Salmonella-mediated tumor regression involves targeting of tumor myeloid suppressor cells causing a shift to M1-like phenotype and reduction in suppressive capacity

Kaimala, Suneesh; Mohamed, Yassir A.; Nader, Nader D.; Issac, Jincy M.; Elkord, Eyad; Chouaı̈b, Salem; Fernández-Cabezudo, Maria J.; al-Ramadi, Basel K.

doi:10.1007/s00262-014-1543-x

Cited by 76 publications

(98 citation statements)

References 49 publications

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“…Salmonella -induced tumor inhibition occurs with alterations in myeloid cells consistent with maturation to macrophage effectors and a reduction in their suppressive capacity. The antitumor effectiveness of Salmonella relies on the induction of the innate immune response through the toll-like receptor-myeloid differentiation primary response gene ( TLR-MYD88 ) signaling pathway [14]. This is consistent with our previous report demonstrating that Salmonella induce cytokine production and antitumor activities via TLR4 signaling, which may help clarify the molecular mechanism of Salmonella -induced host antitumor responses [15].…”

Section: Host Immunity and Salmonellasupporting

confidence: 89%

Salmonella as an Innovative Therapeutic Antitumor Agent

Chang

Lee

2014

IJMS

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Lack of specificity of the therapeutic agent is a primary limitation in the treatment of a tumor. The use of preferentially replicating bacteria as therapeutic agents is an innovative approach to tumor treatment. This is based on the observation that certain obligate or facultative anaerobic bacteria are capable of multiplying selectively in tumors and inhibiting their growth. Bacteria have been employed as antitumor agents that are capable of preferentially amplifying within tumors and inhibiting their growth. Moreover, bacteria-derived factors have an immune-stimulation effect. Therefore, bacteria are able to transfer therapeutic genes into the tumor cells using their infective ability. Herein, we introduce the application of bacteria for tumor therapy and focus on Salmonella, which have been widely used for tumor therapy. Salmonella have mainly been applied as gene-delivery vectors, antitumor immune activators and tumor cell death inducers. This study will not only evaluate the therapeutic efficacy of Salmonella for the treatment of tumor but will also elucidate the mechanisms underlying the antitumor activities mediated by Salmonella, which involve host immune responses and cellular molecular responses.

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Section: Host Immunity and Salmonellasupporting

confidence: 89%

Salmonella as an Innovative Therapeutic Antitumor Agent

Chang

Lee

2014

IJMS

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“…Second, a definitive M1 macrophage marker would enhance the findings of our manuscript for this would give a true insight in the M1/M2 macrophage ratio. NOS2 expression has proven be a useful marker for M1 macrophages in several tumor types [31]–[33]. However, for mesothelioma, Soini et al and others [34], [35] have demonstrated that NOS2 is highly expressed in healthy pleura as well as in cancerous mesothelioma tissues and mesothelioma cell lines.…”

Section: Discussionmentioning

confidence: 99%

Ratio of Intratumoral Macrophage Phenotypes Is a Prognostic Factor in Epithelioid Malignant Pleural Mesothelioma

et al. 2014

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HypothesisThe tumor micro-environment and especially the different macrophage phenotypes appear to be of great influence on the behavior of multiple tumor types. M1 skewed macrophages possess anti-tumoral capacities, while the M2 polarized macrophages have pro-tumoral capacities. We analyzed if the macrophage count and the M2 to total macrophage ratio is a discriminative marker for outcome after surgery in malignant pleural mesothelioma (MPM) and studied the prognostic value of these immunological cells.Methods8 MPM patients who received induction chemotherapy and surgical treatment were matched on age, sex, tumor histology, TNM stage and EORTC score with 8 patients who received chemotherapy only. CD8 positive T-cells and the total macrophage count, using the CD68 pan-macrophage marker, and CD163 positive M2 macrophage count were determined in tumor specimens prior to treatment.ResultsThe number of CD68 and CD163 cells was comparable between the surgery and the non-surgery group, and was not related to overall survival (OS) in both the surgery and non-surgery group. However, the CD163/CD68 ratio did correlate with OS in both in the total patient group (Pearson r −0.72, p<0.05). No correlation between the number of CD8 cells and prognosis was found.ConclusionsThe total number of macrophages in tumor tissue did not correlate with OS in both groups, however, the CD163/CD68 ratio correlates with OS in the total patient group. Our data revealed that the CD163/CD68 ratio is a potential prognostic marker in epithelioid mesothelioma patients independent of treatment but cannot be used as a predictive marker for outcome after surgery.

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“…Total RNA was extracted from a second biopsy of each patient using the TRIzol reagent protocol (Invitrogen) and repurified on Qiagen columns (RNeasy Plus Mini kit, Qiagen) as previously described (44). Similarly, total RNA was extracted from MCF-7 and MDA-MB-231 human breast cancer cell lines.…”

Section: Methodsmentioning

confidence: 99%

Deficiency of mitochondrial modulator MCJ promotes chemoresistance in breast cancer

et al. 2016

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Despite major advances in early detection and prognosis, chemotherapy resistance is a major hurdle in the battle against breast cancer. Identifying predictive markers and understanding the mechanisms are key steps to overcoming chemoresistance. Methylation-controlled J protein (MCJ, also known as DNAJC15) is a negative regulator of mitochondrial respiration and has been associated with chemotherapeutic drug sensitivity in cancer cell lines. Here we show, in a retrospective study of a large cohort of breast cancer patients, that low MCJ expression in breast tumors predicts high risk of relapse in patients treated with chemotherapy; however, MCJ expression does not correlate with response to endocrine therapy. In a prospective study in breast cancer patients undergoing neoadjuvant therapy, low MCJ expression also correlates with poor clinical response to chemotherapy and decreased disease-free survival. Using MCJ-deficient mice, we demonstrate that lack of MCJ is sufficient to induce mammary tumor chemoresistance in vivo. Thus, loss of expression of this endogenous mitochondrial modulator in breast cancer promotes the development of chemoresistance.

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Salmonella-mediated tumor regression involves targeting of tumor myeloid suppressor cells causing a shift to M1-like phenotype and reduction in suppressive capacity

Cited by 76 publications

References 49 publications

Salmonella as an Innovative Therapeutic Antitumor Agent

Salmonella as an Innovative Therapeutic Antitumor Agent

Ratio of Intratumoral Macrophage Phenotypes Is a Prognostic Factor in Epithelioid Malignant Pleural Mesothelioma

Deficiency of mitochondrial modulator MCJ promotes chemoresistance in breast cancer

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