Past and future of trypanosomatids high-throughput phenotypic screening

Dantas, Rafael Ferreira; Torres-Santos, Eduardo Caio; Silva Jr, Floriano Paes

doi:10.1590/0074-02760210402

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PERSPECTIVE • Mem. Inst. Oswaldo Cruz 117 • 2022 • https://doi.org/10.1590/0074-02760210402 copy

Past and future of trypanosomatids high-throughput phenotypic screening

Authorship SCIMAGO INSTITUTIONS RANKINGS

Diseases caused by trypanosomatid parasites affect millions of people mainly living in developing countries. Novel drugs are highly needed since there are no vaccines and available treatment has several limitations, such as resistance, low efficacy, and high toxicity. The drug discovery process is often analogous to finding a needle in the haystack. In the last decades a so-called rational drug design paradigm, heavily dependent on computational approaches, has promised to deliver new drugs in a more cost-effective way. Paradoxically however, the mainstay of these computational methods is data-driven, meaning they need activity data for new compounds to be generated and available in databases. Therefore, high-throughput screening (HTS) of compounds still is a much-needed exercise in drug discovery to fuel other rational approaches. In trypanosomatids, due to the scarcity of validated molecular targets and biological complexity of these parasites, phenotypic screening has become an essential tool for the discovery of new bioactive compounds. In this article we discuss the perspectives of phenotypic HTS for trypanosomatid drug discovery with emphasis on the role of image-based, high-content methods. We also propose an ideal cascade of assays for the identification of new drug candidates for clinical development using leishmaniasis as an example.

Key words:
trypanosomatids; phenotypic; high-content screening; bioimaging; drug discovery

Instituto Oswaldo Cruz, Ministério da Saúde Av. Brasil, 4365 - Pavilhão Mourisco, Manguinhos, 21040-900 Rio de Janeiro RJ Brazil, Tel.: (55 21) 2562-1222, Fax: (55 21) 2562 1220 - Rio de Janeiro - RJ - Brazil
E-mail: memorias@fiocruz.br

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[1] + Corresponding author: floriano@ioc.fiocruz.br

Genus	Species	Strains	Evolutionary forms	Reporter	Host cell	Main measurements	Assay principle	Screened compounds	Pipeline step	References
Trypanosoma	T. brucei brucei (wild type and genetically engineered kDNA-independent cell line)¹⁰¹101. Dean S, Gould MK, Dewar CE, Schnaufer AC. Single point mutations in ATP synthase compensate for mitochondrial genome loss in trypanosomes. Proc Natl Acad Sci USA. 2013; 110(36): 14741-6.	Laboratory strain: Lister 427	Bloodstream	None	-	kDNA/nucleus ratio	Parasite nuclear DNA and kDNA detected by Hoescht 33342 while viable parasites by CFDA-SE	13,486 compounds from three commercial libraries (Prestwick Chemical Library, Screen-Well PKE library and BioAscent 12,000 diverse chemical libraries)	Primary screening	⁽⁸⁰⁾
	T. cruzi	Laboratory strain: Y	Intracellular amastigotes	None	Human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CM)	Number of host cells (lethal cytotoxicity evaluation), number of amastigotes per cell, infection ratio and sublethal cytotoxicity-related parameters	Screening: Parasites DNA spots and cell nucleus detected by Draq5 while cell cytoplasm by cTNT immunostaining; Cytotoxicity assay: Cell nucleus, cytoskeleton and mitochondria detected by DAPI, Phalloidin-488 and MitoTracker^TM Red, respectively	4 compounds with known anti-trypanosomatid activity	Primary screening (dose-response) and cytotoxicity assay	⁽⁷¹⁾
		Laboratory strain: Tulahuen	Intracellular amastigotes	Escherichia coli beta-galactosidase gene⁽⁴⁴⁾	Rat cardiomyocytes (H9c2)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and percentage of infected cells per well	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	20 compounds with known anti-trypanosomatid activity	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay	⁽⁶⁹⁾
