Your search keyword '"Saenger, Yvonne"' showing total 7 results

1. Urine Proteomics Link Complement Activation with Interstitial Fibrosis/Tubular Atrophy in Lupus Nephritis Patients.

Author

Wang, Shudan, Broder, Anna, Shao, Daming, Kesarwani, Vartika, Boderman, Brianna, Aguilan, Jennifer, Sidoli, Simone, Suzuki, Masako, Greally, John M., Saenger, Yvonne M., Rovin, Brad H., and Michelle Kahlenberg, J.

Abstract

Intrarenal complement activation has been implicated in the pathogenesis of tubulointerstitial fibrosis in lupus nephritis (LN) based on prior animal studies. The assembly of the membrane attack complex (MAC) by complement C5b to C9 on the cell membrane leads to cytotoxic pores and cell lysis, while CD59 inhibits MAC formation by preventing C9 from joining the complex. We hypothesize that complement activation and imbalance between complement activation and inhibition, as defined by increased production of individual complement components and uncontrolled MAC activation relative to CD59 inhibition, are associated with interstitial fibrosis and tubular atrophy (IFTA) in LN and correlate with the key mediators of kidney fibrosis- transforming growth factor receptors beta (TGFRβ), platelet-derived growth factor beta (PDGFβ) and platelet-derived growth factor receptor beta (PDGFRβ). We included urine samples from 46 adults and pediatric biopsy-proven lupus nephritis patients who underwent clinically indicated kidney biopsies between 2010 and 2019. We compared individual urinary complement components and the urinary C9-to-CD59 ratio between LN patients with moderate/severe IFTA and none/mild IFTA. IFTA was defined as none/mild (<25% of interstitium affected) versus moderate/severe (≥ 25% of interstitium affected). Proteomics analysis was performed using mass spectrometry (Orbitrap Fusion Lumos, Thermo Scientific) and processed by the Proteome Discoverer. Urinary complement proteins enriched in LN patients with moderate/severe IFTA were correlated with serum creatinine, TGFβR1, TGFβR2, PDGFβ, and PDGFRβ. Of the 46 LN patients included in the study, 41 (89.1%) were women, 20 (43.5%) self-identified as Hispanic or Latino, and 26 (56.5%) self-identified as Black or African American. Ten of the 46 (21.7%) LN patients had moderate/severe IFTA on kidney biopsy. LN patients with moderate/severe IFTA had an increased urinary C9-to-CD59 ratio [median 0.91 (0.83-1.05) vs 0.81 (0.76-0.91), p=0.01]. Urinary C3 and CFI levels in LN patients with moderate/severe IFTA were higher compared to those with none/mild IFTA [C3 median (IQR) 24.4(23.5-25.5) vs. 20.2 (18.5–22.2), p= 0.02], [CFI medium (IQR) 28.8 (21.8-30.6) vs. 20.4 (18.5-22.9), p=0.01]. Complement C9, CD59, C3 and CFI correlated with TGFβR1, PDGFβ, and PDGFRβ, while C9, CD59 and C3 correlated with TGFβR2. This study is one of the first to compare the urinary complement profile in LN patients with moderate/severe IFTA and none/mild IFTA in human tissues. This study identified C3, CFI, and C9-to-CD59 ratio as potential markers of tubulointerstitial fibrosis in LN. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

2. LBP-23-Prognostic Impact of Peritumoral Neutrophil Infiltration on Hepatocellular Carcinoma Recurrence Following Liver Transplantation

Author

Najjar, Marc, Halazun, Karim, Srivastava, Ayush, Moore, Michael, Chyong, Donian, Gartrell, Robyn, Rizk, Emanuelle, Lieberman, Evan, Perez, Olivia, Robbins-Juarez, Shelief, Drake, Charles, Fazlollahi, Ladan, Remotti, Helen, Emond, Jean, and Saenger, Yvonne

Published

2019

3. Activation of Toll-like Receptor-2 by Endogenous Matrix Metalloproteinase-2 Modulates Dendritic-Cell-Mediated Inflammatory Responses.

