Searching Appalachia for Next Great Cancer Drug

Publication
Article
Oncology Live®Vol. 17/No. 21
Volume 17
Issue 21

In Partnership With:

The natural products produced by microbes found in the environment have led to major therapeutic breakthroughs for a variety of conditions ranging from infectious disease to cancer.

Jon Thorson, PhD

Associate Professor, University of Kentucky

Director, UK Center for Pharmaceutical Research and Innovation

Co-Director, UK Markey Cancer Center

Drug Discovery, Delivery and Translational Therapeutics Program

Microbial natural products, a key source of blockbuster drugs and new drug leads, are highly complex molecules, each evolved for specific function and fine-tuned to interact with and modulate an array of central cellular targets. Within this context, the natural products produced by microbes found in the environment have led to major therapeutic breakthroughs for a variety of conditions ranging from infectious disease to cancer. A key to reducing the rate of rediscovery, and thus improving the chances of finding new microbial natural products, is exploration in untapped or previously unexplored environments.

The University of Kentucky’s Natural Products Discovery Program, part of the UK College of Pharmacy’s Center for Pharmaceutical Research and Innovation (CPRI), is exploring untapped environments in our own back yard.

Appalachia, as one of the largest contiguous biodiversity “hot spots” in the nation, is expected to serve as fertile ground for the discovery of new microbes.

Specifically, Kentucky’s mines provide unprecedented access to biodiverse environments, particularly unique locations that may present access to unexplored terrain containing bacteria or microbes that have yet to be discovered. Subterranean environments represent the ocean beds of many centuries ago, where microbial spores have also been exposed to dramatic extremes in salinity, heavy metal exposure, temperature, and pressure.

Building Collaborations

In short, microbes from such unexplored environments are expected to be unprecedented and thereby present a greater chance for the discovery of new natural products.To access unique environments across the state, CPRI initially teamed up with the UK’s Center for Applied Energy Research. This connection helped establish additional collaborations with the Kentucky Division of Abandoned Mines, the Kentucky Geological Survey, and a number of mining operators across the commonwealth.

These cumulative relationships provide access to a wide array of unusual environments from the microbial natural products discovery perspective, including underground and surface coal mines, thermal vents from underground coal mine fires, mining reclamation sites, and deep-well core drilling operations.

Collaboration is also key to determining the function and therapeutic relevance of the natural products discovered. The pure natural products isolated as a result of UK’s program are cataloged and stored in CPRI’s Natural Products Repository as a unique resource.

Within this context, CPRI also works with UK investigators to develop and validate bioactivity assays relevant to their scientific or therapeutic areas of interest and subsequently employs these assays to screen the repository for compounds that display the desired activity. CPRI also has established strategic external collaborations, including with the National Cancer Institute (NCI).

Natural Product Discovery Process

This early collaborative work sets the stage for downstream studies. Should the compounds display sufficient activity with tolerable toxicity or perceived therapeutic index, potential preclinical development studies could be pursued.Once soil samples are collected, the CPRI team extracts bacteria and bacterial spores from a small amount of each soil sample and deposits portions of these extracts on media plates to begin the painstaking process of purifying and growing each individual strain of bacteria. Each recovered strain is phenotypically and genotypically characterized and then grown in liquid media to prepare extracts for metabolomic analysis. Strains are prioritized based on their potential for novel metabolite production with a bias toward bacteria genera/species underrepresented in natural products discovery.

High-priority strains are then grown on a large scale from which all accessible metabolites are purified via a range of selective extractions and chromatographic techniques, and then fully characterized structurally using mass spectrometry, nuclear magnetic resonance, and other spectrophotometric methods.

Samples are cataloged and deposited in the CPRI Natural Products Repository where each natural product is given a “CN” designator (eg, CN200) to ensure downstream bioactivity assays are completely unbiased and conducted in a blinded environment.

Deliverables and Discoveries

It can take up to 6 months or more from soil collection to compound deposition in part due to the inherent slow growth of high-priority strains. In addition to expanding the repository, CPRI staff also must continually replenish materials and conduct periodic quality assurance analysis to sustain a high-quality library of natural products.CPRI’s proprietary repository currently contains 758 distinct microbial strains isolated from Kentucky environments and 236 pure, fully characterized microbial natural products (64% of which are exclusive to the UK collection).

Not surprisingly, chemoinformatic analysis of the repository reveals that the chemical diversity and structural complexity far surpass that represented in commercial compound libraries used for typical high-throughput drug discovery screening.

Markey’s Qing-Bai She, PhD, was one of the first investigators to utilize the repository for screening. Dr She is interested in the pathways that contribute to, and the impact of, 4E-BP1 phosphorylation. 4E-BP1 is a repressor of cap-dependent translation. However, in many cancers, the oncogenic actions of aberrant signaling pathways lead to hyperphosphorylation of 4E-BP1. This, in turn, relieves 4E-BP1 inhibitory control on eIF4Einitiated cap-dependent translation of oncogenic mRNAs and thereby drives oncoprotein production.

Screening the repository revealed a class of natural products that selectively inhibit 4E-BP1 phosphorylation in a mechanistically unique manner. Inspired by this discovery, CPRI scientists developed improved analogs that are well tolerated and inhibit tumor growth in standard mouse tumor xenografts.

Moving Forward

These preliminary data also provided the basis for a recent 5-year, $2.5 million grant from the NCI to support molecular target identification, mechanistic studies, and lead optimization efforts.The pendulum is swinging back toward increased biotech and pharma interest in natural product— based assets. Thus, UK’s program is well positioned to take advantage of this momentum. Early results from other screening campaigns using the CPRI Natural Products Repository also suggest a high probability of additional compelling lead discovery/development programs such as the one exemplified by Dr She’s 4E-BP1 project.

Although such initiatives are often highly competitive for extramural funding for advancing compelling “hits,” such grants do not support the fundamental infrastructure. Looking forward, a key challenge will be to develop a mechanism for the sustainability and growth of this valuable new resource.

Related Videos
Aman Chauhan, MD, of the University of Kentucky
Reema A. Patel, MD, of University of Kentucky
Michael J. Cavnar, MD, discusses the use of hepatic artery infusion pumps in patients with colorectal cancer with liver metastases.
Joseph Kim, MD
Reema A. Patel, MD
Michael J. Cavnar, MD
Prakash Pandalai, MD
Prakash Pandalai, MD, ​discusses the use of cytoreductive surgery plus heated intraperitoneal chemotherapy in the treatment of patients with colorectal peritoneal carcinomatosis.
Joseph Kim, MD, discusses the multidisciplinary management of hepatocellular carcinoma.
Joseph Kim, MD, of University of Kentucky Markey Cancer Center