		Laboratory strain: Tulahuen	Intracellular amastigotes	None	Mouse embryo fibroblast (3T3)	Number of amastigotes per cell and number of infected cells per well	Parasites DNA spots and cell nucleus detected with Hoescht 33342 while cell cytoplasm with HCS CellMask Green^TM	741 compounds (FDA-approved and with biological activity) from a in-house library and 685 compounds from a pilot collection of Medicines for Malaria Venture Malaria Box	Primary screening and dose-response assay	⁽⁷⁹⁾
		Laboratory strain: Tulahuen	Intracellular amastigotes	None	Mouse embryo fibroblast (3T3)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and number of infected cells per well	Parasites DNA spots and cell nucleus detected with Hoescht 33342 while cell cytoplasm with HCS CellMask Green^TM	24,993 compounds optimised for lead-like properties	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves and for further profiling of selectively active compounds. Protocol based on a previous report⁽⁷⁹⁾. A wash-off assay was also carried out by HCS.	⁽⁷²⁾
Trypanosoma		Laboratory strains: Silvio X10/7 subclone A1, Y, M6241 Clone 6, ERA Clone 2, PAH179 Clone 5, Tula Clone 2 and CL Brener.	Trypomastigotes and intracellular amastigotes	CL Brener strain carrying a gene reporter (red-shifted luciferase¹⁰²102. Lewis MD, Fortes FA, Taylor MC, Burrell-Saward H, McLatchie AP, Miles MA, et al. Bioluminescence imaging of chronic Trypanosoma cruzi infections reveals tissue-specific parasite dynamics and heart disease in the absence of locally persistent infection. Cell Microbiol. 2014; 16(9): 1285-300.)	Cercopithecus aethiops kidney cell (Vero)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell, number of amastigotes per well, percentage of infected cells and percentage of EdU (nucleoside analog) positive cells and parasites	Primary screeninging and replication assay (amastigotes): parasites DNA spots as well as cell nucleus and cytoplasm detected by Hoechst 33342; Proliferation assay : EdU incorporation by parasites (trypomastigotes and amastigotes) and cell nucleus detected by Click-iT Plus EdU Alexa- Fluor 488 Imaging Kit. Trypomastigote flagellum was also detected by immunostaining (anti-PFR1 antibody)	3 trypanocidal drugs	Primary screening (dose-response) and cytotoxic evaluation performed in the same assay. Replication and proliferation assays were also carried out using a HCS system. Protocol based on a previous report⁽⁹⁴⁾.	⁽⁷³⁾
		Not declared	Intracellular amastigotes	None	Human osteosarcoma cells (U2OS)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	2 trypanocidal drugs	Primary screening (dose-response) and cytotoxicity evaluation in the same assay	⁽¹⁰⁰⁾
		Laboratory strains: Dm28c, Y, ARMA13 cl1, ERA cl2, 92-80 cl2, CL Brener and Tulahuen	Intracellular amastigotes	None	Human osteosarcoma cells (U2OS)	Number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	8 lead/clinical compounds with anti-trypanosomatid activity	Primary screening (dose-response) and time-kill assay. Protocols based on a previous report⁽¹⁰⁰⁾.	⁽⁷⁰⁾
		Laboratory strain: Y	Intracellular amastigotes	None	Human osteosarcoma cells (U2OS)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	39 commercial compounds selected from a virtual screening of the ChemBridge chemical database (1 M compounds)	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay. Protocol based on a previous report⁽⁷⁰⁾.	⁽⁸¹⁾
		Laboratory strains: Y-H10, Sylvio X10/1 and CL Brener	Intracellular amastigotes	None	Human osteosarcoma cells (U2OS), human acute monocytic leukemia (THP-1) cells, Cercopithecus aethiops kidney cell (Vero) and rat skeletal myoblast (L6) cells	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cells nucleus and cytoplasm detected by Draq5	1,280 compounds from LOPAC library (Sigma-Aldrich)	Primary screening and cytotoxicity evaluation performed in the same assay using Y-H10 strain. Similar method was employed to dose-response curves. Protocol based on a previous report ⁽⁹³⁾	⁽²⁷⁾
