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夜猴对乙肝DNA疫苗的免疫反应:疫苗配方、接种途径及接种方法的比较

Immune response to a hepatitis B DNA vaccine in Aotus monkeys: a comparison of vaccine formulation, route, and method of administration.

作者信息

Gramzinski R A, Millan C L, Obaldia N, Hoffman S L, Davis H L

机构信息

Naval Medical Research Institute, Malaria Program, Rockville, Maryland, USA.

出版信息

Mol Med. 1998 Feb;4(2):109-18.

Abstract

BACKGROUND

Attempts to optimize DNA vaccines in mice include using different routes of administration and different formulations. It may be more relevant to human use to carry such studies out in nonhuman primates. Here we compare different approaches to delivery of a DNA vaccine against the hepatitis B virus (HBV) in Aotus monkeys.

MATERIALS AND METHODS

Thirty-two adult Aotus l. lemurinus monkeys divided into 8 groups of four were immunized with 400 microg of a DNA vaccine which encoded hepatitis B surface antigen (HBsAg). DNA in saline was administered by intradermal (ID) or intramuscular (IM) injection with needle and syringe, IM injection with the Biojector needleless injection system or combined ID (needle) and IM (Biojector). DNA formulated with cationic liposomes (CellFECTIN) was injected IM with needle or Biojector. DNA with added E. coli DNA (100 microg) was injected IM with the Biojector or ID. A ninth group of 4 monkeys was injected IM (needle) with Engerix-B, a commercial vaccine containing recombinant HBsAg (10 microg) adsorbed onto alum. Monkeys were boosted in an identical fashion to their prime at 8 weeks, but all received the protein vaccine (Engerix-B) at 16 weeks. Sera was assessed for antibodies against HBsAg (anti-HBs) by enzyme-linked imunosorbent assay (ELISA).

RESULTS

The primary humoral response induced by IM delivery of the DNA vaccine was very poor. In most cases there was no detectable anti-HBs even after 2 DNA doses but the kinetics of the response to subsequent protein indicated that a memory B cell response had been induced. In contrast, following IM-administration of DNA using the Biojector, detectable anti-HBs were observed in 3 of 8 animals and evidence for immunological priming was apparent in an additional 4 of the 8 monkeys. ID injection of DNA vaccine in saline induced a potent antibody response which was augmented 6-fold by the addition of E. coli DNA. Combining ID and IM administration did not improve humoral immunity over ID injection alone.

CONCLUSIONS

For immunization of primates with DNA vaccines, ID may be a preferable route to IM, although it is not clear whether the Aotus monkey is a relevant model for humans in this respect. Nevertheless, the use of the Biojector needleless injection system may improve responses with IM delivery of DNA vaccines. As well, the immunostimulatory action of E. coli DNA may be used to augment the humoral response induced by a DNA vaccine.

摘要

背景

在小鼠中优化DNA疫苗的尝试包括采用不同的给药途径和不同的配方。在非人类灵长类动物中开展此类研究可能与人类应用更为相关。在此,我们比较了在夜猴中递送针对乙型肝炎病毒(HBV)的DNA疫苗的不同方法。

材料与方法

将32只成年普通狨猴分成8组,每组4只,用400微克编码乙型肝炎表面抗原(HBsAg)的DNA疫苗进行免疫。盐水中的DNA通过皮内(ID)或肌肉内(IM)注射,使用针头和注射器,或用Biojector无针注射系统进行肌肉内注射,或联合皮内(用针头)和肌肉内(用Biojector)注射。用阳离子脂质体(CellFECTIN)配制的DNA用针头或Biojector进行肌肉内注射。添加了大肠杆菌DNA(100微克)的DNA用Biojector进行肌肉内注射或皮内注射。第九组4只猴子用Engerix - B进行肌肉内(用针头)注射,Engerix - B是一种商业疫苗,含有吸附在明矾上的重组HBsAg(10微克)。猴子在8周时以与初次免疫相同的方式进行加强免疫,但在16周时均接受蛋白质疫苗(Engerix - B)。通过酶联免疫吸附测定(ELISA)评估血清中针对HBsAg的抗体(抗 - HBs)。

结果

通过肌肉内递送DNA疫苗诱导的初次体液反应非常差。在大多数情况下,即使接种2剂DNA后也检测不到抗 - HBs,但对后续蛋白质的反应动力学表明已诱导出记忆B细胞反应。相比之下,使用Biojector进行肌肉内注射DNA后,8只动物中有3只检测到可检测到的抗 - HBs,并且在另外4只猴子中明显有免疫启动的证据。在盐水中皮内注射DNA疫苗诱导了强烈的抗体反应,添加大肠杆菌DNA后反应增强了6倍。联合皮内和肌肉内给药并没有比单独皮内注射改善体液免疫。

结论

对于用DNA疫苗免疫灵长类动物,皮内注射可能是比肌肉内注射更可取的途径,尽管尚不清楚在这方面普通狨猴是否是人类的相关模型。然而,使用Biojector无针注射系统可能会改善肌肉内递送DNA疫苗的反应。此外,大肠杆菌DNA的免疫刺激作用可用于增强DNA疫苗诱导的体液反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f7ac/2230303/36fa69be8649/molmed00014-0056-a.jpg

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