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Thavy Long

Thavy Long

Assistant Professor

T: 514-398-7541 | thavy.long [at] mcgill.ca (Email) | Parasitology Building, P-211

Degrees

BSc, MSc, University of Lille 1 - France
PhD, University of Lille 2 - France

Short Bio

Dr. Thavy Long obtained her MSc thesis in Genetic and Microbiology and PhD in Cell Biology from University of Lille (France). It was during her PhD with Dr Colette Dissous that she really developed an interest in the molecular and cellular biology of helminths and particularly of Schistosoma mansoni, a parasitic flatworm of humans. Her past project involved studies on protein kinases that regulate the development of reproductive organs and egg production in S. mansoni. She has also led numerous drug discovery and development projects against schistosomes during her postdoc-trainings with Dr. Conor Caffrey and Dr. James McKerrow at UC San Francisco and UC San Diego. Recently, she gained expertise on the biology of filarial parasites including the heartworm Dirofilaria immitis that infects companion animals by investigating the signaling pathways that govern the development of the infective stage. As an Assistant Professor at the Institute of Parasitology, Dr Long is interested in understanding the molecular mechanisms involved in immune evasion, developmental processes and metabolism of helminths including trematodes and filarial nematodes, to identify novel targets that could be the basis for new anthelminthics. In addition, her research focuses on developing tools to monitor the spread of drug resistance and elucidating the mechanisms of drug resistance in helminth parasites.

Awards and Recognitions

Prestige Marie Curie Fellowship - Postdoctoral Fellowship

Research Interests

Professor Long's research focuses on the molecular basis underlying the intracellular communication in schistosomes as well as the dialogue between schistosomes and their host. In her laboratory, they aim to identify schistosome molecular actors that are involved in this process as well as their associated receptors in the parasite and/or the host which could be the basis for the development of novel therapies against schistosomiasis.

Current Research

Helminths are parasitic worms of medical and veterinary importance. They infect billions of individuals worldwide and are responsible for chronic diseases in livestock and companion animals leading to significant economic losses. Treatment and control of helminthiasis are limited and mostly rely on a few anthelminthics (AHs) for which mass drug administration has already led to drug resistance in nematodes, and threats to extend to trematodes. No recombinant vaccines are available. Alternative treatment strategies are urgently needed. In this context, understanding the worm biology and the strategies employed by those parasites to thrive in hostile environment or under drug pressure is crucial to the identification of novel gene/protein targets for drug or vaccine development. Moreover, epidemiological studies around the world reported an inverse relationship between the prevalence of inflammatory diseases (ID) and helminth infections, leading to the 鈥渉ygiene hypothesis鈥 and suggesting the potential protection of helminths against ID, via host immune system regulation.

Schistosomes can establish long-term chronic infections as they can survive for up to 40 years in their human host. Clearly, these parasites have evolved to evade or manipulate the host immune system by creating an immunoregulatory environment. The mechanisms by which schistosomes interact with its mammalian host and alter the host immune response remain unknown. Like all helminths, schistosomes release excretory-secretory products (ESPs) which are at the heart of molecular dialogues in host-parasite interactions (HPI). Helminth extracellular vesicles (EVs) are components of ESPs and recently emerge as key players in cell-to-cell communication and in regulating the immune response. However, their specific role in the infection process and pathology of S. mansoni is not well understood.

Another interesting aspect of helminths is their reliance on the host cholesterol and sterol derivatives as helminths are incapable of synthesizing sterols de novo which emphasizes how intricate is the parasite-host interplay. How helminths acquire sterols and whether they metabolize them are unknown. Derivatives of cholesterol such as steroid hormones or bile acids exercise their function via the binding to nuclear receptors (NRs) that work in concert with other proteins to regulate the expression of specific genes controlling development, homeostasis, reproduction and metabolism. In schistosomes, steroid hormones have been shown to impact their physiology and NRs have been structurally characterized but their function are still unknown, and no apparent hormone-receptor complex has been described so far.