		Laboratory strains: Y	Intracellular amastigotes	None	Human osteosarcoma cells (U2OS)	Number of host cells (cytotoxicity evaluation) and infection ratio	Parasites DNA spots as well as cells nucleus and cytoplasm detected by Draq5	24 novel compounds derived from farnesyltransferase inhibitors	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay . Protocol based on a previous report⁽⁷⁰⁾),	⁽⁹³⁾
		Laboratory strains: Y	Intracellular amastigotes	None	Murine fibroblasts (NIH 3T3) expressing GFP	Number of amastigotes per cell and percentage of infected cells	Parasites DNA spots and cells nucleus detected by DAPI while cell body detected by GFP	21 treatment groups from an on-going study	Primary screening	⁽²⁵⁾
Trypanosoma		Laboratory strain: CA-I/72	Intracellular amastigotes	None	Mouse myoblasts (C2C12)	Number of host cells (cytotoxicity evaluation) and infection level (number of amastigotes per cell as determined by nuclei counting)	Parasites DNA spots and cells nucleus detected by DAPI	7,680 compounds from ReFRAME library	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocol based on previous reports^(86,87,100)	⁽⁸⁵⁾
		Laboratory strains: CA-I/72	Intracellular amastigotes	None	Mouse myoblasts (C2C12)	Number of host cells (cytotoxicity evaluation) and infection level (number of amastigotes per cell)	Parasites DNA spots and cells nucleus detected by DAPI	Gallinamide A and 15 analogs	Primary screening (dose-response) and cytotoxic evaluation performed in the same assay. Protocol based on a previous report⁽⁸⁷⁾	⁽⁸⁶⁾
		Laboratory strain: CA-I/72	Intracellular amastigotes	None	Mouse myoblasts (C2C12)	Number of host cells (cytotoxicity evaluation) and infection ratio	Parasites DNA spots and cell nucleus detected by DAPI	97 commercial compounds selected by virtual screening	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves	⁽⁸⁷⁾
		Laboratory strain: Silvio X10/7 A1	Intracellular amastigotes	None	Cercopithecus aethiops kidney cells (Vero)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and percentage of infected cells	Parasites DNA spots as well as cells nucleus and cytoplasm detected by Hoechst 33342	14,080 commercial compounds from NIH (clinical collection) and Selleck-Chem (FDA-approved drug library) libraries	Primary screening and cytotoxicity evaluation performed in the same assay. Similar methods were used to dose-response, cell replication, static-cidal and rate-of-kill assays. Protocols based on previous reports^{(25,53,69,89)}.	⁽⁹⁴⁾
		Laboratory strains: CA-I/72, PSD-1 and Sylvio X10/7	Intracellular amastigotes	None	Bovine embryo skeletal muscle (BESM) and human hepatoma (Huh-7) cells	Number of host cells (cytotoxicity evaluation) and kDNA/host nuclei ratio	Parasites kDNA and cell nucleus detected by DAPI	909 clinical compounds library from Iconix Biosciences	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves	⁽⁸⁹⁾
		Laboratory strain: CA-I/72	Intracellular amastigotes	None	Mouse myoblasts (C2C12)	Number of host cells (cytotoxicity evaluation), infection ratio and area of infection (area of kinetoplastids/total nuclei)	Parasites DNA spots and cell nucleus detected by DAPI, cell body inferred by aggregating parasites DNA spots and cell nucleus image objects	180,329 compounds from GNF Academic Collaboration Library	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocols based on a previous report⁽⁸⁹⁾	⁽⁸⁸⁾
		Laboratory strain: Tulahuen	Intracellular amastigotes	Escherichia coli β-galactosidase gene⁽⁴⁴⁾	Rat cardiomyocytes (H9c2)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	2,310 compounds from GlaxoSmithKline HTS screening collection	Orthogonal assay (screening and cytotoxicity evaluation). Protocol based on a previous report⁽⁶⁹⁾	⁽⁶⁰⁾
