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23 results on '"Garfinkle, Elizabeth A. R."'

1. Cellular taxonomy of the preleukemic bone marrow niche of acute myeloid leukemia

Author

Goda, Chinmayee, Kulkarni, Rohan, Bustos, Yaphet, Li, Wenjun, Rudich, Alexander, Balcioglu, Ozlen, Chidester, Sadie, Urs, Amog P., Karunasiri, Malith, Al-Marrawi, Yzen, Korn, Erin, Kanna, Sanjay, Garfinkle, Elizabeth A. R., Shah, Nisarg, Wooten, Ashley, Mundy-Bosse, Bethany, Sehgal, Lalit, Zhang, Bin, Marcucci, Guido, Mardis, Elaine R., Garzon, Ramiro, Bowman, Robert L., Viny, Aaron D., Miles, Linde A., Miller, Katherine E., and Dorrance, Adrienne M.

Published
2025
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2. Multiomic profiling identifies predictors of survival in African American patients with acute myeloid leukemia

Author

Stiff, Andrew, Fornerod, Maarten, Kain, Bailee N., Nicolet, Deedra, Kelly, Benjamin J., Miller, Katherine E., Mrózek, Krzysztof, Boateng, Isaiah, Bollas, Audrey, Garfinkle, Elizabeth A. R., Momoh, Omolegho, Fasola, Foluke A., Olawumi, Hannah O., Mencia-Trinchant, Nuria, Kloppers, Jean F., van Marle, Anne-Cecilia, Hu, Eileen, Wijeratne, Saranga, Wheeler, Gregory, Walker, Christopher J., Buss, Jill, Heyrosa, Adrienne, Desai, Helee, Laganson, Andrea, Hamp, Ethan, Abu-Shihab, Yazan, Abaza, Hasan, Kronen, Parker, Sen, Sidharth, Johnstone, Megan E., Quinn, Kate, Wronowski, Ben, Hertlein, Erin, Miles, Linde A., Mims, Alice S., Oakes, Christopher C., Blachly, James S., Larkin, Karilyn T., Mundy-Bosse, Bethany, Carroll, Andrew J., Powell, Bayard L., Kolitz, Jonathan E., Stone, Richard M., Duarte, Cassandra, Abbott, Diana, Amaya, Maria L., Jordan, Craig T., Uy, Geoffrey L., Stock, Wendy, Archer, Kellie J., Paskett, Electra D., Guzman, Monica L., Levine, Ross L., Menghrajani, Kamal, Chakravarty, Debyani, Berger, Michael F., Bottomly, Daniel, McWeeney, Shannon K., Tyner, Jeffrey W., Byrd, John C., Salomonis, Nathan, Grimes, H. Leighton, Mardis, Elaine R., and Eisfeld, Ann-Kathrin

Published
2024
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5. Combinatorial macrophage induced innate immunotherapy against Ewing sarcoma: Turning “Two Keys” simultaneously

Author

Luo, Wen, Hoang, Hai, Miller, Katherine E., Zhu, Hongwen, Xu, Serena, Mo, Xiaokui, Garfinkle, Elizabeth A. R., Costello, Heather, Wijeratne, Saranga, Chemnitz, Wiebke, Gandhi, Ronan, Liao, Yanling, Ayello, Janet, Gardenswartz, Aliza, Rosenblum, Jeremy M., Cassady, Kevin A., Mardis, Elaine R., Lee, Dean A., Cripe, Timothy P., and Cairo, Mitchell S.

