啤酒灌装线上生物膜热点的表征

Biofilms Pub Date : 2020-07-01 DOI:10.5194/biofilms9-41
Eva Wagner, Sarah Thalguter, K. Rychli, M. Wagner
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引用次数: 0

摘要

生物膜被认为在食品加工环境中起着重要作用。与生物膜微生物的直接接触或分离可能导致产品污染,从而减少产品的保质期。包装和灌装是产品安全的关键步骤,因为这一步骤中的任何污染都会直接影响产品的保质期和安全性。对于瓶装和罐装饮料,灌装线用于以标准化方式灌装大量产品。在就地清洗(CIP)程序中,这些管线的大部分都是自动清洗和消毒的。这些灌装线的设计非常重要,因为可达性和材料对自动清洁和消毒程序的成功至关重要。一些公司实施了额外的人工清理策略,以彻底清除潜在的问题产生地点。生物膜这个术语从90年代开始在啤酒厂中出现。然而,到目前为止,所有的研究都只关注微生物的存在,而忽略了构成生物膜必不可少的基质成分的存在。在本研究中,研究了一条每小时能灌装60000罐(容积0.5 l)的罐装灌装线,研究了生物膜形成的关键部位。灌装线主要用于啤酒,但混合啤酒饮料也可以灌装。我们在两个时间点使用刮绒拭子法对23个地点进行了采样。第一次采样是在手术中进行的,第二次采样是在自动清洁和消毒程序后一个月进行的。样品的特征是微生物负荷(16S rRNA和18S rRNA基因的qPCR)和生物膜基质的存在(碳水化合物的苯酚硫酸测定,蛋白质的沉淀和SDS-PAGE,随后的银染色和细胞外DNA的沉淀和分光光度定量测定)。在操作过程中,我们可以通过应用微生物和至少两种基质成分的存在定义来确定三个含有生物膜的位点。此外,有7个位点窝藏微生物和1个基质成分。清洗消毒后未检出生物膜。在一个位点,可以检测到微生物和一种基质成分。生物膜阳性位点的急剧减少表明通过清洁和消毒过程成功地去除了生物膜。未来灌装厂的设计应强调卫生设计原则,因为这有助于防止生物膜的形成,并在清洁和消毒过程中有针对性地去除生物膜。这里确定的生物膜热点表明了灌装线设计中潜在的问题产生点和弱点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterisation of biofilm hotspots at a can filling line for beer

Biofilms are thought to play a serious role in the food processing environment. Direct contact with or detachment of microorganisms of biofilms could lead to product contamination resulting in diminished shelf life of the product. Packaging and filling are essential key steps for product safety, as any contamination within this step will directly impact the shelf life and safety of the product. For bottled and canned beverages filling lines are used for filling huge amounts of product in a standardised manner. Most parts of these lines are cleaned and disinfected automatically during cleaning in place (CIP) procedures. The design of these filling lines is of great importance, as accessibility and materials are crucial regarding the success of automatic cleaning and disinfection programs. Some companies implemented additional manual cleaning strategies for the complete removal of potential problem-causing sites. In the brewery setting the term biofilm is manifested since the 90s. However, until now all studies focus only on the presence of microorganisms, neglecting the presence of matrix components, which constitutes an essential component of a biofilm.  

Within this study a filling line for cans, capable of filling 60000 cans per hour (volume 0.5 l), was investigated regarding critical sites for biofilm formation. The filling line is used primarily for beer, but mixed beer drinks are also filled. We sampled 23 sites using a scraper-flocked-swab method at two time points. The first sampling was done during operation and the second sampling was conducted one month later after the automated cleaning and disinfection procedure. The samples were characterised regarding their microbial load (qPCR for 16S rRNA and 18S rRNA genes) and the presence of biofilm matrix (phenol-sulfuric assay for carbohydrates, precipitation and SDS-PAGE with subsequent silver staining for proteins and precipitation and spectrophotometric quantitative measurements for extracellular DNA).

During operation, we could identify three sites harbouring a biofilm by applying the definition of presence of microorganisms and at least two matrix components. Furthermore, there were seven sites harbouring microorganisms and one matrix component. After cleaning and disinfection no biofilm could be detected. At one site, microorganisms and one matrix component could be detected. The drastic reduction of biofilm positive sites indicates the successful removal of biofilms by the cleaning and disinfection process.

The design of future filling plants should emphasise on the principles of hygienic design, as this can help to prevent biofilm formation and targeted removal of biofilms during cleaning and disinfection. The here identified biofilm hotspots indicate potential problem-causing sites and weak-points in the design of the filling line.

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