Comparison between recombinant human parathyroid hormone(1-34) and elcatonin in treatment of primary osteoporosis

Objective:To evaluate the efficacy and safety of rhPTH(1-34) vs.elcatonin.Methods:Sixty palients with primary OP were randomly divided into two groups according to the ratio of 3:1.rhPTH(1-34) group(PTH group) was treated with subcutaneous injection of rhPTH(1-34) 20 μg daily for 18 months,and the elcalonin group(CT group) was treated with intramuscular injection of elcatonin 20 U weekly for 12 months.Bone mineral density(BMD) of the lumbar spine 2-4(L_(2-4))and femoral neck,serum calcium and phosphorus,urinary calcium,serum hone specific alkaline phosphatase(BSAP).and urinary c-terminal telopeptides of type Ⅰ collagen/creatinine(uCTX-Ⅰ /Cn were tested at baseline,and 6.12.and 18 months after treatment.Results:In PTH group.HMD of L_(2-4),at 6,12.and 18 months,BDM of Femoral neck at 18 month,BSAP at 6 and 12 months and uCTX- Ⅰ /Cr at 6.12 and 18 months were all significantly raised.In CT group.HMD of L_(2-4) at12 month and that of femoral neck at 12 and 18 months were significantly elevated,while HSAP was significantly decreased at 12 and 18 months,and no significant difference on CTX- Ⅰ /Cr was observed.When BMD growth and growth rate between two groups were compared.PTH group had better improvement in L_(2-4) BMD and growth rate than CT group at 6.12.and 18 months.BMD growth and growth rale of femoral neck al 12 month and its growth at 18 month in CT group were higher than in PTH group,hut there was no significant difference between two groups regarding the growth rates at 18 month.Besides,there were no significant differences regarding the rales ol adverse reactions between two groups.Conclusions:rhPTH(1—34),is safe and effective in the treatment of primary OP.It is superior to elcatonin in improving vertebral HMD at onset time,growth rate and growth range,but inferior to elcatonin at HMD of femoral neck.

Safety,Tolerability and Pharmacokinetic Study of Recombinant Human Parathyroid Hormone [rhPTH(1-84)] in Chinese Healthy Volunteers

The current study was designed to determine the safety, tolerability and pharmacokinetic parameters of recombinant human parathyroid hormone [rhPTH （1-84）] used for the treatment of osteoporosis. In the single-dose format pharmacokinetic study, thirty-six healthy male volunteers received three dose levels of rhPTH （1-84） subcutaneously： 1, 2, and 4 μg/kg. The blood was timing drawn and the serum concentration of rhPTH （1-84） was determined by enzyme linked immunosorbent assay （ELISA）. Serum concentration-time curves of PTH （1-84） exhibited a double-peak pattern, the first peak appearing about 10 to 30 min after administration and the second peak occurring about 1.5 to2 h after administration. Serum terminal half-time of PTH （1-84） was approximately 2 h. The parameters indicated the serum levels were directly proportional to the administered dose, with the mean Cmax and AUC0_24 ranging from approximately 543.47 to 1845 pg/mL and 2358.6 to 9232.12 pg.h.mL^-1 over the dose range. The drug was well tolerated, the clinical symptoms were generally mild and of short duration.

A randomized, multicenter controlled trial to compare the efficacy of recombinant human parathyroid hormone （1-34） with elcatonin in postmenopausal women with osteoporosis in China

Background Recombinant human parathyroid hormone （1-34） （rhPTH （1-34）） given by injection is a new seventh class drug of biological products, which is prepared by adopting gene recombination technique, rhPTH （1-34） is mainly used to treat osteoporosis, especially for postmenopausal women. This study compared the clinical efficacy and safety of rhPTH （1-34） with elcatonin for treating postmenopausal women with osteoporosis in 11 urban areas of China. Methods Two hundred and five women with osteoporosis were enrolled in a 6-month, multicenter, randomized, controlled study. They were randomized to receive either rhPTH （1-34） 20 ug （200 U） daily or elcatonin 20 U weekly. Lumbar spine （L1-4） and femoral neck bone mineral density （BMD）, as well as biochemical markers of bone turnover were measured. Adverse events were recorded. Results rhPTH （1-34） increased lumbar BMD significantly more than did elcatonin at 3 months and 6 months （2.38% vs 0.59%, P 〈0.05; 5.51% vs 1.55%, P 〈0.01）, but there were no significant increases of BMD in these two groups at femoral neck. There were larger mean increases in bone markers in the rhPTH （1-34） group than in the elcatonin group at 3 months and 6 months （serum bone-specific alkaline phosphatase （BSAP） 36.79% vs 0.31%; 92.42% vs -0.17%; urinary N-telopeptide/creatinine （NTX/Cr） 48.91% vs -5.32%; 68.82% vs -10.86%）. Both treatments were well tolerated and there were no significant differences detected between the two groups in the proportion of any adverse events and any serious adverse events （67.0% vs 59.0%; 0 vs 0）. Conclusions rhPTH （1-34） has more positive effects on bone formation, as shown by the larger increments of lumbar BMD and bone formation markers, than elcatonin, with only mild adverse events and no significant change in the liver, kidney or hematological indices.

