Nucleotide Oligomerization Domain-like receptor 4 (NLR4) Gene Expression and Interleukin 1-β (IL 1-β) Level in Urine Samples Before and After Intravesical BCG Therapy For Treatment of Bladder Cancer

A. Eissa, O. Rasslan, Lamia Fouad, Fahim Hisham Abdelmajeed, Amira Esmail Abdel-Hamid
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The aim of this study was to evaluate NLR4 gene expression and IL-1β as possible prognostic indicators for NMIBC recurrence and BCG treatment failure, and to detect the difference in their levels among muscle invasive bladder cancer (MIBC) and NMIBC that may aid in primary differentiation between cases. This study was conducted in 30 patients who had NMIBC and 17 patients who had MIBC. Urine samples were obtained in sterile cups before operation. From NMIBC cases, four more samples were obtained as mentioned below. Evaluation of NLR4 gene expression was performed in pre-surgical sample for MIBC and in 4 samples for NMIBC: pre-surgical sample, sample collected 4 hours after the 3rd dose of BCG instillation, and samples collected during follow up (3 and 6 months post-surgically). There was statistical significant increase in NLRP4 expression levels in NMIBC (CT=0.87±1.48) compared to MIBC (CT=2.82±2.07). As far as we searched, no published results were found regarding comparative gene expression levels between NMIBC and MIBC cases. Gene expression in recurrent cases was higher in pre-surgical urine samples than in non-recurrent cases. The expression level further increased up to 21 fold than the pre-surgical level in the sample taken after injection of the 3rd dose of BCG. This level decreased distinctly to become 1-fold increase over pre-surgical level at the 3rd month follow up then to only 0.9-fold at the 6th month. In non- recurrent cases, gene expression level started pre-surgically in much lower levels than those encountered in recurrent cases. There were 11-fold increase in expression level after 3rd dose of BCG instillation and then decreased to be 5.6 folds higher in the sample taken at 3rd month follow up than in presurgical samples. Gene expression further decreased to become 4.1 fold higher in samples taken at 6 month follow up than the pre-surgical levels. IL-1β levels were estimated for NMIBC and MIBC cases in urine samples pre-surgically and during BCG therapy in case of NMIBC before and 4 hours after the 3rd dose and during 3rd month follow-up of those cases for searching its possible use of for primary differentiation between NMIBC and MIBC, and also as a prognostic factor for possible recurrence in case of NMIBC cases. The level of IL-1β was generally higher in pre-surgical samples (0.62±0.12 pg/ml) when compared to its level before the 3rd dose of BCG induction therapy (0.53±0.13 pg/ml). Its level was distinctly higher four hours after administration of the 3rd dose BCG (1.96±0.62 pg/ml) than both previous levels. Levels decreased bellow pre-surgical level at 3rd month follow up (0.57±0.099 pg/ml). The levels of IL-1β estimated in samples collected four hours after the 3rd dose BCG was higher in cases that showed recurrence later on than non-recurrent cases. The levels decreased in both cases and became higher in non-recurrent cases (0.64±0.05 pg/ml) than in cases already developed recurrence at the 3rd month diagnosed during follow-up (0.45±0.05 pg/ml). To conclude, on following NLRP4 gene expression and IL-1β levels during BCG administration among recurrent and non-recurrent cases of thirty NMIBC cases, there was a significant statistical difference in both levels for the samples collected after the third dose BCG, being higher in patients who showed subsequent recurrence at the 3rd and 6th month of follow-up. If these preliminary reported findings will be confirmed in upcoming larger cohort’s studies, it could be promising in prognosis of such cases, with the possibility of early manipulation of individualized treatment schedule, keeping patients most probably prone to encounter recurrence safe from possible side effects of BCG therapy. The assessment of NLRP4 expression and IL-1β levels could help predict failure of BCG therapy, playing an appreciable role in early deciding radical surgery. When comparing NLRP4 expression and IL-1β levels between MIBC and NMIBC cases, increased values were noted among non-invasive ones. This finding may serve as a possible diagnostic tool, which represents a challenging issue. Hence, cut-off values for gene expression and cytokine level are to be specified.","PeriodicalId":85139,"journal":{"name":"Medical immunology (London, England)","volume":"1 1","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2021-01-10","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Medical immunology (London, England)","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.15789/1563-0625-nod-2101","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