		Laboratory strain: STIB980 clone 1	Intracellular amastigotes	eGFP	Peritoneal mouse macrophages	Number of host cells (cytotoxic evaluation), number of amastigotes per image and fold change in parasite numbers per hour	Parasite kDNA and cell nucleus detected by Hoechst 33342. Parasites also identified by GFP staining in live imaging assay	2 anti-trypanosomatid drugs	Secondary assay (dose-response and cytotoxicity evaluation)	⁽⁹⁷⁾
Trypanosoma		Laboratory strain: Tulahuen	Intracellular amastigotes	Escherichia coli β-galactosidase gene⁽⁴⁴⁾	Rat cardiomyocytes (H9c2)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	3,598 compounds from Calibr Diversity Library	Secondary assay (screening and cytotoxicity evaluation) and dose-response assay. Protocol based on previous reports^(60,69)	⁽⁸⁴⁾
		Laboratory strain: Talahuen	Intracellular amastigotes	GFP¹⁰³103. Ferreira BL, Orikaza CM, Cordero EM, Mortara RA. Trypanosoma cruzi: single cell live imaging inside infected tissues. Cell Microbiol. 2016; 18(6): 779-83.	Monkey kidney epithelial (LLCMK2) cells	Number of intracellular amastigotes per well	Cells nucleus detected by DAPI and amastigotes by GFP staining	4 phenothiazinium dyes	Primary screening (dose-response)	¹⁰⁴104. Portapilla GB, Pereira LM, da Costa CMB, Providello MV, Oliveira PAS, Goulart A, et al. Phenothiazinium dyes are active against Trypanosoma cruzi in vitro. Biomed Res Int. 2019; 2019: 8301569.
		Laboratory strain Tulahuen	Intracellular amastigotes	None	Mouse embryo fibroblasts (3T3)	Number of amastigotes per cell and number of infected host cells per well	Parasites DNA spots and cell nucleus detected by Hoescht 33342 while cell cytoplasm by HCS CellMask Green™	472 compounds from Davis open access natural product-based library	Primary screening and dose-response assay. Protocol based on a previous report⁽⁷⁹⁾)	⁽⁹⁸⁾
Leishmania	L. donovani, L. amazonensis and L. braziliensis	Laboratory strains: L. donovani (MHOM/IN/1980/DD8), L. amazonensis (MHOM/BR/1977/LTB0016) and L. braziliensis (MHOM/BR/1975/M2903)	Intracellular amastigotes	None	Human acute monocytic leukemia (THP-1) cells	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	1,280 compounds from LOPAC library	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocol based on a previous report⁽⁸²⁾	⁽⁸³⁾
	L. donovani	Laboratory strain: MHOM/SD/62/1SCL2D, LdBOB	Intracellular amastigotes	GFP⁽⁵³⁾	Human acute monocytic leukemia cells (THP-1)	Number of amastigotes per cell, infection ratio and number of parasites labeled with EdU	Cell nucleus and cytoplasm detected by DAPI while amastigotes by GFP staining. In the proliferation assay the incorporation of EdU in newly synthetized DNA was measured using Click-iT^TM Plus Alexa Fluor^TM 647 Picolyl Azide Toolkit	2 antileishmanial drugs	Primary screening (dose-response) and proliferation assay. Protocol based on previous reports^(53,60))	⁽⁷⁴⁾
	L. donovani	Laboratory strain: MHOM/SD/62/1S-cl2D	Intracellular amastigotes	None	Human acute monocytic leukemia (THP-1) cells	Number of host cells (cytotoxicity evaluation) and number of amastigotes per cell	Parasites kDNA and cell nucleus detected by DAPI. Cell boundary was delineated around the nucleus object.	909 bioactive compounds library from Iconix Biosciences	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves	⁽⁹⁶⁾
	L. donovani, L. amazonensis, L. braziliensis, L. major	Laboratory strains: L. donovani (MHOM/ET/67/HU3), L. amazonensis (MHOM/BR/73/M2269), L. braziliensis (MHOM/BR/ 2903) and L. major (MHOM/IL/81/FRIEDLIN)	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots and cell nucleus detected by Draq5. Individual cells were segmented after a series of computational tasks that use the nucleus as a seed point	4 antileishmanial drugs	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay	⁽⁸²⁾
