# Exploiting metabolic reprogramming to target IDH1 mutated cholangiocarcinoma

> **NIH NIH K99** · MASSACHUSETTS GENERAL HOSPITAL · 2021 · $178,200

## Abstract

Project Summary
Considerable interests in understanding and developing therapeutics for cancer have been to study oncogenic
lesion reprogrammed metabolism that is the hallmark of cancer. Gain-of-function hot-spot mutations in the
isocitrate dehydrogenase genes (IDH) are among the most common genetic alterations in intrahepatic
cholangiocarcinoma (ICC). The IDH mutations lead to production of an oncometabolite 2-hydroxygluatrate that
perturbs epigenetics and other cellular processes. However, it was not clear how oncogenic IDH1 mutations alter
metabolism that could underlie novel vulnerabilities in ICC. To uncover novel insights in IDH1 mutant ICC, we
have established and characterized an IDH1 mutant ICC mouse model (GEMM), as well as patient derived
models for in vivo disease biology. Leveraging these models, we demonstrate that mutant IDH1 reprograms
metabolism including suppression of mitochondrial function and selective hinderance of de novo pyrimidine
synthesis, which underlie novel metabolic vulnerability. Coherently, we identified from large-scale screens
selective and potent chemical and genetic vulnerabilities of IDH1 mutant cells that impinge on nucleotide
metabolism. As such, an important scientific goal, and that of this NIH Pathway to Independence, are to further
understand cellular and physiological basis underpinning the crosstalk between reprogrammed metabolism and
vulnerabilities for future therapy development. I propose an innovative research program combining cutting-edge
metabolomics, proteomics, as well as classic biochemistry, genetics and chemical biology approaches to obtain
mechanistic and translational insights in the novel metabolic vulnerabilities of IDH1 mutant ICC using my human
and GEMM models. I hypothesize that oncogenic IDH1 mutations lead to reprogrammed nucleotide synthesis
that can be leveraged upon to target IDH1 mutant ICC. I will focus on three specific aims: 1) understanding the
cellular mechanisms of mutant IDH1 reprogrammed pyrimidine synthesis and its genetic vulnerability; 2)
elucidating how pharmacologic modulation of nucleotide synthesis disrupts DNA replication and accumulates
DNA damage underlying the hypersensitivity of IDH1 mutant cells; and 3) identifying in vivo determinants of IDH1
mutant ICC sensitivity to drug treatments. Dr. Nabeel Bardeesy's laboratory and Massachusetts General Hospital
Cancer Center provide an ideal training environment for the proposed research. I will avail the outstanding
mentorships with a spectrum of expertise in metabolism, DNA damage, chemical biology, proteomic analysis,
and clinical oncology. Thus, I will acquire necessary trainings in DNA damage response pathways, quantitative
proteomics and pre-clinical compound characterizations for mechanistic and translational research during the
mentored K99 phase. The Pathway to Independence Award will enable me to expand my scientific and technical
repertoire and develop a hypothesis-driven research program, with which I w...

## Key facts

- **NIH application ID:** 10115672
- **Project number:** 5K99CA245194-02
- **Recipient organization:** MASSACHUSETTS GENERAL HOSPITAL
- **Principal Investigator:** Lei Shi
- **Activity code:** K99 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2021
- **Award amount:** $178,200
- **Award type:** 5
- **Project period:** 2020-03-01 → 2022-02-28

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10115672

## Citation

> US National Institutes of Health, RePORTER application 10115672, Exploiting metabolic reprogramming to target IDH1 mutated cholangiocarcinoma (5K99CA245194-02). Retrieved via AI Analytics 2026-05-25 from https://api.ai-analytics.org/grant/nih/10115672. Licensed CC0.

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