对他莫昔芬耐药的三阳性乳腺癌进行基于药物反应的精准治疗选择

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-09-17 DOI:10.1016/j.jprot.2024.105319
Vinod S. Bisht , Deepak Kumar , Mohd Altaf Najar , Kuldeep Giri , Jaismeen Kaur , Thottethodi Subrahmanya Keshava Prasad , Kiran Ambatipudi
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引用次数: 0

摘要

乳腺癌对药物环境的适应性降低了化疗反应,并助长了获得性耐药性。与标准化疗相比,癌症特异性疗法对晚期癌症更有效。为了扩展癌症特异性疗法的范例,我们解构了与临床相关的获得性他莫昔芬耐药 MCF-7 蛋白质组,以确定可能的药物靶点(N = 150)。针对确定的可药用靶点使用了 28 种药物抑制剂来抑制非耐药细胞(NC)和耐药细胞(RC)。首先,利用对 NC 和 RC 的生长抑制反应筛选出所选药物。筛选出七种具有时间依赖性(10-12 天)细胞毒性作用的药物,并进一步筛选出三种有效药物(如顺铂、多柔比星和羟氯喹)。所选药物的生长抑制效果在复杂球形模型(渐进和退行)中得到了验证。在渐进模型中,多柔比星(RC:83.64 %,NC:54.81 %)、顺铂(RC:76.66 %,NC:68.94 %)和羟氯喹(RC:68.70 %,NC:61.78 %)具有显著的抑制生长效果。然而,在完全生长的退行性球形体中,经过第 4 次药物处理后,顺铂显著抑制了 RC(84.79 %)和 NC(40.21 %),而多柔比星和羟氯喹仅显著抑制了 RC(76.09 % 和 76.34 %)。我们的深入研究有效地整合了表达数据和癌症特异性治疗研究。此外,我们的三步序贯药物筛选方法无偏见地发现顺铂、多柔比星和羟氯喹是针对异质性癌细胞群的有效药物。然而,耐药性的产生不仅会降低药物反应,还会增加 BC 的侵袭性。此外,替代化疗药物被广泛用于控制晚期 BC。相比之下,我们假设,与标准化疗药物相比,癌症特异性药物对耐药性癌症更有效。虽然癌症特异性治疗的鉴定是一场艰苦的战斗,但我们的工作表明蛋白质组数据可用于药物选择。我们确定了多个可用药的靶点,并利用体外方法将多种药物缩小到针对特定疾病条件的治疗方法。我们认为,我们的研究成功地将表达数据与针对特定疾病的功能性治疗研究联系在一起,所选药物可用于有效的抗药性治疗,且治疗反应更强。
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Drug response-based precision therapeutic selection for tamoxifen-resistant triple-positive breast cancer

Breast cancer adaptability to the drug environment reduces the chemotherapeutic response and facilitates acquired drug resistance. Cancer-specific therapeutics can be more effective against advanced-stage cancer than standard chemotherapeutics. To extend the paradigm of cancer-specific therapeutics, clinically relevant acquired tamoxifen-resistant MCF-7 proteome was deconstructed to identify possible druggable targets (N = 150). Twenty-eight drug inhibitors were used against identified druggable targets to suppress non-resistant (NC) and resistant cells (RC). First, selected drugs were screened using growth-inhibitory response against NC and RC. Seven drugs were shortlisted for their time-dependent (10–12 days) cytotoxic effect and further narrowed to three effective drugs (e.g., cisplatin, doxorubicin, and hydroxychloroquine). The growth-suppressive effectiveness of selected drugs was validated in the complex spheroid model (progressive and regressive). In the progressive model, doxorubicin (RC: 83.64 %, NC: 54.81 %), followed by cisplatin (RC: 76.66 %, NC: 68.94 %) and hydroxychloroquine (RC: 68.70 %, NC: 61.78 %) showed a significant growth-suppressive effect. However, in fully grown regressive spheroid, after 4th drug treatment, cisplatin significantly suppressed RC (84.79 %) and NC (40.21 %), while doxorubicin and hydroxychloroquine significantly suppressed only RC (76.09 and 76.34 %). Our in-depth investigation effectively integrated the expression data with the cancer-specific therapeutic investigation. Furthermore, our three-step sequential drug-screening approach unbiasedly identified cisplatin, doxorubicin, and hydroxychloroquine as an efficacious drug to target heterogeneous cancer cell populations.

Significance statement

Hormonal-positive BC grows slowly, and hormonal-inhibitors effectively suppress the oncogenesis. However, development of drug-resistance not only reduces the drug-response but also increases the chance of BC aggressiveness. Further, alternative chemotherapeutics are widely used to control advanced-stage BC. In contrast, we hypothesized that, compared to standard chemotherapeutics, cancer-specific drugs can be more effective against resistant-cancer. Although cancer-specific treatment identification is an uphill battle, our work shows proteome data can be used for drug selection. We identified multiple druggable targets and, using ex-vivo methods narrowed multiple drugs to disease-condition-specific therapeutics. We consider that our investigation successfully interconnected the expression data with the functional disease-specific therapeutic investigation and selected drugs can be used for effective resistant treatment with higher therapeutic response.

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ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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