Parvovirus 4 in Individuals with Severe Hemophilia A and Matched Control Group.

Q3 Medicine
Sanaz Asiyabi, Seyed Mahdi Marashi, Rouhollah Vahabpour, Ahmad Nejati, Alireza Azizi-Saraji, Aliyeh Sadat Mustafa, Asgar Baghernejad, Zabiholla Shoja, Hassan Mansouritorghabeh
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Abstract

Background: Hemophilia is a well-known bleeding disorder with worldwide distribution. Replacement therapy, using plasma-derived or recombinant coagulation factors, comprises a gold standard regimen for the treatment. Regardless of the advancements made in viral inactivation methods in the production of plasma-derived coagulation factors, the possibility of transmission of new viral infections remained as a noticeable concern yet. The aim of the current study was to investigate the status of parvovirus 4 (PARV4) in severe hemophilia A, von Willebrand disease (vWD), and healthy control. Materials and Methods: In the current case-control study, 76 patients with hemophilia and vWD and 60 individuals from their family members entered the study. Nested PCR used to determine the presence of PARV4 in study subjects (76 cases). To characterize the PARV4 genotype, positive samples subjected to sequencing and phylogenetic analysis. Results: PARV4 genome detected in 11 (14.47%) patients with bleeding disorders. Among whom, nine patients (14.75%) were with severe hemophilia A and two (13.33%) patients with vWD. Only five healthy controls (8.33%) were positive for PARV4. All PARV4 sequences were found to be genotype 1. Conclusion: PARV4 infection in patients with hemophilia and vWD was higher than the control group. While detection of PARV4 DNA in patients with bleeding disorders may not necessarily reflect a clinical urgency, future investigations are needed to define the clinical significance of PARV4. It seems the detection of the virus immune signature of PARV4 infection, particularly in the context of acute and persistent infections, needs to focus on cellular and tissue targets.

Abstract Image

严重A型血友病患者和匹配对照组的细小病毒4
背景:血友病是一种众所周知的出血性疾病,在世界范围内均有分布。使用血浆源性或重组凝血因子的替代疗法是治疗的金标准方案。尽管在生产血浆源性凝血因子的病毒灭活方法方面取得了进展,但新病毒感染传播的可能性仍然是一个值得关注的问题。本研究的目的是调查严重血友病A、血管性血友病(vWD)和健康对照中细小病毒4 (PARV4)的状况。材料与方法:在本病例对照研究中,76例血友病和vWD患者及其60名家庭成员进入研究。巢式PCR用于检测研究对象(76例)中PARV4的存在。为了鉴定PARV4基因型,对阳性样本进行测序和系统发育分析。结果:11例(14.47%)出血性疾病患者检测到PARV4基因组。其中重度A型血友病9例(14.75%),vWD 2例(13.33%)。健康对照仅有5例(8.33%)PARV4阳性。所有PARV4序列均为基因型1。结论:血友病和vWD患者PARV4感染高于对照组。虽然在出血性疾病患者中检测PARV4 DNA可能并不一定反映临床急迫性,但需要进一步的研究来确定PARV4的临床意义。似乎检测PARV4感染的病毒免疫特征,特别是在急性和持续性感染的情况下,需要将重点放在细胞和组织目标上。
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来源期刊
CiteScore
1.30
自引率
0.00%
发文量
32
审稿时长
12 weeks
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