Comparison of parathyroid hormone （1-34） and elcatonin in postmenopausal women with osteoporosis： an 18-month randomized, multicenter controlled trial in China

Background Recombinant human parathyroid hormone （1-34） （rhPTH （1-34）） is the first agent in a unique class of anabolic therapies acting on the skeleton. The efficacy and safety of long-term administration of rhPTH （1-34） in Chinese postmenopausal women had not been evaluated. This study compared the clinical efficacy and safety of rhPTH （1-34） with elcatonin for treating postmenopausal women with osteoporosis in 11 urban areas of China. Methods A total of 453 postmenopausal women with osteoporosis were enrolled in an 18-month, multi-center, randomized, controlled study. They were randomized to receive either rhPTH （1-34） 20 μg （200 U） daily for 18 months, or elcatonin 20 U weekly for 12 months. Lumbar spine （L1-4） and femoral neck bone mineral density （BMD）, fracture rate, back pain as well as biochemical markers of bone turnover were measured. Adverse events were recorded. Results rhPTH （1-34） increased lumbar BMD significantly more than did elcatonin after 6, 12, and 18 months of treatment （4.3% vs. 1.9%, 6.8% vs. 2.7%, 9.5% vs. 2.9%, P 〈0.01）. There was only a small but significant increase of femoral neck BMD after 18 months （2.6%, P 〈0.01） in rhPTH groups. There were larger increases in bone turnover markers in the rhPTH （1-34） group than those in the elcatonin group after 6, 12, and 18 months （serum bone-specific alkaline phosphatase （BSAP） 93.7% vs. -3.6%; 117.8% vs. -4.1%; 49.2% vs. -5.8%, P 〈0.01; urinary C-telopeptide/creatinine （CTX/Cr） 250.0% vs. -29.5%; 330.0% vs. -41.4%, 273.0% vs. -10.6%, P 〈0.01）. rhPTH （1-34） showed similar effect of pain relief as elcatonin. The incidence of clinical fractures was 5.36% （6/112） in elcatonin group and 3.2% （11/341）in rhPTH （1-34）group （P=0.303）. Both treatments were well tolerated. Hypercaluria （9.4%） and hypercalcemia （7.0%） in rhPTH （1-34） group were transient and caused no clinical symptoms. Pruritus （8.2% vs. 2.7%, P=0.044） and redness of injection site （4.4% vs. 0,P=0.024） were more frequent in rhPTH （1-34）. Nausea/vomiting （16.1% vs. 6.2%, P=0.001） and hot flushes （7.1% vs. 0.6%, P 〈0.001） were more common in elcatonin group. Conclusions rhPTH （1-34） was associated with greater increases in lumbar spine BMD and bone formation markers. It could increase femoral BMD after 18 months of treatment, rhPTH could improve back pain effectively. The results of the present study indicate that rhPTH （1-34） is an effective, safe agent in treating Chinese postmenopausal women with osteoporosis. （ChiCTR- TRC-10000924）