Published
2024
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6. Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia

Author

Kamens, Jennifer L., Nance, Stephanie, Koss, Cary, Xu, Beisi, Cotton, Anitria, Lam, Jeannie W., Garfinkle, Elizabeth A. R., Nallagatla, Pratima, Smith, Amelia M. R., Mitchell, Sharnise, Ma, Jing, Currier, Duane, Wright, William C., Kavdia, Kanisha, Pagala, Vishwajeeth R., Kim, Wonil, Wallace, LaShanale M., Cho, Ji-Hoon, Fan, Yiping, Seth, Aman, Twarog, Nathaniel, Choi, John K., Obeng, Esther A., Hatley, Mark E., Metzger, Monika L., Inaba, Hiroto, Jeha, Sima, Rubnitz, Jeffrey E., Peng, Junmin, Chen, Taosheng, Shelat, Anang A., Guy, R. Kiplin, and Gruber, Tanja A.

Published
2023
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7. Author Correction: Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia

Author

Kamens, Jennifer L., Nance, Stephanie, Koss, Cary, Xu, Beisi, Cotton, Anitria, Lam, Jeannie W., Garfinkle, Elizabeth A. R., Nallagatla, Pratima, Smith, Amelia M. R., Mitchell, Sharnise, Ma, Jing, Currier, Duane, Wright, William C., Kavdia, Kanisha, Pagala, Vishwajeeth R., Kim, Wonil, Wallace, LaShanale M., Cho, Ji-Hoon, Fan, Yiping, Seth, Aman, Twarog, Nathaniel, Choi, John K., Obeng, Esther A., Hatley, Mark E., Metzger, Monika L., Inaba, Hiroto, Jeha, Sima, Rubnitz, Jeffrey E., Peng, Junmin, Chen, Taosheng, Shelat, Anang A., Guy, R. Kiplin, and Gruber, Tanja A.

Published
2023
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8. Comprehensive genomic characterization of hematologic malignancies at a pediatric tertiary care center.

Author

Kebede, Ann M., Garfinkle, Elizabeth A. R., Mathew, Mariam T., Varga, Elizabeth, Colace, Susan I., Wheeler, Gregory, Kelly, Benjamin J., Schieffer, Kathleen M., Miller, Katherine E., Mardis, Elaine R., Cottrell, Catherine E., and Potter, Samara L.

Subjects
NUCLEOTIDE sequencing, SINGLE nucleotide polymorphisms, HEMATOLOGIC malignancies, PEDIATRIC oncology, PEDIATRIC therapy
Abstract

Despite the increasing availability of comprehensive next generation sequencing (NGS), its role in characterizing pediatric hematologic malignancies remains undefined. We describe findings from comprehensive genomic profiling of hematologic malignancies at a pediatric tertiary care center. Patients enrolled on a translational research protocol to aid in cancer diagnosis, prognostication, treatment, and detection of cancer predisposition. Disease-involved samples underwent exome and RNA sequencing and analysis for single nucleotide variation, insertion/deletions, copy number alteration, structural variation, fusions, and gene expression. Twenty-eight patients with hematologic malignancies were nominated between 2018-2021. Eighteen individuals received both germline and somatic sequencing; two received germline sequencing only. Germline testing identified patients with cancer predisposition syndromes and non-cancer carrier states. Fifteen patients (15/18, 83%) had cancer-relevant somatic findings. Potential therapeutic targets were identified in seven patients (7/18, 38.9%); three (3/7, 42.9%) received targeted therapies and remain in remission an average of 47 months later. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Myelomodulatory treatments augment the therapeutic benefit of oncolytic viroimmunotherapy in murine models of malignant peripheral nerve sheath tumors.

Author

Paudel, Siddhi N., Hutzen, Brian J., Miller, Katherine E., Garfinkle, Elizabeth A. R., Chun-Yu Chen, Pin-Yi Wang, Glaspell, Andrea M., Currier, Mark A., Ringwalt, Emily M., Boon, Louis, Mardis, Elaine R., Cairo, Mitchell S., Ratner, Nancy, Dodd, Rebecca D., Cassady, Kevin A., and Cripe, Timothy P.

