Your search keyword '"Maxwell Frankfurter"' showing total 5 results

1. Untangling sporadic brain arteriovenous malformations: towards targeting the KRAS/MAPK pathway

Author

Rashad Jabarkheel, Lun Li, Maxwell Frankfurter, Daniel Y. Zhang, Avi Gajjar, Najib Muhammad, Visish M. Srinivasan, Jan-Karl Burkhardt, and Mark Kahn

Subjects

arteriovenous malformation, sporadic, KRAS, MAPK, MEK inhibitor, Surgery, RD1-811

Abstract

Brain arteriovenous malformations (AVMs) are vascular lesions characterized by abnormal connections between parenchymal arteries and veins, bypassing a capillary bed, and forming a nidus. Brain AVMs are consequential as they are prone to rupture and associated with significant morbidity. They can broadly be subdivided into hereditary vs. sporadic lesions with sporadic brain AVMs representing the majority of all brain AVMs. However, little had been known about the pathogenesis of sporadic brain AVMs until the landmark discovery in 2018 that the majority of sporadic brain AVMs carry somatic activating mutations of the oncogene, Kirsten rat sarcoma viral oncogene homologue (KRAS), in their endothelial cells. Here, we review the history of brain AVMs, their treatments, and recent advances in uncovering the pathogenesis of sporadic brain AVMs. We specifically focus on the latest studies suggesting that pharmacologically targeting the KRAS/MEK pathway may be a potentially efficacious treatment for sporadic brain AVMs.

Published

2024

2. Cell-autonomous requirement for ACE2 across organs in lethal mouse SARS-CoV-2 infection.

Author

Alan T Tang, David W Buchholz, Katherine M Szigety, Brian Imbiakha, Siqi Gao, Maxwell Frankfurter, Min Wang, Jisheng Yang, Peter Hewins, Patricia Mericko-Ishizuka, N Adrian Leu, Stephanie Sterling, Isaac A Monreal, Julie Sahler, Avery August, Xuming Zhu, Kellie A Jurado, Mingang Xu, Edward E Morrisey, Sarah E Millar, Hector C Aguilar, and Mark L Kahn

Subjects

Biology (General), QH301-705.5

Abstract

Angiotensin-converting enzyme 2 (ACE2) is the cell-surface receptor for Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2). While its central role in Coronavirus Disease 2019 (COVID-19) pathogenesis is indisputable, there remains significant debate regarding the role of this transmembrane carboxypeptidase in the disease course. These include the role of soluble versus membrane-bound ACE2, as well as ACE2-independent mechanisms that may contribute to viral spread. Testing these roles requires in vivo models. Here, we report humanized ACE2-floxed mice in which hACE2 is expressed from the mouse Ace2 locus in a manner that confers lethal disease and permits cell-specific, Cre-mediated loss of function, and LSL-hACE2 mice in which hACE2 is expressed from the Rosa26 locus enabling cell-specific, Cre-mediated gain of function. Following exposure to SARS-CoV-2, hACE2-floxed mice experienced lethal cachexia, pulmonary infiltrates, intravascular thrombosis and hypoxemia-hallmarks of severe COVID-19. Cre-mediated loss and gain of hACE2 demonstrate that neuronal infection confers lethal cachexia, hypoxemia, and respiratory failure in the absence of lung epithelial infection. In this series of genetic experiments, we demonstrate that ACE2 is absolutely and cell-autonomously required for SARS-CoV-2 infection in the olfactory epithelium, brain, and lung across diverse cell types. Therapies inhibiting or blocking ACE2 at these different sites are likely to be an effective strategy towards preventing severe COVID-19.

Published

2023

3. SARS-CoV-2 infection of olfactory epithelial cells and neurons drives acute lung injury and lethal COVID-19 in mice

Author

Alan T. Tang, David W. Buchholz, Katherine M. Szigety, Brian Imbhiaka, Siqi Gao, Maxwell Frankfurter, Min Wang, Jisheng Yang, Peter Hewins, Patricia Mericko-Ishizuka, N Adrian Leu, Stephanie Sterling, Isaac A. Monreal, Julie Sahler, Avery August, Xuming Zhu, Kellie A. Jurado, Mingang Xu, Edward E. Morrisey, Sarah E. Millar, Hector C. Aguilar, and Mark L. Kahn