重组人甲状旁腺激素(1-34)和依降钙素治疗原发性骨质疏松症的随机对照研究

目的评价重组人甲状旁腺激素(1-34)[rhPTH(1-34)]治疗原发性骨质疏松症(OP)的疗效和安全性,并与依降钙素进行对比。方法 60例原发性OP患者按3:1被随机分入rhPTH(1-34)组(PTH组)和依降钙素组(CT组)。PTH组予rhPTH(1-34)20μg每日1次皮下注射,连续用药18月。CT组予益钙宁20U每周1次肌肉注射,连续用药12月。受试前检测腰2-4椎体(L2-4)和股骨颈骨密度(BMD)、血钙、血磷、尿钙、血清骨特异性碱性磷酸酶(BSAP)、尿Ⅰ型胶原交基C端肽(CTX-I),治疗后6、12、18月复查上述指标。结果与基线时比较,PTH组L2-4BMD在治疗6、12、18月时显著升高,股骨颈BMD在18月时显著升高,BSAP在6、12月时均显著升高,CTX-I校正值在6、12、18月时均显著升高;CT组L2-4BMD在治疗12月前升高,股骨颈BMD在12、18月时升高,BSAP12、18月时均显著下降,CTX-I校正值治疗前后无统计学差异。两组比较,PTH组患者在6、12月和18月时L2-4的BMD增长值和增长率均高于CT组。但CT组在治疗12月时股骨颈BMD增长值高于PTH组,不良反应:两组差异无统计学意义;PTH组有一过性高钙血症。结论 rhPTH(1-34)治疗原发性OP安全有效,对改善椎体BMD起效时间、增长速度和增长幅度均优于依降钙素,但改善股骨颈BMD较依降钙素起效更慢,增长幅度更小。

重组人甲状旁腺激素(1-34)对体外培养成骨细胞骨形成的作用

目的 体外观察重组人甲状旁腺激素[recombinant human parathyroid hormone（1-34），rhPTH（1-34）]对成骨细胞骨形成的刺激作用。方法采用酶消化法分离获得大鼠成骨细胞，间隙加药方法给予rhPTH（1-34），观察药物对成骨细胞增殖、分化及矿化功能的影响。结果 10^-12～10^-8mol／L浓度对成骨细胞的增殖、分化和矿化功能均显示刺激作用。10^-11～10^-8mol／L浓度组的MTT、ALP的A值及矿化结节形态计量结果与对照组比较，具有显著性增加（P〈0．05），增加率以10^-9mol／L浓度组为最高，并呈剂量一效应关系。结论 rhPTH（1-34）对体外培养成骨细胞的增殖、分化和矿化功能具有明显促进作用。

注射用重组人甲状旁腺素(1-34)在健康人体的药代动力学

目的研究注射用重组人甲状旁腺素(1-34)[rhPTH(1-34)](激素)在中国健康人体内的药代动力学特征。方法30名健康受试者随机分为10,20,40μg3个剂量组,每组10人,用免疫放射测定法(IRMA)测定人血浆中甲状旁腺激素(PTH)浓度。结果药代动力学参数:tmax分别为(32.5±9.5),(24.0±9.7)和(35.0±13.5)min;Cmax分别为(0.14±0.04),(0.20±0.05)和(0.30±0.04)ng.mL-1;t1/2分别为(47.7±12.1),(50.1±16.4)和(53.6±14.4)min;AUC(0-240)分别为(9.79±1.46),(15.42±1.66)和(32.72±3.16)ng.min.mL-1。结论单次皮下注射重组人甲状旁腺素(1-34)在低、中、高3个剂量内,Cmax和AUC呈线性增长,与剂量呈正相关;体内代谢呈线性代谢特征,与国外报道基本一致。

注射用重组人甲状旁腺素(1-34)的Ⅰ期临床耐受性研究

目的:评价中国健康志愿者皮下注射重组人甲状旁腺素(1-34)的安全性和耐受性。方法:将40例18～40岁的健康受试者随机分为10,20和40μg 3个剂量组,腹部皮下注射,观察临床症状体征并严密观察记录试验期间发生的不良反应事件。结果:各组受试者体检及实验室检查各项指标均在正常范围,具较好的可比性。给药后生命体征和实验室检查均未见有临床意义的改变,试验中未见严重不良反应发生。结论:健康受试者皮下注射甲状旁腺素(1-34)40μg以内安全性和耐受性较好。

重组人甲状旁腺素（1-34）治疗原发性骨质疏松症疗效观察

目的 观察对比重组人甲状旁腺素（1-34）[PTH（1-34）]和降钙素对原发性骨质疏松症的疗效.方法 将20例原发性骨质疏松症患者随机分为试验组和对照组.试验组皮下注射PTH（1-34）20μg,每天1次;对照组肌肉注射降钙素20 IU,每周1次,两组均每日口服钙尔奇D 600mg,连续治疗6个月.所有患者于治疗前后枪测腰椎（L2～L4）、股骨颈骨密度、血钙及血清骨特异性碱性磷酸酶（BSAP）、血清I型胶原交基C端肽（CTX）、PTH等指标及观察有无不良反应.结果 治疗后PTH组和降钙素组腰椎（L2～L4）骨密度变化较治疗前均有明显增加,且有统计学意义.治疗后两组股骨颈骨密度变化较治疗前无明显改善（P〉0.05）,两组间比较无明显差异（P〉0.05）.PTH组BSAP变化值明显高于对照组,两组间比较差异有统计学意义（P〈0.01）;两组治疗后血、尿常规、肝、肾功能均未见明显异常.结论 PTH（1-34）与降钙素都能显著提高腰椎（L2～L4）骨密度,对于原发性骨质疏松症治疗安全有效.