Subjects
SCHWANNOMAS, PERIPHERAL nerve tumors, MYELOID-derived suppressor cells, MYELOID cells, HERPES simplex virus, AZACITIDINE, SMALL molecules
Abstract

Introduction: Malignant peripheral nerve sheath tumors (MPNST) pose a significant therapeutic challenge due to high recurrence rates after surgical resection and a largely ineffective response to traditional chemotherapy. An alternative treatment strategy is oncolytic viroimmunotherapy, which can elicit a durable and systemic antitumor immune response and is Food and Drug Administration (FDA)-approved for the treatment of melanoma. Unfortunately, only a subset of patients responds completely, underscoring the need to address barriers hindering viroimmunotherapy effectiveness. Methods: Here we investigated the therapeutic utility of targeting key components of the MPNST immunosuppressive microenvironment to enhance viroimmunotherapy's antitumor efficacy in three murine models, one of which showed more immunogenic characteristics than the others. Results: Myelomodulatory therapy with pexidartinib, a small molecule inhibitor of CSF1R tyrosine kinase, and the oncolytic herpes simplex virus T-VEC exhibited the most significant increase in median survival time in the highly immunogenic model. Additionally, targeting myeloid cells with the myelomodulatory therapy trabectedin, a small molecule activator of caspase-8 dependent apoptosis, augmented the survival benefit of T-VEC in a less immunogenic MPNST model. However, tumor regressions or shrinkages were not observed. Depletion experiments confirmed that the enhanced survival benefit relied on a T cell response. Furthermore, flow cytometry analysis following combination viroimmunotherapy revealed decreased M2 macrophages and myeloid-derived suppressor cells and increased tumor-specific gp70+ CD8 T cells within the tumor microenvironment. Discussion: In summary, our findings provide compelling evidence for the potential to leverage viroimmunotherapy with myeloid cell targeting against MPNST and warrant further investigation. [ABSTRACT FROM AUTHOR]

Published
2024
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12. A Novel Humanized Murine Model to Identify Neoantigen-Specific T Cells in CBFA2T3-GLIS2 Positive Acute Megakaryoblastic Leukemia

Author

Garfinkle, Elizabeth A. R., primary, Crawford, Jeremy Chase, additional, Zamora, Anthony E., additional, Croft, Nathan P., additional, Purcell, Anthony W., additional, Cotton, Anitria, additional, Kirk, Allison, additional, Chou, Ching-Heng, additional, Thomas, Paul G., additional, and Gruber, Tanja Andrea, additional

Published
2021
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13. Corrigendum: Myelomodulatory treatments augment the therapeutic benefit of oncolytic viroimmunotherapy in murine models of malignant peripheral nerve sheath tumors.

Author

Paudel, Siddhi N., Hutzen, Brian J., Miller, Katherine E., Garfinkle, Elizabeth A. R., Chun-Yu Chen, Pin-Yi Wang, Glaspell, Andrea M., Currier, Mark A., Ringwalt, Emily M., Boon, Louis, Mardis, Elaine R., Cairo, Mitchell S., Ratner, Nancy, Dodd, Rebecca D., Cassady, Kevin A., and Cripe, Timothy P.

Subjects
SCHWANNOMAS, PERIPHERAL nerve tumors
Abstract

This document is a corrigendum for an article titled "Myelomodulatory treatments augment the therapeutic benefit of oncolytic viroimmunotherapy in murine models of malignant peripheral nerve sheath tumors." The corrigendum addresses an error in the legend for Figure 1, where the tumor models were mistakenly referred to as xenografts instead of syngeneic models. The corrected legend clarifies that the study used syngeneic tumor models. The authors apologize for the error and state that it does not affect the scientific conclusions of the article. [Extracted from the article]

Published
2024
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15. Tucetona isabellae Valentich-Scott & Garfinkle, new species

Author

Valentich-Scott, Paul and Garfinkle, Elizabeth A. R.

