Your search keyword '"Schmid, A. C."' showing total 8 results

1. PI3Kα activates integrin α4β1 to establish a metastatic niche in lymph nodes

Author

Garmy-Susini, Barbara, Avraamides, Christie J., Desgrosellier, Jay S., Schmid, Michael C., Foubert, Philippe, Ellies, Lesley G., Lowy, Andrew M., Blair, Sarah L., Vandenberg, Scott R., Datnow, Brian, Wang, Huan-You, Cheresh, David A., and Varner, Judith

Published

2013

2. The neuronal guidance cue Slit2 induces targeted migration and may play a role in brain metastasis of breast cancer cells

Author

Schmid, Bernd C., Rezniczek, Günther A., Fabjani, Gerhild, Yoneda, Toshiyuki, Leodolter, Sepp, and Zeillinger, Robert

Published

2007

3. Macrophages as Key Drivers of Cancer Progression and Metastasis.

Author

Nielsen, Sebastian R. and Schmid, Michael C.

Subjects

*CANCER invasiveness, *MACROPHAGES, *METASTASIS, *IMMUNE system, *NEOVASCULARIZATION

Abstract

Macrophages are one of the most abundant immune cells in the tumour microenvironment of solid tumours and their presence correlates with reduced survival in most cancers. Macrophages are present at all stages of tumour progression and stimulate angiogenesis, tumour cell invasion, and intravasation at the primary site. At the metastatic site, macrophages and monocytes prepare for the arrival of disseminated tumour cells and promote their extravasation and survival by inhibiting immune-mediated clearance or by directly engaging with tumour cells to activate prosurvival signalling pathways. In addition, macrophages promote the growth of disseminated tumour cells at the metastatic site by organising the formation of a supportive metastatic niche. The development of agents inhibiting the recruitment or the protumorigenic effector functions of macrophages in both the primary tumour and at the metastatic site is a promising strategy to improve cancer survival in the future. [ABSTRACT FROM AUTHOR]

Published

2017

4. Evaluation of Computed Tomography for Lymph Node Staging in Bladder Cancer Prior to Radical Cystectomy.

Author

Horn, Thomas, Zahel, Tina, adt, Nathanja, Schmid, Sebastian C., Heck, Matthias M., Thalgott, Mark K., Hatzichristodoulou, Georgios, Haller, Bernhard, autenrieth, Michael, Kübler, Hubert R., Gschwend, Jürgen E., Holzapfel, Konstantin, and Maurer, Tobias

Subjects

BLADDER cancer treatment, LYMPH node surgery, COMPUTED tomography, CYSTECTOMY, METASTASIS

Abstract

Objectives: To retrospectively evaluate the value of CT for lymph node (LN) staging in bladder cancer. Methods: Two uroradiologists reviewed CT scans of 231 patients who underwent radical cystectomy and pelvic lymphadenectomy according to a predefined 12-field template. A 5-step model was used to grade the radiological likelihood of a LN to represent malignant spread based on size, configuration and structure as well as regional clustering. Statistical analyses were performed both on patient- and field-based levels. Results: LN metastases were found in 59 of 231 patients (25.5%). On a patient-based level, sensitivity, specificity, positive predictive value (PPV), negative predictive value (NPV) and accuracy were 52.6, 93.6, 73.2, 85.6 and 83.4%, respectively. Using the field-based approach, a total of 1,649 anatomical fields were evaluable, of which 114 fields showed malignancy (6.9%). On a field basis, sensitivity, specificity, PPV, NPV and accuracy were 30.2, 98, 51.5, 94.5 and 93.3%, respectively. Concerning local staging (pT category), the overall accuracy was 78%; overstaging occurred in 6% and understaging in 16%. Conclusions: In line with prior studies, the sensitivity of CT imaging for the detection of LN metastases was low, while high values for specificity were achieved. This was further underlined by analyzing standardized anatomical fields. Concerning local staging, postoperative changes after TURB-T rarely led to overstaging. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2016

5. Detection of underlying malignancy in patients with paraneoplastic neurological syndromes: comparison of F-FDG PET/CT and contrast-enhanced CT.

Author

Schramm, N., Rominger, A., Schmidt, C., Morelli, J., Schmid-Tannwald, C., Meinel, F., Reiser, M., and Rist, C.

Subjects

METASTASIS, PARANEOPLASTIC syndromes, COHEN'S kappa coefficient (Statistics), TUMORS, CANCER invasiveness

