Senior scientist at Marengo therapeutics
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Highly motivated, versatile Ph.D. scientist, with an extensive scientific background and industry experience in immuno-oncology, oncology, molecular biology, assay development and protein sciences. Effective, independent researcher and enthusiastic team contributor. Excellent communication, writing and supervisory skills.
Marengo (former Elstar) therapeutics, Cambridge, MA
Senior scientist, Immuno-oncology Mar 2022 to present
Scientist II, Immuno-oncology Sep 2019 to Feb 2022
Scientist I, Immuno-oncology Aug 2017-Sep 2019
--- Expanded T cells using bispecific Abs and detected expanded T cells using FACS
--- Measured TRBV selectivity using nanostring technologies
--- Worked on T cell activation assay and T cell proliferation assay
--- Cell binding studies
--- Worked on Ab internalization, target receptor density measurement
--- Did pstat5 signaling assay in PBMCs (T, NK, Treg)
--- Did signaling assays (pSLP76, pERK and pstat5)
--- Measured cytokines in the supernatant of PBMCs using 10-plex cytokine kit from MSD
--- Worked on ex vivo PD study (immune profiling of tumor, spleen and blood)
--- Prepared drug candidate data for filing IND
--- Prepared drug candidate data report for Ipsen
--- Worked on T cell engager molecules (signaling, cytotoxicity assays)
--- Planned & executed experiments, presented data in project team meetings to CSO, head of research and other people
--- Selected lead molecules of NK cell engager Abs by performing cell binding, NK cytotoxicity assay (NK cell line, primary NK/PBMCs)
--- Characterized lead molecules via NK cell activation and proliferation assay
--- Worked on model build and PD studies using NOG-IL15 mice injected with expanded NK cells, target cells and bispecific Abs
--- Worked on PD studies: immune profiling of tumors and spleen from mice to study the MOA of the antibodies
--- Screened TGFβtrap molecules using TGFβ reporter assay
MERRIMACK PHARMACEUTICALS, Cambridge, MA Jan 2009-April 2017
Scientist, Cancer cell biology
--- Studied mechanisms of action of MM141 by assessing its effects on receptor and downstream signaling pathways
--- Elucidated signaling networks related to IGF-IR and Insulin R (IR) and thus generated data to support MM141 model generation and combination therapy predictions
--- Quantified signaling protein levels in xenograft tumor tissues, by using western blot and Luminex
--- Generated stable cancer cell lines: knock down IGF-IR, ErbB3, IR and over-express IR
--- 3D spheroid assay showing the combination effect of MM141 and chemotherapeutic drug
--- RNA profiling on MM141 treated cell line samples
binding affinity using Octet, cell binding, ligand competition assay (ELISA),
epitope binning, binding on mouse/human chimeric receptors, poly-specificity assay.
--- Helped screening of lead antibody molecules in mouse syngeneic tumor models
--- Purified antibodies and did binding, epitope binning, Fc gamma receptor binding studies using Octet system, Cell line development to express therapeutic antibodies.
Scientist, Biology
2001 –2007
Postdoctoral fellow, Cancer metabolism and vascular biology
PI: Prof. Vikas Sukhatme (Victor J Aresty Prof. of Medicine, Chief academic officer of BIDMC);
Postdoctoral fellow, glycobiology
PI: Prof. Pamela Stanley (Horace W. Goldsmith professor, associate director for laboratory research of the Albert Einstein Cancer Center)
THE INSTITUTE OF MICROBIOLOGY, CHINESE ACADEMY OF SCIENCES, P.R. CHINA, 1995 –1998
Ph.D candidate, antibody engineering
PI: Prof. Po Tien and Prof. Xiyun Yan (Academicians of Chinese Academy of Sciences)