Subjects
Mollusca, Arcoida, Animalia, Tucetona, Glycymerididae, Tucetona isabellae, Biodiversity, Taxonomy, Bivalvia
Abstract

Tucetona isabellae Valentich-Scott & Garfinkle, new species Figures 1 A ���G Glycymeris (Glycymeris) cabazoni Bramkamp, 1935, unnumbered pages, plate 2, figures 2, 3; Tucetona (Bellaxinaea) new species, Powell, 1986: 79 ���81, plate 2, figures 5, 7. Shell shape. Subovate to subtrigonal, moderately inflated, height and length about equal; beaks narrow, pointed, opisthogyrate. Sculpture and color. About 29 (20���48, n= 15) heavy, broad radial ribs, many bifurcate in larger specimens, overlain by strong, fine, well-spaced, commarginal ribs forming crossbars over ribs and in interspaces; interspaces moderately wide, frequently with intercalary ribs; periostracum inconspicuous; exterior color tan, with few dark brown blotches; interior color white to cream, with brown mottling in some specimens, some specimens mostly brown internally. Hinge. Hinge plate curved, narrow, posterior tooth series about 8 (4���11, n= 10), anterior about 7 (3���11), ligament asymmetrical, much longer anteriorly, moderate in length, moderately narrow, with about 3 (2���6) chevron grooves. Adductor muscle and pallial scars. Moderate in size, moderately impressed, anterior scar subovate, posterior scar ovate-elongate; pallial line narrow, with long, narrow dorsally directed lines extending from it. Inner ventral crenulations. About 24 (14���43) rectangular, flat topped. Distribution. Modern specimens are only known from a small region off the northwest end of Isla Smith, Baja California, Mexico (29.1�� N), 120��� 170 m. Fossil specimens are present in the late Miocene ���Imperial��� Formation in Riverside County, southern California (Powell, 1986; 1988). Type locality and type specimens. Mexico, Baja California, off the northwest end of Isla Smith; 29 ��05��� 12 ���N, 113 �� 32 ��� 12 ���W; 120��� 170 m. All paratypes listed below are from the same lot as the holotype. Holotype. SBMNH 149636, length 14.5 mm, height 15.0 mm. Paratypes. SBMNH 149637, 34 paired valves, 31 separate valves; BMNH 20100629, 2 paired valves, 2 separate valves; CASIZ 184502, 3 paired valves; USNM (1149245), 2 paired valves, 2 separate valves. Etymology. Named in honor of Isabella M. A. Rocha from Santa Barbara, California, a close friend of the junior author. Comparisons. Tucetona isabellae differs from Tucetona bicolor Reeve, 1843 (Figures 1 H���J), which has a subtrigonal shell shape, about 39 radial ribs with moderately shallow, very narrow interspaces, with very fine, very closely spaced commarginal ribs, and a moderately wide, curved hinge plate. Tucetona multicostata G. B. S ow e r b y I, 1833 (Figures 1 K���M) has a subovate shell shape, about 32 non-bifurcate radial ribs with wide, deep interspaces, with moderately spaced commarginal ribs, and a moderately wide, curved hinge plate. Tucetona isabellae differs from Tucetona strigilata G. B. Sowerby I, 1833 (Figures 1 N���P), which has a subtrigonal shell shape, about 24 non-bifurcate radial ribs with moderately wide, moderately