain-Barrésyndrome:A case report

BACKGROUND Guillain-Barrésyndrome(GBS)is a rare disorder that typically presents with ascending weakness,pain,paraesthesias,and numbness,which mimic the findings in lumbar spinal stenosis.Here,we report a case of severe lumbar spinal stenosis combined with GBS.CASE SUMMARY A 70-year-old man with a history of lumbar spinal stenosis presented to our emergency department with severe lower back pain and lower extremity numbness.Magnetic resonance imaging confirmed the diagnosis of severe lumbar spinal stenosis.However,his symptoms did not improve postoperatively and he developed dysphagia and upper extremity numbness.An electromyogram was performed.Based on his symptoms,physical examination,and electromyogram,he was diagnosed with GBS.After 5 d of intravenous immunoglobulin(0.4 g/kg/d for 5 d)therapy,he gained 4/5 of strength in his upper and lower extremities and denied paraesthesias.He had regained 5/5 of strength in his extremities when he was discharged and had no symptoms during follow-up.CONCLUSION GBS should be considered in the differential diagnosis of spinal disorder,even though magnetic resonance imaging shows severe lumbar spinal stenosis.This case highlights the importance of a careful diagnosis when a patient has a history of a disease and comes to the hospital with the same or similar symptoms.

Guillain-Barré综合征患者空肠弯曲菌的主要外膜蛋白基因的分子分型(英文)

目的 :研究空肠弯曲菌 (Cj)的主要外膜蛋白 (momp)基因的分子分型。方法 :采用PCR方法对 163株空肠弯曲菌的主要外膜蛋白基因进行扩增 ,用HindⅢ ,HaeⅢ ,MboⅡ和HhaⅠ四种内切酶消化后进行电泳分析 ,并与热稳定性血清型 (HS)和鞭毛蛋白A基因 (flagellinAgene ,falA)分型方法相比较。结果 :共观察到 8种不同的主要外膜蛋白的限制性片段长度多态性的基因型 ,其中主要外膜蛋白基因 3 (momp 3 )占 61%。Guillain Barr啨综合征(GBS)和腹泻患者所有 3 4株HS 19:Cj(fla) 1菌株均属同一个单一基因型 ,即主要外膜蛋白基因 1(momp 1)。结论 :HS 19:Cj(fla) 1:momp 1菌株是空肠弯曲菌的一个特殊类型 ,与HS 19相关的GBS可能是阐明GBS发病机制最好的模型。