Author

Godefroy, Emmanuelle, Gallois, Anne, Idoyaga, Juliana, Merad, Miriam, Tung, Navpreet, Monu, Ngozi, Saenger, Yvonne, Fu, Yichun, Ravindran, Rajesh, Pulendran, Bali, Jotereau, Francine, Trombetta, Sergio, and Bhardwaj, Nina

Abstract

Summary Matrix metalloproteinase-2 (MMP-2) is involved in several physiological mechanisms, including wound healing and tumor progression. We show that MMP-2 directly stimulates dendritic cells (DCs) to both upregulate OX40L on the cell surface and secrete inflammatory cytokines. The mechanism underlying DC activation includes physical association with Toll-like receptor-2 (TLR2), leading to NF-κB activation, OX40L upregulation on DCs, and ensuing T H 2 differentiation. Significantly, MMP-2 polarizes T cells toward type 2 responses in vivo, in a TLR2-dependent manner. MMP-2-dependent type 2 polarization may represent a key immune regulatory mechanism for protection against a broad array of disorders, such as inflammatory, infectious, and autoimmune diseases, which can be hijacked by tumors to evade immunity. [ABSTRACT FROM AUTHOR]

Published

2014

4. Tissue-Resident Memory T Cells Mediate Immune Homeostasis in the Human Pancreas through the PD-1/PD-L1 Pathway.

Author

Weisberg, Stuart P., Carpenter, Dustin J., Chait, Michael, Dogra, Pranay, Gartrell-Corrado, Robyn D., Chen, Andrew X., Campbell, Sean, Liu, Wei, Saraf, Pooja, Snyder, Mark E., Kubota, Masaru, Danzl, Nichole M., Schrope, Beth A., Rabadan, Raul, Saenger, Yvonne, Chen, Xiaojuan, and Farber, Donna L.

Abstract

Non-recirculating tissue-resident memory T cells (TRMs) are the predominant T cell subset in diverse tissue sites, where they mediate protective immune responses in situ. Here, we reveal a role for TRM in maintaining immune homeostasis in the human pancreas through interactions with resident macrophages and the PD-1/PD-L1 inhibitory pathway. Using tissues obtained from organ donors, we identify that pancreas T cells comprise CD8+PD-1hi TRMs, which are phenotypically, functionally, and transcriptionally distinct compared to TRMs in neighboring jejunum and lymph node sites. Pancreas TRMs cluster with resident macrophages throughout the exocrine areas; TRM effector functions are enhanced by macrophage-derived co-stimulation and attenuated by the PD-1/PD-L1 pathways. Conversely, in samples from chronic pancreatitis, TRMs exhibit reduced PD-1 expression and reduced interactions with macrophages. These findings suggest important roles for PD-1 and TRM-macrophage interactions in controlling tissue homeostasis and immune dysfunctions underlying inflammatory disease, with important implications for PD-1-based immunotherapies. • The human pancreas contains CD8+ TRMs exhibiting tissue-specific molecular signatures • Pancreas TRMs express high levels of PD-1 yet maintain strong effector function • During homeostasis, pancreas TRMs are regulated by PD-L1+ tissue macrophages • In chronic pancreatitis, TRM PD-1 levels and PD-L1+ macrophage density are reduced Non-recirculating tissue-resident memory T cells (TRMs) mediate immune responses in non-lymphoid tissues. Using a human organ donor tissue resource, Weisberg et al. reveal that PD-1hi pancreas TRMs are regulated by PD-L1+ macrophages during homeostasis. Comparison with chronic pancreatitis patient samples shows how pancreas TRM regulation is altered during inflammation. [ABSTRACT FROM AUTHOR]

Published

2019

5. A Listeria Vaccine and Depletion of T-Regulatory Cells Activate Immunity Against Early Stage Pancreatic Intraepithelial Neoplasms and Prolong Survival of Mice.