Abstract

Purpose: To determine the value of combined F-FDG PET/CT with diagnostic contrast-enhanced CT (CECT) in detecting primary malignancies and metastases in patients with paraneoplastic neurological syndromes (PNS) and to compare this with CECT alone. Methods: PET/CT scans from 66 patients with PNS were retrospectively evaluated. Two blinded readers initially reviewed the CECT portion of each PET/CT scan. In a second session 3 months later, the readers analysed the combined PET/CT scans. Findings on each study were assessed using a four-point-scale (1 normal/benign; 2 inconclusive, further diagnostic work-up may be necessary; 3 malignant; 4 inflammatory). Sensitivity and specificity for malignant findings were calculated for PET/CT and CECT. Interreader agreement was determined by calculating Cohen's kappa. Pooled data from clinical follow-up (including histopathology and follow-up imaging, median follow-up 20.0 months) served as the reference gold standard. Results: Both readers classified 12 findings in ten patients (15 %) as malignant on the PET/CT scans (two patients had two primary tumours). One such imaging finding (suspected thymic cancer) was false-positive (i.e. benign histology). The most common tumours were bronchial carcinoma ( n = 3), lymph node metastases of gynaecological tumours ( n = 3) and tonsillar carcinoma ( n = 2). Three of 12 findings (25 %) were not detected by CECT alone (cervical carcinoma, lymph node metastasis and tonsillar carcinoma). In a per-patient analysis, sensitivity and specificity for malignant findings were 100 % and 90 % for PET/CT and 78 % and 88 % for CECT. In 24 % (reader 1) and 21 % (reader 2) of the patients, the PET/CT findings were inconclusive. Of these findings, 57 % (reader 1) and 56 % (reader 2) were only diagnosed with PET (e.g. focal FDG uptake of the thyroid, gastrointestinal tract and ovaries). On follow-up, none of these findings corresponded to malignancy. Overall agreement between the two readers was excellent with a Cohen's kappa of 0.95 ± 0.04 ( p < 0.001) for PET/CT and 0.97 ± 0.03 ( p < 0.001) for CECT alone. Conclusion: In this cohort of patients with PNS, PET/CT exhibited improved detection of underlying malignancy versus CECT alone. While hybrid imaging produces a greater number of inconclusive findings, sensitivity is increased for the detection of head and neck and gynaecological malignancies as well as metastatic lymph node involvement. [ABSTRACT FROM AUTHOR]

Published

2013

6. PI3-Kinase γ Promotes Rap1a-Mediated Activation of Myeloid Cell Integrin α4β1, Leading to Tumor Inflammation and Growth.

Author

Schmid, Michael C., Franco, Irene, Kang, Sang Won, Hirsch, Emilio, Quilliam, Lawrence A., and Varner, Judith A.

Subjects

*TUMOR treatment, *TUMOR growth, *IMMUNOSUPPRESSION, *NEOVASCULARIZATION, *METASTASIS, *MYELOID leukemia, *PHOSPHOINOSITIDE-dependent kinase-1, *INTEGRINS, *CANCER invasiveness, *INFLAMMATION

Abstract

Tumor inflammation, the recruitment of myeloid lineage cells into the tumor microenvironment, promotes angiogenesis, immunosuppression and metastasis. CD11b+Gr1lo monocytic lineage cells and CD11b+Gr1hi granulocytic lineage cells are recruited from the circulation by tumor-derived chemoattractants, which stimulate PI3-kinase γ (PI3Kγ)-mediated integrin α4 activation and extravasation. We show here that PI3Kγ activates PLCγ, leading to RasGrp/CalDAG-GEF-I&II mediated, Rap1a-dependent activation of integrin α4β1, extravasation of monocytes and granulocytes, and inflammation-associated tumor progression. Genetic depletion of PLCγ, CalDAG-GEFI or II, Rap1a, or the Rap1 effector RIAM was sufficient to prevent integrin α4 activation by chemoattractants or activated PI3Kγ (p110γCAAX), while activated Rap (RapV12) promoted constitutive integrin activation and cell adhesion that could only be blocked by inhibition of RIAM or integrin α4β1. Similar to blockade of PI3Kγ or integrin α4β1, blockade of Rap1a suppressed both the recruitment of monocytes and granulocytes to tumors and tumor progression. These results demonstrate critical roles for a PI3Kγ-Rap1a-dependent pathway in integrin activation during tumor inflammation and suggest novel avenues for cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2013

7. Myeloid Cells in the Tumor Microenvironment: Modulation of Tumor Angiogenesis and Tumor Inflammation.

Author

Schmid, Michael C. and Varner, Judith A.

Subjects

*TUMORS, *NEOVASCULARIZATION, *METASTASIS, *CANCER treatment, *INTERLEUKIN-6, *CLINICAL medicine research

Abstract

Myeloid cells are a heterogeneous population of bone marrow-derived cells that play a critical role during growth and metastasis of malignant tumors. Tumors exhibit significant myeloid cell infiltrates, which are actively recruited to the tumor micro environment. Myeloid cells promote tumor growth by stimulating tumor angiogenesis, suppressing tumor immunity, and promoting metastasis to distinct sites. In this review, we discuss the role of myeloid cells in promoting tumor angiogenesis. Furthermore, we describe a subset of myeloid cells with immunosuppressive activity (known as myeloid-derived suppressor cells). Finally, we will comment on the mechanisms regulating myeloid cell recruitment to the tumor microenvironment and on the potential of myeloid cells as new targets for cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2010

8. Myeloid cell trafficking and tumor angiogenesis

Author

Schmid, Michael C. and Varner, Judith A.

Subjects

*TUMOR growth, *METASTASIS, *CANCER invasiveness, *IMMUNE system

Abstract

Abstract: Tumor growth and metastasis depend on neovascularization, the growth of new blood vessels. Recent findings have revealed that tumor neovascularization is regulated in part by monocytes, which are myeloid lineage cells from the bone marrow. Tumors exhibit significant monocyte infiltrates, which are actively recruited to the tumor microenvironment. Upon tumor infiltration, monocytes can participate in tumor neovascularization. Monocytes can either differentiate into macrophages, which express proangiogenic growth factors, or into endothelial-like cells, which may directly participate in neovascularization. Preliminary studies in animals suggest that modulation of bone marrow-derived cell trafficking into tumors will provide a useful new approach in cancer therapy. [Copyright &y& Elsevier]

Published

2007