甘油脱水酶gldC基因克隆、表达与鉴定

目的 :表达及纯化甘油脱水酶γ亚基蛋白。方法 :使用PCR及DNA重组技术 ,将甘油脱水酶γ亚基基因gldC重组到含麦芽糖结合蛋白 (MBP)的融合蛋白表达载体pMAL -c2x中 ,在大肠杆菌中进行表达。结果 :转化重组质粒pMAL gldC的大肠杆菌经IPTG诱导 ,SDS -PAGE分析显示表达出的MBP -gldC融合蛋白相对分子质量约 6 6kD ,与预期大小一致 ,并经Westernblot分析证实。用直链淀粉树脂亲和层析纯化得到电泳均一的融合蛋白。结论 :成功地获得甘油脱水酶γ亚基融合蛋白 。

GLDC基因复合杂合突变致非经典型非酮性高甘氨酸血症家系的临床和遗传学分析

非酮性高甘氨酸血症(NKH)是由甘氨酸裂解系统缺陷引起的常染色体隐性遗传疾病,分经典型和非经典型,而非经典型表现复杂多样,诊断较为困难。该文报道1个NKH家系,父母表型正常,兄妹均非新生儿期起病,哥哥表现为难治性癫癎、严重的双侧痉挛性瘫痪和智力低下,血和脑脊液的甘氨酸浓度增高,尿甘氨酸与肌酐的比值增高,脑脊液与血甘氨酸浓度的比增高;妹妹表现为语言发育迟缓、共济失调、舞蹈病和发热诱发的精神行为异常和肌张力减退,脑脊液甘氨酸浓度增高、脑脊液与血甘氨酸浓度比增高。高通量测序提示兄妹均存在GLDC基因母源c.3006C>G(p.C1002W)错义突变和父源c.1256C>G(p.S419X)无义突变,生物学软件预测均提示致病突变。转染两种突变体GLDC基因的H293T细胞甘氨酸脱羧酶活性均有下调。NKH表型多样,二代高通量测序有利于疑似病例的确认,非经典NKH与基因突变导致的甘氨酸脱羧酶活性下调相关。

以婴儿癫痫伴游走性局灶性发作的非酮症性高甘氨酸血症1例报告

报告1例遵义医科大学附属医院确诊的以婴儿癫痫伴游走性局灶性发作(EIMFS)的非酮症性高甘氨酸血症(NKH)患儿的临床特点。该男性患儿年龄2个月零14 d,出生后3 d起病,临床以癫痫发作、嗜睡、反应差及肌无力起病,头颅影像学提示大脑白质多发异常信号,脑电图示多部位起始的局灶性发作伴游走,加用丙戊酸钠治疗后发作加重。血尿代谢提示甘氨酸增高,患儿及其父母的全外显子测序发现患儿GLDC基因复合杂合变异:c.2528_2530del(p.Arg843del)/c.1969A>G(p.Ser657Gly)。突变基因分别来自父母。该患儿最终确诊为NKH,停用丙戊酸钠改为奥卡西平治疗后发作无减少,但吃奶有所改善。通过对该病例的报告,扩大EIMFS的病因及NKH的表型,提高临床医生对该病的认识。对新生儿起病的肌无力、呼吸衰竭及癫痫发作的患儿需考虑NKH可能,此类患儿应避免使用丙戊酸钠。另外对于KCNT1、SLC12A5等基因阴性的早发EIMFS,有显著脑病者也需警惕NKH可能,血尿代谢筛查及全外显子检测能提供早期诊断,指导合理治疗及优生优育。