Author

Keenan, Bridget P., Saenger, Yvonne, Kafrouni, Michel I., Leubner, Ashley, Lauer, Peter, Maitra, Anirban, Rucki, Agnieszka A., Gunderson, Andrew J., Coussens, Lisa M., Brockstedt, Dirk G., Dubensky, Thomas W., Hassan, Raffit, Armstrong, Todd D., and Jaffee, Elizabeth M.

Abstract

Background & Aims: Premalignant lesions and early stage tumors contain immunosuppressive microenvironments that create barriers for cancer vaccines. Kras G12D/+ ;Trp53 R172H/+ ;Pdx-1-Cre (KPC) mice, which express an activated form of Kras in pancreatic tissues, develop pancreatic intraepithelial neoplasms (PanIN) that progress to pancreatic ductal adenocarcinoma (PDA). We used these mice to study immune suppression in PDA. Methods: We immunized KPC and Kras G12D/+ ;Pdx-1-Cre mice with attenuated intracellular Listeria monocytogenes (which induces CD4+ and CD8+ T-cell immunity) engineered to express KrasG12D (LM-Kras). The vaccine was given alone or in sequence with an anti-CD25 antibody (PC61) and cyclophosphamide to deplete T-regulatory (Treg) cells. Survival times were measured; pancreatic and spleen tissues were collected and analyzed by histologic, flow cytometry, and immunohistochemical analyses. Results: Interferon γ–mediated, CD8+ T-cell responses were observed in KPC and Kras G12D/+ ;Pdx-1-Cre mice given LM-Kras, but not in unvaccinated mice. Administration of LM-Kras to KPC mice 4–6 weeks old (with early stage PanINs), depleted of Treg cells, significantly prolonged survival and reduced PanIN progression (median survival, 265 days), compared with unvaccinated mice (median survival, 150 days; P = .002), mice given only LM-Kras (median survival, 150 days; P = .050), and unvaccinated mice depleted of Treg cells (median survival, 170 days; P = .048). In 8- to 12-week-old mice (with late-stage PanINs), LM-Kras, alone or in combination with Treg cell depletion, did not increase survival time or slow PanIN progression. The combination of LM-Kras and Treg cell depletion reduced numbers of Foxp3+CD4+ T cells in pancreatic lymph nodes, increased numbers of CD4+ T cells that secrete interleukin 17 and interferon γ, and caused CD11b+Gr1+ cells in the pancreas to acquire an immunostimulatory phenotype. Conclusions: Immunization of KPC mice with Listeria monocytogenes engineered to express KrasG12D, along with depletion of Treg cells, reduces progression of early stage, but not late-stage, PanINs. This approach increases infiltration of the lesion with inflammatory cells. It might be possible to design immunotherapies against premalignant pancreatic lesions to slow or prevent progression to PDA. [Copyright &y& Elsevier]

Published

2014

6. Defining the role of CD2 in disease progression and overall survival among patients with completely resected stage-II to -III cutaneous melanoma.

Author

Harcharik, Sara, Bernardo, Sebastian, Moskalenko, Marina, Pan, Michael, Sivendran, Meera, Bell, Heather, Hall, Lawrence D., Castillo-Martín, Mireia, Fox, Kelly, Cordon-Cardo, Carlos, Chang, Rui, Sivendran, Shanthi, Phelps, Robert G., and Saenger, Yvonne