胰岛素样生长因子-1对甲状旁腺激素介导成骨细胞增殖及成骨活性的影响

目的通过构建乳鼠颅盖骨成骨细胞分离培养与鉴定方法,研究胰岛素样生长因子-1(Insulin-like growth factor-1,IGF-1)及IGF-1联合重组人甲状旁腺激素1-34(recombinant human parathyroid hormone 1-34,rhPTH1-34)对成骨细胞增殖及I型胶原蛋白mRNA表达的影响。方法培养乳鼠成骨细胞,并观察其形态及功能,以原代培养乳鼠成骨细胞为实验模型,分空白组、PTH组、IGF-1组及不同浓度IGF-1作用的PTH介导的成骨细胞组(0、10、50、100 ng/L)。通过不同剂量的胰岛素样生长因子-1(0、10、50、100 ng/L)联合10-9mol/L重组人甲状旁腺素刺激体外培养的成骨细胞,用噻唑蓝(MTT)法检测细胞的增殖能力,RT-PCR法检测成骨细胞I型胶原蛋白mRNA的表达。结果 PTH和IGF-1均可促进成骨细胞增殖;IGF-1联合PTH可以促进成骨细胞增殖,且具有剂量依赖性。PTH联合IGF-1使成骨细胞增殖能力增强、I型胶原蛋白mRNA表达增强。IGF-1可以促进成骨细胞I型胶原蛋白mRNA的表达,且具有剂量依赖性。IGF-1可以促进成骨细胞I型胶原蛋白mRNA的表达,且具有剂量依赖性。结论 PTH与IGF-1均可刺激成骨细胞增殖和分化,IGF-1可促进PTH对成骨细胞的分化、增殖。两者合用其作用增强,有协同促进作用。

重组人甲状旁腺素1-34治疗绝经后骨质疏松症的临床研究

目的观察重组人甲状旁腺素1-34(recombinant human parathyroid hormone 1-34)应用于绝经后骨质疏松症(postmenopausal osteoporosis,PMOP)患者的临床疗效。方法筛选出68例绝经后骨质疏松症患者,所有患者入组后均口服元素钙500 mg/d和维生素D 200 U/d,连续服用26周后加用皮下注射重组人甲状旁腺素1-34(特立帕肽)20μg/d,再连续治疗26周,于应用特立帕肽治疗前及治疗后的13和26周测定腰椎(L_(1-4))和股骨近端骨密度(BMD),采静脉血测定血清骨钙素(OC)、碱性磷酸酶(AKP)水平,应用疼痛视觉模拟评分法(VAS评分)评价患者的疼痛程度,并记录不良反应情况。结果 68位患者均完成全疗程治疗。应用特立帕肽治疗13周时,腰椎L_(1-4)、股骨颈、大粗隆和股骨干骨密度改善不明显(P>0.05),血清骨钙素和碱性磷酸酶较治疗前升高(P<0.05),疼痛缓解明显(P<0.05);治疗26周时,腰椎L_(1-4)和股骨颈骨密度较治疗前明显增高(P<0.05),而大粗隆和股骨干骨密度改善不明显(P>0.05),血清骨钙素和碱性磷酸酶呈持续升高趋势(P<0.05),疼痛明显减轻(P<0.05)。治疗期间不良反应的情况均较轻微,没有给予特殊处理即自行缓解。结论连续26周使用重组人甲状旁腺素1-34能有效地促进患者骨形成,缓解骨质疏松症患者疼痛症状,提高患者腰椎、股骨骨密度。