Leishmania	L. donovani and L. major	Laboratory strains: L. donovani (MHOM/ ET/67/HU3 ) and L. major (MHOM/IL/81/FRIEDLIN)	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	124 compounds from TimTec library	Hit confirmation assay (dose-response)	⁽⁶⁸⁾
	L. donovani	Laboratory strain: MHOM/SD/62/1S-CL2D (LdBOB)	Intracellular amastigotes	Aequorea victoria eGFP	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and number of infected cells	Cell nucleus and body detected by DAPI and HCS Cellmask^TM Deep Red, respectively. Parasites detected by GFP staining	15,659 diverse compounds library	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves	⁽⁵³⁾
	LRV1-containing L. guyanensis	Laboratory strain: MHOM/ BR/75/M4147	Intracellular amastigotes	None	Primary murine bone-marrow derived macrophages	Number of host cells (cytotoxicity evaluation) and number of amastigotes per cell	Parasites DNA spots and cells nucleus detected by DAPI while cell cytoskeleton (cytosol) by phalloidin-Alexa488	1,520 compounds from Prestwick Chemical Library	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocol based on a previous report⁽⁷⁶⁾	⁽⁵⁷⁾
	L. infantum and L. amazonensis	Laboratory strains: L. infantum (MHOM/MA/67/ITMAP-263) and L. amazonensis (MHOM/ BR/LTB0016)	Intracellular amastigotes	None	Primary murine bone-marrow derived macrophages	Number of amastigotes per cell and percentage of infected cells	Parasites DNA spots and cells nucleus detected by DAPI while cell body by CellMask^TM Deep Red	1 antileishmanial drug	Primary screening (dose-response). Protocol based on previous reports^{(53,57,82,96)}	⁽⁵⁸⁾
	L. donovani and L. amazonensis	Laboratory strains: L. donovani (MHOM/SD/62/1S-CL2D) and L. amazonensis (MPRO/BR/1972/M1841)	Intracellular amastigotes	mCherry (L. amazonensis)	Primary murine bone-marrow derived macrophages	L. donovani: Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and percentage of infected cells; L. amazonensis: Number of amastigotes, number of total host cells (TM, nucleus counting), number of healthy host cells (HM, based on nucleus size and intensity features), number of parasitophorous vacuoles (PV), viability index (HM/TM) and PV/HM ratio	L. donovani assay: parasites DNA spots and cell nucleus detected by Hoescht 33342 while cell body by HCS CellMask^TM Blue. Parasites detected by immunostaining using hamster (infected with L. donovani) immune serum and secondary antibody anti-hamster conjugated with Alexa Fluor 488; L. amazonensis assay: cell nucleus, parasitophorous vacuoles and parasites detected by Hoescht 33342, LysoTracker Green DND-26 and mCherry staining, respectively	188 compounds from Leish-Box	Primary screening and cytotoxicity evaluation performed in the same assay (L.donovani and L. amazonensis). A similar method was used to generate the dose-response curves (L. donovani). Protocol based on a previous report⁽⁷⁶⁾	⁽⁷⁵⁾
Leishmania	L. major, L. donovani and L. infantum	Laboratory strains: L. major (MHOM/SU/73/5ASKH), L. donovani (BPK190), L. infantum (MHOM /FR/91/LEM 2259, belonging to zymodeme MON-1 clone 3511) and L. braziliensis (MHOM/PE/01/PER005 cl.2)	Intracellular amastigotes	None	Primary murine bone-marrow derived macrophages	Number of host cells (cytotoxicity evaluation), number of amastigotes per well, number of amastigotes per cell and infection ratio	Cell nucleus detected by DAPI while cell cytoplasm and parasites detected by immunostaining using mouse anti-Hsp9 primary antibody and anti-mouse secondary antibody conjugated with Alexa Fluor 647	6 immunostimulatory EhPIb-compounds	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay	⁽⁷⁷⁾