shallow interspaces, with very fine, closely spaced commarginal ribs, and a wide hinge plate with curved teeth. The North Atlantic Tucetona pectinata (Gmelin, 1791) has fewer, non-bifurcating radial ribs with narrow interspaces when compared to T. isabellae. The new species has a similar number of radial ribs when compared to the northern Atlantic Tucetona subtilis Nicol, 1956, but the ribs are not bifurcate, and the latter species has fewer teeth on the hinge plate. Remarks. Tucetona isabellae has also been found in the fossil record although never formally described (Bramkamp, 1935; Powell, 1986). Powell (1986) compares this species to two fossil species from Venezuela and Columbia, both of which have significant differences in dentition and ligamental grooves, and thus are not included in the comparisons above. We have done a close examination of the Panamic members of the genus Tucetona and found that it has been difficult to differentiate the species. Many of the specimens in the museum collections we examined were incorrectly identified due to a misunderstanding of important characters within the genus. We found that the most distinct differences between the different Panamic species were, 1) presence or absence of rib bifurcation, 2) width and depth of interspaces, 3) size of the commarginal ribs, and 4) the width of the hinge plate. These characters alone can still sometimes lead to incorrect identifications. Further study, using molecular tools, likely would produce additional characters and might lead to the discovery of additional new species., Published as part of Valentich-Scott, Paul & Garfinkle, Elizabeth A. R., 2011, A new species of Tucetona (Bivalvia: Glycymerididae) from Mexico, pp. 65-68 in Zootaxa 2769 on pages 65-67, DOI: 10.5281/zenodo.276860, {"references":["Bramkamp, R. A. (1935) Stratigraphy and molluscan fauna of the Imperial Formation of San Gorgonio Pass, California. Unpublished Ph. D. dissertation, University of California, Berkeley, 86 pp. + unnumbered pages, 10 pl.","Powell, C. L., II (1986) Stratigraphy and bivalve molluscan paleontology of the Neogene Imperial Formation in Riverside County, California. Unpublished M. S. thesis, San Jose State University, San Jose, California, 324 pp., 13 pl.","Powell, C. L., II (1988) The Miocene and Pliocene Imperial Formation of southern California and its molluscan fauna: an overview. Western Society of Malacologists Annual Report, 20, 11 - 18.","Reeve, L. A. (1843) Monograph of the genus Pectunculus. Conchologia iconica; or, illustrations of the shells of molluscous animals, 1, 9 pls.","Sowerby, G. B., I (1833) [... the collection of shells formed by Mr. Cuming on the western coast of South America, and among the islands of the southern Pacific Ocean]. Proceedings of Zoological Society of London, 1832, 194 - 202.","Gmelin, J. F. (1791) Caroli a Linne ... Systema naturae per regna tria naturae ... editio decima tertia, acuta, reformata, Lepzig (Beer), 1 (6), 3021 - 3910.","Nicol, D. (1956) Distribution of living glycymerids with a new species from Bermuda. The Nautilus, 70, 48 - 53."]}