Resistance to current anthelminthics such as macrocyclic lactones (ML) is a significant problem worldwide threatening the health of individuals and animals. The mechanisms of resistance to ML are not completely understood. Moreover, monitoring the spread of drug resistance is challenging in absence of adequate tools. Understanding how helminths survive to drug pressure could lead to new treatment options that could also potentiate current AHs.

Dr Long鈥檚 laboratory is interested in:

  • Identifying the schistosome- and heartworm-derived molecules with immunomodulation and therapeutic potential
  • Deciphering the genetic and molecular basis by which steroid hormones affect the development in trematodes and filarial parasites
  • Investigating the role of steroid hormones in the phenotypic plasticity of S. mansoni and particularly in the adaptation to a parasitic lifestyle
  • Unravelling the mechanisms developed by the parasite to exploit cholesterol from the host
  • Unravelling strategies employed by the parasite to survive to drug pressure
  • Developing novel tools to understand and monitor drug resistance in helminths

Courses

LSCI 211. Biochemistry 1.

Credits: 3
Offered by: Parasitology (Faculty of Agric Environ Sci)
Terms offered: Fall 2025, Winter 2026
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Description

Biochemistry of carbohydrates, lipids, proteins, nucleic acids; enzymes and coenzymes. Introduction to intermediary metabolism.
  • Co-requisite: FDSC 230
  • Restriction: Not open to students who have taken FDSC 211

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BTEC 619. Biotechnology Laboratory 2.

Credits: 4
Offered by: Parasitology (Graduate Studies)
Terms offered: Winter 2026
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Description

A laboratory-based course in a variety of topics including: proteomics, protein expression and purification, conventional and HPLC chromatography, protein-protein interactions, ELISA, and Western blot analysis and hybridoma techniques.
  • Prerequisite: BTEC 620 or permission of the instructor.
  • The fee of $598.39 is used to support the cost of chemical reagents, kits, disposables and minor equipment necessary to run this hands-on laboratory course.

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PARA 606. Parasitology Seminar.

Credits: 2
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

A seminar series in which students present seminars covering topics in parasitology, in areas relevant to their research interests. Students register for the course in their second term of residency. Attendance and participation are compulsory for M.Sc. students.

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PARA 607. Parasitology Research Seminar.

Credits: 2
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

This is a required course for M.Sc. students. A seminar course in which students registered at the Institute of Parasitology present seminars on the results of their thesis research. Students register for the course in the final term prior to thesis submission.

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PARA 687. Thesis Research 1.

Credits: 11
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

Independent research work under the direction of the Thesis Supervisor.

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PARA 688. Thesis Research 2.

Credits: 11
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

Independent research work under the direction of the Thesis Supervisor.

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PARA 689. Thesis Research 3.

Credits: 13
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

Independent research work under the direction of the Thesis Supervisor.

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PARA 710. Parasitology Ph.D. Seminar 1.

Credits: 2
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

This first seminar is a review of the scientific literature in the topic area of the thesis research.

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PARA 711. Parasitology Ph.D. Seminar 2.

Credits: 2
Offered by: Parasitology (Graduate Studies)
Terms offered: Fall 2025, Winter 2026
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Description

A seminar series in which students present seminars covering topics in parasitology in areas relevant to their research interests. Attendance and participation are compulsory.

Most students use Visual Schedule Builder (VSB) to organize their schedules. VSB helps you plan class schedules, travel time, and more.


PARA 701. PhD Comprehensive Exam.

Credits: 0
Offered by: Parasitology (Graduate Studies)
Terms offered: Summer 2025, Fall 2025, Winter 2026
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Description

Consists of a written proposal outlining the research planned and an oral examination.

Most students use Visual Schedule Builder (VSB) to organize their schedules. VSB helps you plan class schedules, travel time, and more.

Publications

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