Clinico-Pathological Factors and AR-LBD Mutations in Early and Late Castration-Resistant Prostate Cancer.

IF 2.5 4区 医学 Q3 ONCOLOGY
Cancer Management and Research Pub Date : 2024-10-21 eCollection Date: 2024-01-01 DOI:10.2147/CMAR.S477439
Monu Deswal, Durgavati Yadav, Vinay Kumar, Meenakshi Meenu, Pranay Tanwar, Shivani Srivastava, Prabhjot Singh, Kumar Sandeep
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引用次数: 0

Abstract

Background: Prostate cancer (PCa) is not well understood because of its enormous biological heterogeneity and unreliable progression. We conducted this retrospective analysis to examine the variables predicting early and late progression to castration-resistant PCa (CRPC) for better management of this disease.

Methods: This single institutional retrospective study was conducted from January 2018 to January 2022. A total of 98 consecutive men meeting with the diagnosis of CRPC as per the inclusion criteria were included in the study and were stratified in four quartiles on the basis of time to CRPC (time to castration resistance [TTCR]) development. Early CRPC (1st quartile, TTCR = 6-12 months) and late CRPC (4th quartile, TTCR = 38-120 months) were then compared on the basis of different clinical, pathological and AR-LBD sequence to find the correlation with response duration.

Results: Median time to develop castration resistance was 25 ± 26.44 months. The mean age of the patients was 66.8 ± 9.20 years and median baseline PSA was calculated 100±685.06 ng/mL respectively. Higher Gleason score (≥7-10) was found to be significantly associated with early development of CRPC (p<0.001) and lower nadir PSA was significantly indicating late CRPC progression (p<0.005). No mutations were found in androgen receptor exon-5, 6, 7 except a homozygous mutation in the 7th intronic region, which is involved in splice variants formation playing noteworthy role in CRPC development.

Conclusion: Time for metastatic PCa to CRPC ranges from 6-120 months revealing its heterogeneous nature. Early age presentation in the clinic and high initial PSA and high grade (GS>7) at diagnosis were positively associated with early CRPC while lower nadir PSA was correlated with late CRPC progression. No remarkable genomic mutations were discovered. Therefore, more data are needed and further research is required with large no. of patients to discover the predictive prognostic biomarkers for better patients' management.

早期和晚期阉割耐药前列腺癌的临床病理因素和 AR-LBD 基因突变
背景:前列腺癌(PCa)因其巨大的生物学异质性和不可靠的进展而不为人们所熟知。我们进行了这项回顾性分析,研究预测早期和晚期进展为耐阉割性前列腺癌(CRPC)的变量,以便更好地管理这种疾病:这项单一机构回顾性研究于 2018 年 1 月至 2022 年 1 月进行。研究共纳入了98名符合纳入标准、诊断为CRPC的连续男性患者,并根据CRPC(阉割耐药时间[TTCR])的发展时间分为四个四分位。然后根据不同的临床、病理和AR-LBD序列对早期CRPC(第1四分位数,TTCR=6-12个月)和晚期CRPC(第4四分位数,TTCR=38-120个月)进行比较,以找出与反应持续时间的相关性:出现阉割抵抗的中位时间为 25 ± 26.44 个月。患者的平均年龄为(66.8 ± 9.20)岁,中位基线 PSA 分别为(100±685.06)纳克/毫升。研究发现,较高的格里森评分(≥7-10分)与CRPC的早期发展显著相关(pth内含子区参与剪接变体的形成,在CRPC的发展中起着值得注意的作用):结论:从转移性 PCa 到 CRPC 的时间范围为 6-120 个月,揭示了其异质性。临床表现年龄早、诊断时初始PSA高和分级高(GS>7)与早期CRPC呈正相关,而较低的Nadir PSA与晚期CRPC进展相关。没有发现明显的基因组突变。因此,还需要更多的数据,并需要对大量患者进行进一步研究,以发现预测预后的生物标志物,从而更好地管理患者。
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来源期刊
Cancer Management and Research
Cancer Management and Research Medicine-Oncology
CiteScore
7.40
自引率
0.00%
发文量
448
审稿时长
16 weeks
期刊介绍: Cancer Management and Research is an international, peer reviewed, open access journal focusing on cancer research and the optimal use of preventative and integrated treatment interventions to achieve improved outcomes, enhanced survival, and quality of life for cancer patients. Specific topics covered in the journal include: ◦Epidemiology, detection and screening ◦Cellular research and biomarkers ◦Identification of biotargets and agents with novel mechanisms of action ◦Optimal clinical use of existing anticancer agents, including combination therapies ◦Radiation and surgery ◦Palliative care ◦Patient adherence, quality of life, satisfaction The journal welcomes submitted papers covering original research, basic science, clinical & epidemiological studies, reviews & evaluations, guidelines, expert opinion and commentary, and case series that shed novel insights on a disease or disease subtype.
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