重组人甲状旁腺素(1-34)与雌激素对去卵巢大鼠骨代谢的影响

目的观察重组人甲状旁腺素(1-34)与雌激素单用和联用对去卵巢大鼠骨代谢的影响。方法选用雌性4月龄SD大鼠45只,随机分为5组:①假手术(Sham)8只;②去卵巢(OVX)9只;③雌激素治疗组(OVX+E)10只:OVX2个月后给予苯甲酸雌二醇治疗6w;④PTH治疗组(OVX+PTH)9只:OVX2个月后给予rhPTH(1-34)治疗6w;⑤雌激素与PTH联合治疗组(OVX+E+PTH)9只:OVX2个月后给予rhPTH(1-34)和E2联合治疗6w。观察各组大鼠胫骨近端松质骨骨小梁形态计量学参数,椎体生物力学指标及部分血清骨生化代谢指标。结果雌激素治疗组和PTH治疗组的骨静态参数均表现为骨量增加;雌激素治疗组的骨形成参数和骨吸收参数降低;PTH治疗组的骨形成指标明显升高,而骨吸收指标虽较Sham高,但较OVX组有所降低;E2与PTH联合治疗组与单用E2组和单用PTH组比较,骨量明显提高,骨转换率参数介于单用E2和单用PTH组之间。3个治疗组的生物力学指标较OVX组均有明显提高,其中E2与PTH联合治疗组改善最明显。结论雌激素和PTH可使去卵巢大鼠松质骨骨量增加和改善生物力学性能,两者联合治疗有协同作用。

重组人甲状旁腺激素1-34多次皮下注射给药的人体药动学特征

目的研究健康志愿者多次皮下注射重组人甲状旁腺激素1-34[(rhPTH(1-34)]后体内的药动学特征。方法8名健康志愿者多次皮下注射rhPTH(1-34)后,采用放射免疫法测定血浆中rhPTH(1-34)浓度,评估它的药动学特性。结果rhPTH(1-34)的主要药动学参数如下:d 1,AUC0→t为(17103.3±2243.3)ng.min.L-1,AUC0→∞为(20471.3±2444.6)ng.min.L-1,ρmax为(171.2±34.2)ng.L-1,tmax为(38.1±15.1)min,t12为(55.7±3.9)min;d 7,AUC0→t为(17759.6±3781.5)ng.min.L-1,AUC0→∞为(20698.4±3374.6)ng.min.L-1,ρmax为(184.6±36.8)ng.L-1,tmax为(35.0±16.0)min,t12为(51.6±7.6)min,蓄积系数R为1.02±0.18。结论多次皮下注射rhPTH(1-34)后,与单次给药相比它在人体内的吸收、消除不随连续给药变化,药物在体内没有蓄积作用。rhPTH(1-34)的安全耐受性良好。性别对药动学参数没有影响。

绝经期骨质疏松患者PTH治疗后对骨硬化蛋白的影响及意义

目的观察更年期女性使用重组人甲状旁腺素(1-34)治疗后血清骨硬化蛋白(SO)水平的变化,探讨SO与雌二醇、骨密度等指标的相关性。方法选择更年期骨质疏松女性58例,更年期正常对照组50例。骨质疏松组皮下注射PTH 20 ug/d,同时口服钙片500 mg/d,分别于治疗6个月、12个月时检测患者血钙、磷、骨密度、血清ALP、雌二醇及SO等指标。结果治疗前骨质疏松组血清SO含量显著高于正常对照组,经rhPTH(1-34)治疗6个月和12个月后,骨质疏松组血清SO水平较治疗前均明显下降[6月时:(10.2±1.21)vs.(13.1±1.41)pg/mL;12月时:(7.81±1.12)vs.(13.1±1.41)pg/mL,P<0.05]。相关性分析显示,血清SO水平与雌二醇、骨密度呈负相关,与年龄、绝经年限呈正相关(P<0.05)。结论更年期骨质疏松患者血清SO水平明显升高,经rhPTH(1-34)治疗后血清SO水平显著下降。血清SO水平与雌二醇、骨密度密切相关,提示SO在更年期骨质疏松的发生发展中起着重要作用。

重组人甲状旁腺激素安全性药理学研究

目的:观察重组人甲状旁腺激素(rh-PTH)对大鼠心血管、呼吸系统和对小鼠神经系统的影响。方法:大鼠实验分高、中、低3个剂量及空白对照共4个组,给药组分别单次及连续7d皮下注射rh-PTH 160,80和40μg·kg^(-1),对血压、心电图(ECG)、呼吸频率及节律进行观察。小鼠实验分高、中、低3个剂量及空白对照共4个组,给药组分别单次及连续7d皮下注射rh-PTH 320,160,和80μg·kg^(-1),对动物自发活动和爬杆能力进行观察。结果:单次及连续7d皮下注射rh-PTH使大鼠收缩压、舒张压、平均动脉压降低,心率增加,且存在量效关系,但2h后上述指标基本恢复正常。对心律、ECG之QRS时间、T波、ST段、呼吸频率、节律和幅度无明显影响。对小鼠自发活动和爬杆能力无明显影响。结论:rh-PTH对心血管系统有一定影响,可使收缩压、舒张压、平均动脉压降低,心率增加。