Clinical and genetic analysis of nonketotic hyperglycinemia:A case report

BACKGROUND Nonketotic hyperglycinemia(NKH)is a rare autosomal recessive genetic disorder of abnormal glycine metabolism caused by insufficient activity of the glycine cleavage enzyme system.Glycine is believed to function mainly as an inhibitory neurotransmitter,but it can also act as a co-agonist of the N-methyl-D-aspartate(NMDA)receptor.The accumulation of a large amount of glycine in the brain leads to neuronal and axonal injury via overactivation of NMDA receptors located in the hippocampus,cerebral cortex,olfactory bulb,and cerebellum and to stimulation of the inhibitory function of glycine receptors located in the spinal cord and brain stem,resulting in central apnea,hiccups,and hypotonia in the early stage of the disease.CASE SUMMARY The child described in this report had typical clinical manifestations of NKH,such as hiccups,disturbance of consciousness,hypotonia,and convulsions,within the first week after birth.Whole-exome genetic testing revealed that the child had a compound heterozygous mutation,namely,c.395C>A(p.S132X)and c.2182G>A(p.G728R),in the GLDC gene,and he was diagnosed with NKH.For treatment,we administered an oral levetiracetam solution and added topiramate and prednisone for epilepsy control,but the epilepsy remained uncontrollable.Ketogenic diet therapy was started at 6 mo of age,his seizures were significantly reduced,and there were no obvious adverse reactions during ketogenic treatment.Furthermore,we found that with the development of the disease,high levels of serum glycine decreased or even disappeared without intervention,and as the disease progressed,the corpus callosum became dysplastic.CONCLUSION This case shows that plasma glycine levels cannot be used to evaluate the prognosis of NKH,that the development of the corpus callosum can be affected by NKH,and that a ketogenic diet may be effective for seizure control in NKH patients.

新生儿非酮症性高甘氨酸血症1例并文献复习

目的:探讨新生儿非酮症性高甘氨酸血症(nonketotic hyperglycinemia,NKH)的临床表型和基因型特点。方法:对苏州大学附属儿童医院收治的1例重症NKH患儿临床资料进行回顾性分析。并以“甘氨酸裂解酶”、“甘氨酸脱羧酶”、“非酮症性高甘氨酸血症”、“甘氨酸脑病”为关键词,检索中国知网、维普数据库、万方数据库和中华医学期刊全文数据库,以“glycine cleavage enzyme”、“glycine decarboxylase”、“nonketotic hyperglycinemia”、“glycine encephalopathy”为关键词检索生物医学文献数据库、web of science数据库和Embase数据库,检索时间自建库至2022年12月31日。总结新生儿NKH的临床表型和基因型特点。结果:本例患儿生后第2天出现反应差、纳差,继而出现阵发性惊厥、呼吸不规则,需要机械通气,于3周龄死亡。全外显子组基因测序发现GLDC基因中有两个复合杂合变异,分别为母源的c.848C>G(p.A283G)和父源的c.1607G>A(p.R536Q),前者为未报道过的变异。检索国内外文献共收集到基因变异所致新生儿NKH 53例,加上本例共54例。NKH患儿主要表现为纳差、肌张力减低、呃逆、进行性嗜睡、呼吸不规则或呼吸暂停、新生儿惊厥。54例变异序列中GLDC基因变异42例(77.8%),AMT基因变异9例(16.7%),LIAS基因变异2例(3.7%),GCSH基因变异1例(1.9%)。结论:新生儿NKH临床表现多样,以神经系统表现最多见,GLDC基因变异为主要致病变异。

1个非酮性高甘氨酸血症家系的临床和分子遗传学分析

非酮性高甘氨酸血症(NKH)是一种罕见的先天性遗传代谢性疾病,该文报道1例GLDC基因突变所致NKH的中国患儿,就其临床经过、基因缺陷进行研究。患儿以早发性代谢性脑病以及大田原综合征起病,血、尿串联质谱分析均未见异常,颅脑MRI提示胼胝体发育欠佳,脑电图提示爆发抑制。目标基因捕获下代测序结合多重连接探针扩增发现,患儿存在GLDC基因的母源外显子15 c.1786 C>T(p.R596X)杂合无义突变及父源外显子4-15大片段杂合缺失,均为明确致病突变,确诊为NKH。经过促肾上腺皮质激素、托吡酯、右美沙芬治疗后,患儿病情无好转,4月龄死亡。NKH临床表型复杂,可通过代谢筛查以及分子遗传学分析获得确诊。

甘氨酸脑病两例

本文报道2例新生儿期发病的甘氨酸脑病患儿,主要表现为反应差、肌张力低下、呼吸节律改变、惊厥及打嗝等,并且症状在短期内进行性加重,治疗效果差,均因呼吸衰竭死亡。基因检测分别发现GLDC基因和AMT基因突变,均为甘氨酸脑病的致病基因。新生儿期发病的甘氨酸脑病预后差、病死率高,临床医生应提高对该病的认识。