Published
2011
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16. Tucetona Iredale 1931

Author

Valentich-Scott, Paul and Garfinkle, Elizabeth A. R.

Subjects
Mollusca, Arcoida, Animalia, Tucetona, Glycymerididae, Biodiversity, Taxonomy, Bivalvia
Abstract

Genus Tucetona Iredale, 1931 Pectunculus Lamarck, 1799, non da Costa, 1778. Type species (monotypy): Arca pectunculus Linnaeus, 1758. Holocene, IndoPacific. Tucetona Iredale, 1931. Type species (original designation): Pectunculus flabellatus Tenison-Woods, 1878. Holocene, southwestern Pacific. Bellaxinaea Nicol & Jones, 1984. Type species (original designation): Axinaea intercostata Gabb, 1860. Eocene��� Oligocene, southeastern U.S. Description. Shell subcircular to subtrigonal; beaks orthogyrate, small to moderate in size, narrow to broad; sculpture of about 18���46 rounded to rectangular radial ribs, bifurcate in some species, commarginal striae weak to strong; interspaces narrow to moderately wide, shallow to moderately deep; posterior and anterior adductor scars and pallial line well impressed; hinge plate moderately curved, narrow to moderately wide; teeth straight to moderately curved; hinge plate of about 18���20 taxodont teeth; ligament with 3���5 chevron grooves. This genus differs from Axinactis M��rch, 1861, which has fewer, wider radial ribs with moderately wide interspaces, deep radial grooves on the ribs and interspaces, and a moderately broad beak. This genus differs from Glycymeris da Costa, 1778, which has low, rounded, smooth radial ribs that do not bifurcate, narrow interspaces, and a narrow beak. Species with a greater tendency for rib splitting, such as Tucetona bicolor Reeve, 1843, have been segregated as subgenus Bellaxinaea., Published as part of Valentich-Scott, Paul & Garfinkle, Elizabeth A. R., 2011, A new species of Tucetona (Bivalvia: Glycymerididae) from Mexico, pp. 65-68 in Zootaxa 2769 on page 65, DOI: 10.5281/zenodo.276860, {"references":["Iredale, T. (1931) Australian molluscan notes, No. 1. Records of the Australian Museum, 18, 201 - 235, pls. 22 - 25.","Lamarck, J. B. P. A. (1799) Prodrome d'une nouvelle classification des coquilles, comprenant une redaction appropriee des caracteres generiques, et l'etablissement d'un grand nombre de genres nouveaux. Memoires de la Societe d'Histoire Naturelle de Paris, 1, 63 - 91.","da Costa, E. M. (1778) Historia naturalis testaceorum Britanniae, or the British Conchology. Containing the descriptions and other particulars of natural history of the shells of Great Britain and Ireland: illustrated with figures. London (the author). xii + 254 + [x] pp., 17 pls.","Linnaeus, C. (1758) Systema naturae per regna tria naturae ... editio decima, reformata, vol. 1 (Regnum animale). Stockholm (Salvii), 824 + iii pp.","Tenison-Woods, J. E. (1878) On some new marine Mollusca. Transactions and Proceedings of the Royal Society of Victoria, 14, 55 - 65.","Nicol, D. & Jones, D. S. (1984) Bellaxinaea, a new subgenus of glycymeridids (Pelecypoda) from the western Hemisphere. The Nautilus, 98, 126 - 128.","Gabb, W. M. (1860) Descriptions of new species of American Tertiary and Cretaceous fossils. Journal of the Academy of Natural Sciences of Philadelphia, series 2, 4, 375 - 406, pls. 67 - 69.","Morch, O. A. L. (1861 in 1859 - 1861) Beitrage zur Molluskenfauna Central-Amerika's. Malakozoologische Blatter 6, 102 - 126 (Oct. 1859); 7 (2), 66 - 96 (July 1860); (3), 97 - 106 (Aug); (4), 170 - 192 (Dec.); (5), 193 - 213 (Jan. 1861).","Reeve, L. A. (1843) Monograph of the genus Pectunculus. Conchologia iconica; or, illustrations of the shells of molluscous animals, 1, 9 pls."]}

Published
2011
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17. Identification of Clinical and Biologic Correlates Associated With Outcome in Children With Adrenocortical Tumors Without Germline TP53 Mutations: A St Jude Adrenocortical Tumor Registry and Children's Oncology Group Study.

Author

Pinto, Emilia Modolo, Rodriguez-Galindo, Carlos, Pounds, Stanley B., Wang, Lei, Clay, Michael R., Neale, Geoffrey, Garfinkle, Elizabeth A. R., Lam, Catherine G., Levy, Carolyn Fein, Pappo, Alberto S., Zambetti, Gerard P., and Ribeiro, Raul C.

Published
2017
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19. A review of North American Recent Radiolucina (Bivalvia, Lucinidae) with the description of a new species.

Author

Garfinkle, Elizabeth A. R.

Subjects
*LUCINIDAE, *BIOLOGICAL specimens, *SPECIES diversity, *BIOLOGICAL classification
Abstract

North American members in the genus Radiolucina are reviewed. A lectotype for the type species, Radiolucina amianta, is designated and descriptions and illustrations are provided. A description of a new species, Radiolucina jessicae, from the west coast of Mexico is presented. Key diagnostic species characteristics are outlined and compared among members of the genus. [ABSTRACT FROM AUTHOR]

Published
2012
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20. Single Nuclei Sequencing Reveals Intratumoral Cellular Heterogeneity and Replication Stress in Adrenocortical Carcinoma.