Abstract

Background: Accurate assessment of prognosis remains clinically challenging in stage II to III cutaneous melanoma. Studies have implicated CD2 in immune surveillance, T-cell activation, and antitumor immunity, but its role in melanoma progression warrants further investigation. Objective: We sought to investigate the prognostic role of CD2 in primary cutaneous melanoma. Methods: Patients with American Joint Committee on Cancer stage II and III cutaneous melanoma were identified by retrospective review of dermatopathology databases from 2001 to 2010 at Mount Sinai Medical Center and Geisinger Medical Center. Additional patients were provided by New York University Medical Center based on retrospective review and tissue availability. Immunohistochemistry was performed on tumors from 90 patients with known recurrence status and documented follow-up. Results: Primary tumors from patients who developed recurrent disease had fewer CD2+ cells (P = .0003). In multivariable analyses including standard clinicopathologic predictors, CD2 was an independent predictor of disease recurrence (P = .008) and overall survival (P = .007). CD2 count correlated with characterization of tumor-infiltrating lymphocytes (P = .0004). Among the intermediate prognosis group of patients with nonbrisk tumor-infiltrating lymphocytes, CD2 count was predictive of disease recurrence (P = .0006) and overall survival (P = .0318). Limitations: Our retrospective design may have resulted in incomplete representation of patients lacking documented follow-up. Conclusions: CD2 may be an independent predictor of disease recurrence and overall survival among patients with primary cutaneous melanoma. [Copyright &y& Elsevier]

Published

2014

7. Quality Assessment of Stereotactic Radiosurgery of a Melanoma Brain Metastases Model Using a Mouselike Phantom and the Small Animal Radiation Research Platform.

Author

Wu, Cheng-Chia, Chaudhary, Kunal R., Na, Yong Hum, Welch, David, Black, Paul J., Sonabend, Adam M., Canoll, Peter, Saenger, Yvonne M., Wang, Tony J.C., Wuu, Cheng-Shie, Hei, Tom K., and Cheng, Simon K.

Subjects

*STEREOTACTIC radiosurgery, *MAGNETIC resonance imaging, *CANCER cell analysis, *METASTASIS, *CANCER treatment, *LABORATORY mice, *ANIMAL experimentation, *ANTHROPOMETRY, *BRAIN tumors, *COMPUTED tomography, *DIAGNOSTIC imaging, *MELANOMA, *MICE, *IMAGING phantoms, *QUALITY assurance, *RADIATION doses, *RADIOSURGERY, *TIME, *CONTRAST media

Abstract

Purpose: To establish a novel preclinical model for stereotactic radiosurgery (SRS) with combined mouselike phantom quality assurance in the setting of brain metastases.Methods and Materials: C57B6 mice underwent intracranial injection of B16-F10 melanoma cells. T1-weighted postcontrast magnetic resonance imaging (MRI) was performed on day 11 after injection. The MRI images were fused with cone beam computed tomography (CBCT) images using the Small Animal Radiation Research Platform (SARRP). The gross tumor volume (GTV) was contoured using the MRI. A single sagittal arc using the 3 × 3 mm2 collimator was used to deliver 18 Gy prescribed to the isocenter. MRI was performed 7 days after radiation treatment, and the dose delivered to the mice was confirmed using 2 mouselike anthropomorphic phantoms: 1 in the axial orientation and the other in the sagittal orientation. The SARRP output was measured using a PTW Farmer type ionization chamber as per the American Association of Physicists in Medicine Task Group report 61, and the H-D curve was generated up to a maximum dose of 30 Gy. Irradiated films were analyzed based on optical density distribution and H-D curve.Results: The tumor volume on day 11, before intervention, was 2.48 ± 1.37 mm3 in the no-SRS arm versus 3.75 ± 1.19 mm3 in the SRS arm (NS). In the SRS arm, GTV maximum dose (Dmax) and mean dose were 2048 ± 207 and 1785 ± 14 cGy. Using the mouselike phantoms, the radiochromic film showed close precision in comparison with projected isodose lines, with a Dmax of 1903.4 and 1972.7 cGy, the axial and sagittal phantoms, respectively. Tumor volume 7 days after treatment was 7.34 ± 8.24 mm3 in the SRS arm and 60.20 ± 40.4 mm3 in the no-SRS arm (P=.009). No mice in the control group survived more than 22 days after implantation, with a median overall survival (mOS) of 19 days; mOS was not reached in the SRS group, with 1 death noted.Conclusions: Single-fraction SRS of 18 Gy delivered in a single arc can be delivered accurately with MRI T1-weighted postcontrast-based treatment planning. The mouse like phantom allows for verification of dose delivery and accuracy. [ABSTRACT FROM AUTHOR]

Published

2017