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Abstract

Bladder cancer is the 7th most commonly diagnosed cancer in males worldwide and the 11th when both genders are considered. Seventy five per cent of bladder cancer cases are non-muscle invasive bladder cancer (NMIBC). Bacillus Calmette–Gu rin (BCG) immunotherapy remains the standard intravesical agent for NMIBC. The exact mechanism by which BCG prevents recurrence is unknown. The aim of this study was to evaluate NLR4 gene expression and IL-1β as possible prognostic indicators for NMIBC recurrence and BCG treatment failure, and to detect the difference in their levels among muscle invasive bladder cancer (MIBC) and NMIBC that may aid in primary differentiation between cases. This study was conducted in 30 patients who had NMIBC and 17 patients who had MIBC. Urine samples were obtained in sterile cups before operation. From NMIBC cases, four more samples were obtained as mentioned below. Evaluation of NLR4 gene expression was performed in pre-surgical sample for MIBC and in 4 samples for NMIBC: pre-surgical sample, sample collected 4 hours after the 3rd dose of BCG instillation, and samples collected during follow up (3 and 6 months post-surgically). There was statistical significant increase in NLRP4 expression levels in NMIBC (CT=0.87±1.48) compared to MIBC (CT=2.82±2.07). As far as we searched, no published results were found regarding comparative gene expression levels between NMIBC and MIBC cases. Gene expression in recurrent cases was higher in pre-surgical urine samples than in non-recurrent cases. The expression level further increased up to 21 fold than the pre-surgical level in the sample taken after injection of the 3rd dose of BCG. This level decreased distinctly to become 1-fold increase over pre-surgical level at the 3rd month follow up then to only 0.9-fold at the 6th month. In non- recurrent cases, gene expression level started pre-surgically in much lower levels than those encountered in recurrent cases. There were 11-fold increase in expression level after 3rd dose of BCG instillation and then decreased to be 5.6 folds higher in the sample taken at 3rd month follow up than in presurgical samples. Gene expression further decreased to become 4.1 fold higher in samples taken at 6 month follow up than the pre-surgical levels. IL-1β levels were estimated for NMIBC and MIBC cases in urine samples pre-surgically and during BCG therapy in case of NMIBC before and 4 hours after the 3rd dose and during 3rd month follow-up of those cases for searching its possible use of for primary differentiation between NMIBC and MIBC, and also as a prognostic factor for possible recurrence in case of NMIBC cases. The level of IL-1β was generally higher in pre-surgical samples (0.62±0.12 pg/ml) when compared to its level before the 3rd dose of BCG induction therapy (0.53±0.13 pg/ml). Its level was distinctly higher four hours after administration of the 3rd dose BCG (1.96±0.62 pg/ml) than both previous levels. Levels decreased bellow pre-surgical level at 3rd month follow up (0.57±0.099 pg/ml). The levels of IL-1β estimated in samples collected four hours after the 3rd dose BCG was higher in cases that showed recurrence later on than non-recurrent cases. The levels decreased in both cases and became higher in non-recurrent cases (0.64±0.05 pg/ml) than in cases already developed recurrence at the 3rd month diagnosed during follow-up (0.45±0.05 pg/ml). To conclude, on following NLRP4 gene expression and IL-1β levels during BCG administration among recurrent and non-recurrent cases of thirty NMIBC cases, there was a significant statistical difference in both levels for the samples collected after the third dose BCG, being higher in patients who showed subsequent recurrence at the 3rd and 6th month of follow-up. If these preliminary reported findings will be confirmed in upcoming larger cohort’s studies, it could be promising in prognosis of such cases, with the possibility of early manipulation of individualized treatment schedule, keeping patients most probably prone to encounter recurrence safe from possible side effects of BCG therapy. The assessment of NLRP4 expression and IL-1β levels could help predict failure of BCG therapy, playing an appreciable role in early deciding radical surgery. When comparing NLRP4 expression and IL-1β levels between MIBC and NMIBC cases, increased values were noted among non-invasive ones. This finding may serve as a possible diagnostic tool, which represents a challenging issue. Hence, cut-off values for gene expression and cytokine level are to be specified.