Subjects

Article

Abstract

Lethal COVID-19 is associated with respiratory failure that is thought to be caused by acute respiratory distress syndrome (ARDS) secondary to pulmonary infection. To date, the cellular pathogenesis has been inferred from studies describing the expression of ACE2, a transmembrane protein required for SARS-CoV-2 infection, and detection of viral RNA or protein in infected humans, model animals, and cultured cells. To functionally test the cellular mechanisms of COVID-19, we generated hACE2fl animals in which human ACE2 (hACE2) is expressed from the mouse Ace2 locus in a manner that permits cell-specific, Cre-mediated loss of function. hACE2fl animals developed lethal weight loss and hypoxemia within 7 days of exposure to SARS-CoV-2 that was associated with pulmonary infiltrates, intravascular thrombosis and patchy viral infection of lung epithelial cells. Deletion of hACE2 in lung epithelial cells prevented viral infection of the lung, but not weight loss, hypoxemia or death. Inhalation of SARS-CoV-2 by hACE2fl animals resulted in early infection of sustentacular cells with subsequent infection of neurons in the neighboring olfactory bulb and cerebral cortex— events that did not require lung epithelial cell infection. Pharmacologic ablation of the olfactory epithelium or Foxg1Cre mediated deletion of hACE2 in olfactory epithelial cells and neurons prevented lethality and neuronal infection following SARS-CoV-2 infection. Conversely, transgenic expression of hACE2 specifically in olfactory epithelial cells and neurons in Foxg1Cre; LSL-hACE2 mice was sufficient to confer neuronal infection associated with respiratory failure and death. These studies establish mouse loss and gain of function genetic models with which to genetically dissect viral-host interactions and demonstrate that lethal disease due to respiratory failure may arise from extrapulmonary infection of the olfactory epithelium and brain. Future therapeutic efforts focused on preventing olfactory epithelial infection may be an effective means of protecting against severe COVID-19.

Published

2021

4. FZD2 Regulates Murine Hair Follicle Function and Maintenance

Author

Donna M. Brennan-Crispi, Maxwell Frankfurter, Christina Murphy, Emily Sheng, Mingang Xu, Edward E. Morrisey, Sarah E. Millar, and Thomas H. Leung

Subjects

Mice, Animals, Cell Biology, Dermatology, Molecular Biology, Biochemistry, Hair Follicle

Published

2021

5. Overexpression of Desmoglein 2 in a Mouse Model of Gorlin Syndrome Enhances Spontaneous Basal Cell Carcinoma Formation through STAT3-Mediated Gli1 Expression

Author

Frédéric Charron, Sarah E. Millar, Andrew M. Overmiller, Julio C. Salas-Alanis, Molly R. Marous, Donna M. Brennan-Crispi, Felicia Cooper, Joya Sahu, Natalia A. Riobo-Del Galdo, Kathleen P. McGuinn, Ioanna Ch. Georgiou, Maxwell Frankfurter, Lukas Tamayo-Orrego, and Mỹ G. Mahoney

Subjects

0301 basic medicine, STAT3 Transcription Factor, Skin Neoplasms, Mice, Transgenic, Dermatology, Biochemistry, Zinc Finger Protein GLI1, Article, 03 medical and health sciences, Paracrine signalling, Mice, 0302 clinical medicine, GLI1, Cell Line, Tumor, medicine, Animals, Humans, Basal cell carcinoma, Hedgehog Proteins, Gene Knock-In Techniques, Sonic hedgehog, Phosphorylation, Autocrine signalling, Molecular Biology, Hedgehog, Skin, Desmoglein 2, biology, integumentary system, Cadherin, Chemistry, Basal Cell Nevus Syndrome, Cell Biology, medicine.disease, Molecular biology, Hedgehog signaling pathway, Patched-1 Receptor, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, biology.protein

Abstract

Activation of the hedgehog pathway is causative of virtually all sporadic and Gorlin syndrome-related basal cell carcinomas (BCCs), with loss of function of Ptc1 being the most common genomic lesion. Sporadic BCCs also overexpress Dsg2, a desmosomal cadherin normally found in the basal layer. Using a mouse model of Gorlin syndrome (Ptc1+/lacZ mice), we found that overexpressing Dsg2 in the basal layer (K14-Dsg2/Ptc1+/lacZ mice) or the superficial epidermis (Inv-Dsg2/Ptc1+/lacZ mice) resulted in increased spontaneous BCC formation at 3 and 6 months, respectively. The tumors did not show loss of heterozygosity of Ptc1, despite high levels of Gli1 and phosphorylated Stat3. A panel of sporadic human BCCs showed increased staining of both Dsg2 and phosphorylated Stat3 in all nine samples. Overexpression of Dsg2 in ASZ001 cells, a Ptc1–/– BCC cell line, induced Stat3 phosphorylation and further increased Gli1 levels, in both an autocrine and paracrine manner. Three different Stat3 inhibitors reduced viability and Gli1 expression in ASZ001 cells but not in HaCaT cells. Conversely, stimulation of Stat3 in ASZ001 cells with IL-6 increased Gli1 expression. Our results indicate that Dsg2 enhances canonical hedgehog signaling downstream of Ptc1 to promote BCC development through the activation of phosphorylated Stat3 and regulation of Gli1 expression.

Published

2018