重组人甲状旁腺激素相关蛋白1-141序列的克隆和表达载体构建

目的:构建人甲状旁腺激素相关蛋白1-141(hPTHrP1-141)基因的表达载体。方法:提取人基因组DNA,PCR扩增PTHrP1-141基因,将其克隆入原核表达载体pQE-30Xa,构建重组表达载体pQE-30Xa/hPTHrP1-141。结果:重组载体pQE-30Xa/hPTHrP1-141经限制性核酸内切酶PvuⅡ酶切鉴定,得到符合预期大小的核酸片段。结论:表达载体pQE-30Xa/hPTHrP1-141构建成功。

人甲状旁腺素在甲醇毕赤酵母中的分泌表达

选用酵母偏爱的密码子,人工合成长度为282bp的人甲状旁腺素(hPTH)基因,将其克隆于M13载体中,DNA测序验证正确。通过PCR从含有hPTH基因的M13载体获得了该基因,将其插入到含有AOX1启动子和α因子信号肽序列的表达载体pPIC9K中,构建了重组质粒pPIC9K-hPTH,电击法转化甲醇毕赤酵母(Pichiapastoris)GS115菌株,经G418筛选得到高拷贝转化子,甲醇诱导表达,Tricine-SDS-PAGE电泳结果表明在9 3kDa处有明显的诱导蛋白带,与报道的hPTH的相对分子质量相近;酶联免疫沉淀法(ELISA)检测证明表达的蛋白具有hPTH免疫活性为132ng/L。

重组人甲状旁腺激素氨基端1-34对绝经后骨质疏松症的作用

重组人甲状旁腺激素氨基端1-34(rh PTH1-34)是促骨形成的代表性药物,具有提高绝经后骨质疏松症患者骨密度,降低发生脆性骨折风险的作用。本文介绍rh PTH1-34抗骨质疏松机制、临床疗效、对骨转换标志物的影响、疗效的影响因素和不良反应,并对临床应用提出建议。

激素替代疗法对分化型甲状腺癌术后甲状旁腺功能减退症患者的临床疗效

目的:观察激素替代疗法治疗分化型甲状腺癌术后甲状旁腺功能减退症患者的疗效,主要分析患者甲状旁腺激素(PTH)水平的变化,以期指导未来该类疾病的治疗方案提供选择。方法:收集2016年3月~2019年7月本院接受标准治疗方案+激素替代疗法治疗的病例52例作为观察组,回顾性分析分化型甲状腺癌术后甲状旁腺功能减退症患者病历资料;同期本院接受标准治疗方案的46例分化型甲状腺癌术后甲状旁腺功能减退症患者病历资料作为对照组。比较两组治疗前、治疗1个月、治疗3个月血钙、PTH水平;比较两组血钙、PTH恢复时间及两组治疗期间不良反应情况。结果:两组治疗1个月、治疗3个月血钙水平高于治疗前,且观察组各时点血钙水平高于对照组(P <0.05);两组治疗1个月、治疗3个月PTH水平高于治疗前,且观察组各时点PTH水平高于对照组(P <0.05);观察组血钙和PTH水平恢复时间短于对照组(P <0.05);两组恶心呕吐、便秘、心率加快和高钙尿症不良反应发生率相近。结论:激素替代疗法可有效改善分化型甲状腺术后甲状旁腺功能减退症患者血钙和PTH水平,促进患者病情恢复,且不良反应较少,安全性较高。

纳升电喷雾串联质谱鉴定重组人甲状旁腺素(1-34)

用先进的纳升电喷雾-四极杆-飞行时间串联质谱鉴定重组人PTH(1-34)。通过ESI-MS测定重组人PTH(1-34)分子量及MS/MS对其胰蛋白酶酶解后的肽段的序列和数据库查询进行结构鉴定。重组PTH(1-34)测定分子量为4115.21,与理论值相比测定相差0.06%。MS/MS测定出其中双电荷离子峰m/z728.4肽段序列为VSEIQLMHNLG,以及其他3个单电荷离子峰的序列。数据库检索后确定重组表达的PTH(1-34)一级结构完全正确,纳升电喷雾串联质谱以其灵敏、快速和准确为蛋白质鉴定提供了有效的手段。