Author

Popova LV, Garfinkle EAR, Chopyk DM, Navarro JB, Rivaldi A, Shu Y, Lomonosova E, Phay JE, Miller BS, Sattuwar S, Mullen M, Mardis ER, Miller KE, and Dedhia PH

Abstract

Adrenocortical carcinoma (ACC) is a rare endocrine malignancy with a poor prognosis and limited treatment options. Bulk genomic characterization of ACC has not yielded obvious therapeutic or immunotherapeutic targets, yet novel therapies are needed. We hypothesized that elucidating the intratumoral cellular heterogeneity by single nuclei RNA sequencing analyses would yield insights into potential therapeutic vulnerabilities of this disease. In addition to characterizing the immune cell and fibroblast landscape, our analyses of single nuclei gene expression profiles identified an adrenal cortex cell cluster exhibiting a program of replication stress and DNA damage response in primary and metastatic ACC. In vitro assessment of replication stress and DNA damage response using an ACC cell line and a series of newly-derived hormonally active patient-derived tumor organoids revealed ATR sensitivity. These findings provide novel mechanistic insight into ACC biology and suggest that an underlying dependency on ATR may be leveraged therapeutically in advanced ACC.

Published
2024
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21. Integrating Multisector Molecular Characterization into Personalized Peptide Vaccine Design for Patients with Newly Diagnosed Glioblastoma.

Author

Johanns TM, Garfinkle EAR, Miller KE, Livingstone AJ, Roberts KF, Rao Venkata LP, Dowling JL, Chicoine MR, Dacey RG, Zipfel GJ, Kim AH, Mardis ER, and Dunn GP

Subjects
Humans, Female, Male, Middle Aged, Brain Neoplasms immunology, Brain Neoplasms therapy, Brain Neoplasms genetics, Brain Neoplasms pathology, Adult, Aged, Immunotherapy methods, Protein Subunit Vaccines, Glioblastoma immunology, Glioblastoma therapy, Glioblastoma genetics, Glioblastoma pathology, Cancer Vaccines immunology, Cancer Vaccines administration & dosage, Cancer Vaccines therapeutic use, Vaccines, Subunit immunology, Vaccines, Subunit administration & dosage, Vaccines, Subunit therapeutic use, Precision Medicine methods, Antigens, Neoplasm immunology
Abstract

Purpose: Outcomes for patients with glioblastoma (GBM) remain poor despite multimodality treatment with surgery, radiation, and chemotherapy. There are few immunotherapy options due to the lack of tumor immunogenicity. Several clinical trials have reported promising results with cancer vaccines. To date, studies have used data from a single tumor site to identify targetable antigens, but this approach limits the antigen pool and is antithetical to the heterogeneity of GBM. We have implemented multisector sequencing to increase the pool of neoantigens across the GBM genomic landscape that can be incorporated into personalized peptide vaccines called NeoVax., Patients and Methods: In this study, we report the findings of four patients enrolled onto the NeoVax clinical trial (NCT0342209)., Results: Immune reactivity to NeoVax neoantigens was assessed in peripheral blood mononuclear cells pre- and post-NeoVax for patients 1 to 3 using IFNγ-ELISPOT assay. A statistically significant increase in IFNγ producing T cells at the post-NeoVax time point for several neoantigens was observed. Furthermore, a post-NeoVax tumor biopsy was obtained from patient 3 and, upon evaluation, revealed evidence of infiltrating, clonally expanded T cells., Conclusions: Collectively, our findings suggest that NeoVax stimulated the expansion of neoantigen-specific effector T cells and provide encouraging results to aid in the development of future neoantigen vaccine-based clinical trials in patients with GBM. Herein, we demonstrate the feasibility of incorporating multisector sampling in cancer vaccine design and provide information on the clinical applicability of clonality, distribution, and immunogenicity of the neoantigen landscape in patients with GBM., (©2024 The Authors; Published by the American Association for Cancer Research.)