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膀胱内卡介苗治疗膀胱癌前后尿样中核苷酸寡聚结构域样受体4 (NLR4)基因表达及白细胞介素1-β (IL 1-β)水平的变化
膀胱癌是全球男性中第七大最常诊断的癌症,如果将男女都考虑在内,则排名第11位。75%的膀胱癌病例是非肌肉浸润性膀胱癌(NMIBC)。卡介苗免疫疗法仍然是NMIBC的标准膀胱内治疗药物。卡介苗预防复发的确切机制尚不清楚。本研究的目的是评估NLR4基因表达和IL-1β作为NMIBC复发和卡介苗治疗失败的可能预后指标,并检测它们在肌肉浸润性膀胱癌(MIBC)和NMIBC之间的水平差异,这可能有助于病例之间的初步鉴别。本研究在30例NMIBC患者和17例MIBC患者中进行。术前取尿样于无菌杯内。从NMIBC病例中,又获得了如下所述的4个样本。对MIBC术前样本和NMIBC 4例样本进行NLR4基因表达评估:术前样本、第3次卡介苗注射后4小时采集的样本、术后3个月和6个月随访时采集的样本。NLRP4在NMIBC中的表达水平(CT=0.87±1.48)高于MIBC (CT=2.82±2.07),差异有统计学意义。在我们的搜索中,没有发现关于NMIBC和MIBC病例之间基因表达水平比较的已发表的结果。术前尿样中复发病例的基因表达高于非复发病例。在注射第3剂卡介苗后,其表达水平进一步升高,达到术前水平的21倍。这一水平明显下降,在第3个月随访时比术前水平增加了1倍,而在第6个月随访时仅为0.9倍。在非复发病例中,术前基因表达水平比复发病例低得多。接种第3次卡介苗后,表达量增加11倍,随访第3个月时,表达量下降至手术前的5.6倍。在随访6个月的样本中,基因表达进一步下降,比术前水平高4.1倍。IL-1β水平在术前、BCG治疗期间(NMIBC患者在第3次给药前、第4小时后和第3个月随访期间)评估NMIBC和MIBC患者尿液样本中的IL-1β水平,以寻找IL-1β可能用于NMIBC和MIBC的初步鉴别,并作为NMIBC患者可能复发的预后因素。术前样本IL-1β水平(0.62±0.12 pg/ml)普遍高于第3次卡介苗诱导治疗前(0.53±0.13 pg/ml)。第3次卡介苗给药后4 h,其水平明显高于前两次(1.96±0.62 pg/ml)。3个月随访时,水平低于术前水平(0.57±0.099 pg/ml)。在第3次卡介苗接种4小时后收集的样本中,IL-1β水平在出现复发的病例中高于非复发病例。两例患者的水平均有所下降,非复发患者的水平(0.64±0.05 pg/ml)高于随访中诊断的第3个月已经复发的患者(0.45±0.05 pg/ml)。综上所述,在30例NMIBC复发和非复发病例中,在BCG给药期间NLRP4基因表达和IL-1β水平的随访中,在第三次接种BCG后收集的样本中,NLRP4基因表达和IL-1β水平有显著的统计学差异,在随访第3和第6个月出现复发的患者中,NLRP4基因表达和IL-1β水平更高。如果这些初步报告的发现将在即将到来的更大规模的队列研究中得到证实,它可能在这类病例的预后方面有希望,有可能早期操纵个体化治疗计划,使最容易复发的患者免受卡介苗治疗可能的副作用的影响。NLRP4表达和IL-1β水平的评估可以帮助预测卡介苗治疗的失败,在早期决定根治性手术中发挥重要作用。当比较NLRP4表达和IL-1β水平在MIBC和NMIBC病例中,非侵入性的值明显升高。这一发现可能作为诊断工具,这是一个具有挑战性的问题。因此,必须指定基因表达和细胞因子水平的临界值。
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