	L. amazonensis	LV79 (MPRO/BR/1972/M1841)	Intracellular amastigotes	DsRed2¹⁰⁵105. Lecoeur H, de La Llave E, Osorio Y Fortéa J, Goyard S, Kiefer-Biasizzo H, Balazuc A-M, et al. Sorting of Leishmania-bearing dendritic cells reveals subtle parasite-induced modulation of host-cell gene expression. Microbes Infect. 2010; 12(1): 46-54.	Primary murine bone-marrow derived macrophages	Number of amastigotes, number of total host cells (TM, nucleus counting), number of healthy host cells (HM, based on nucleus size and intensity features), number of parasitophorous vacuoles (PV), viability index (HM/TM) and PV/HM ratio	Cell nucleus, parasitophorous vacuoles and parasites detected by Hoescht 33342, LysoTracker Green DND-26 and DsRed2 staining, respectively	60 compounds with established or potential leishmanicidal, antifungal or antimicrobial and cytotoxic activities	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves	⁽⁷⁶⁾
	L. mexicana	MNYC/BZ/62/ M379	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), average number of amastigotes per cell and frequency distribution of intracellular amastigotes	Parasites detected by CellTracker^TM Orange CMRA while cell body and nucleus detected by CellTracker^TM Green CMFDA and DAPI, respectively	3 antileishmanial drugs	Primary screening (dose-response) and cytotoxicity evaluation performed in the same assay	⁽⁷⁸⁾
	L. donovani	Recent clinical isolates sensitive and resistant to pentavalent antimonials (SSG):SSG-sensitive (MHOM/NP/03/BPK282/0 clone 4) and SSG-resistant (MHOM/NP/03/BPK275/0 clone 18)	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cells nucleus and cytoplasm detected by Draq5	130 compounds from Leish-box (GSK)	Primary screening (dose-response). Protocol based on previous reports^(53,60)	⁽⁶⁷⁾
	L. donovani	Laboratory strain: MHOM/SD/62/1S-CL2D	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Parasites DNA spots as well as cell nucleus and cytoplasm detected by Draq5	1,742 bioactive compounds from MedChem Express	Primary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocol based on a previous report⁽⁸²⁾	⁽⁹⁵⁾
	L. donovani	Laboratory strain: MHOM/SD/62/1S-CL2D, LdBOB	Intracellular amastigotes	Aequorea victoria eGFP	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Cell nucleus and cytoplasm detected by DAPI while parasites by GFP staining	32,200 compounds from GlaxoSmithKline HTS screening collection	Secondary screening and dose-response assay (also cytotoxicity evaluation). Protocol based on previous reports^(53,76)	⁽⁶⁰⁾
Leishmania	L. donovani	Laboratory strain: MHOM/SD/62/1S-CL2D, LdBOB	Intracellular amastigotes	Aequorea victoria eGFP	Human acute monocytic leukemia cells (THP-1)	Number of host cells (cytotoxicity evaluation), number of amastigotes per cell and infection ratio	Cell nucleus and cytoplasm detected by DAPI while parasites by GFP staining	1,392 compounds from Diversity Library from Calibr	Secondary screening and cytotoxicity evaluation performed in the same assay. A similar method was used to generate the dose-response curves. Protocol based on previous reports^(60,74))	⁽⁸⁴⁾
	L. donovani	Laboratory strain: MHOM/IN/80 DD8	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of amastigotes per cell and number of infected cells normalized to the positive and negative controls	Parasites DNA spots detected by SYBR green while cell body and nucleus by CellMask^TM Deep Red and SYBR green, respectively	472 natural product-derived library from Davis open access	Primary screening and dose-response assay. Protocol based on a previous report⁽⁹⁹⁾	⁽⁹⁸⁾
	L. donovani	Laboratory strain: MHOM/IN/80 DD8	Intracellular amastigotes	None	Human acute monocytic leukemia cells (THP-1)	Number of amastigotes per cell and number of infected cells normalized to the positive and negative controls	Parasites DNA spots detected by SYBR green while cell body and nucleus by CellMask^TM Deep Red and SYBR green, respectively	400 compounds from Medicines for Malaria Venture Pathogen Box	Primary screening and dose-response assay	⁽⁹⁹⁾