Published
2024
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22. CBFA2T3-GLIS2-dependent pediatric acute megakaryoblastic leukemia is driven by GLIS2 and sensitive to navitoclax.

Author

Neault M, Lebert-Ghali CÉ, Fournier M, Capdevielle C, Garfinkle EAR, Obermayer A, Cotton A, Boulay K, Sawchyn C, St-Amand S, Nguyen KH, Assaf B, Mercier FE, Delisle JS, Drobetsky EA, Hulea L, Shaw TI, Zuber J, Gruber TA, Melichar HJ, and Mallette FA

Subjects
Animals, Mice, Child, Humans, Aniline Compounds, Sulfonamides, Oncogene Proteins, Fusion metabolism, Repressor Proteins, Leukemia, Megakaryoblastic, Acute drug therapy, Leukemia, Megakaryoblastic, Acute genetics
Abstract

Pediatric acute megakaryoblastic leukemia (AMKL) is an aggressive blood cancer associated with poor therapeutic response and high mortality. Here we describe the development of CBFA2T3-GLIS2-driven mouse models of AMKL that recapitulate the phenotypic and transcriptional signatures of the human disease. We show that an activating Ras mutation that occurs in human AMKL increases the penetrance and decreases the latency of CBF2AT3-GLIS2-driven AMKL. CBFA2T3-GLIS2 and GLIS2 modulate similar transcriptional networks. We identify the dominant oncogenic properties of GLIS2 that trigger AMKL in cooperation with oncogenic Ras. We find that both CBFA2T3-GLIS2 and GLIS2 alter the expression of a number of BH3-only proteins, causing AMKL cell sensitivity to the BCL2 inhibitor navitoclax both in vitro and in vivo, suggesting a potential therapeutic option for pediatric patients suffering from CBFA2T3-GLIS2-driven AMKL., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2023
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23. Analysis of rare driving events in pediatric acute myeloid leukemia.

Author

Noort S, Oosterwijk JV, Ma J, Garfinkle EAR, Nance S, Walsh M, Song G, Reinhardt D, Pigazzi M, Locatelli F, Hasle H, Abrahamsson J, Jarosova M, Kelaidi C, Polychronopoulou S, Van den Heuvel-Eibrink MM, Fornerod M, Gruber TA, and Zwaan CM

Subjects
Child, Adult, Humans, Nucleophosmin, Mutation, Transcriptome, Prognosis, Sarcoma, Ewing, Leukemia, Myeloid, Acute diagnosis, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute metabolism
Abstract

Elucidating genetic aberrations in pediatric acute myeloid leukemia (AML) provides insight in biology and may impact on risk-group stratification and clinical outcome. This study aimed to detect such aberrations in a selected series of samples without known (cyto)genetic aberration using molecular profiling. A cohort of 161 patients was selected from various study groups: DCOG, BFM, SJCRH, NOPHO and AEIOP. Samples were analyzed using RNA sequencing (n=152), whole exome (n=135) and/or whole genome sequencing (n=100). In 70 of 156 patients (45%), of whom RNA sequencing or whole genome sequencing was available, rearrangements were detected, 22 of which were novel; five involving ERG rearrangements and four NPM1 rearrangements. ERG rearrangements showed self-renewal capacity in vitro, and a distinct gene expression pattern. Gene set enrichment analysis of this cluster showed upregulation of gene sets derived from Ewing sarcoma, which was confirmed comparing gene expression profiles of AML and Ewing sarcoma. Furthermore, NPM1-rearranged cases showed cytoplasmic NPM1 localization and revealed HOXA/B gene overexpression, as described for NPM1 mutated cases. Single-gene mutations as identified in adult AML were rare. Patients had a median of 24 coding mutations (range, 7-159). Novel recurrent mutations were detected in UBTF (n=10), a regulator of RNA transcription. In 75% of patients an aberration with a prognostic impact could be detected. Therefore, we suggest these techniques need to become standard of care in diagnostics.

Published
2023
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