A D V E R T I S E M E N T F E A T U R E

A D V E R T I S E R R E TA I N S S O L E R E S P O N S I B I L I T Y F O R C O N T E N T

Kaleido Bioscienceswww.kaleido.com

Small molecules harnessing the gut microbiomeMaximizing the potential of the resident gut microbiome, Kaleido Biosciences is developing novel glycans with the abilityto change the metabolic output of the microbiome and have a clinically significant impact across a broad range of diseases.

Science on the human microbiome represents oneof the most exciting areas of innovation. A broadand rapidly growing body of research has revealedthat humans live in intimate association with thevast and diverse microbial communities of the gut.These microorganisms are not just passengers, butactively take part in a complex network of molecularinteractions with the host, which directly impactsthe maintenance of health as well as the onset andprogression of diseases.

These insights have fueled an increase in invest-ment in microbiome therapeutic development.Most aim at selectively adding or subtracting bacte-ria to correct microbiomes. These first microbiometherapies have recently seen notable success inClostridium difficile infection; however, challengesremain as to the choice of strains, utility across indi-cations, and product complexity and manufacturing.

Kaleido Biosciences, a clinical-stage health-carecompany, is taking a differentiated therapeuticapproach by developing small molecules thatselectively restore the composition and metabolicoutput of damaged resident microbiomes. Thisunique modality, consisting of synthetic glycansand a proprietary development platform, enablesdrug discovery research and clinical translation atunprecedented speed.

Inspired by natureGut microorganisms are genetically and function-ally differentiated by their ability to utilize specificstructurally distinct glycans (polysaccharides).Kaleido capitalizes on this principle to synthesizenovel, structurally diverse glycan ensembles,Microbiome Metabolic Therapies (MMTs) thatare selectively utilized by specific microorganismsor by broader microbial populations that havethe receptive genetic make-up. The diversity ofstructure and microbiome-modulating activity ofMMTs is achieved by controlling their building blockcomposition, linkage distribution and size (Fig. 1).

“Recent clinical advancements have providedgreater confidence that microbiome-basedapproaches can be translated into clinically vali-dated therapies. Given that our tailored MMTs acton specific metabolic pathways that occur acrossspecies, we have demonstrated that we can drivethe microbiome towards a desired compositionand activity, in a targeted and optimized mannerand across diverse diseases,” explained Johan vanHylckama Vlieg, Kaleido’s CSO.

Platform for rapid advancementUsing its synthetic glycan chemistry, Kaleidohas created a library containing more than 1,500MMTs that have a unique ability to re-engineer the

composition of existing microbiomes and promotethe production of specific metabolites, makingthem potent polypharmacological therapeuticcandidates. Furthermore, they can be producedon easily scalable small-molecule manufacturingplatforms and can move rapidly to clinical studies.

The effect of MMTs is first tested ex vivo usinga highly multiplexed advanced screening platformwith microbiome communities from both healthyand patient populations. To establish how MMTsimpact therapeutically relevant pathways, a broadrange of bioanalytical technologies are used toanalyze metabolites, effector molecules and hostresponses, while sequencing determines key micro-bial population changes.

A candidate MMT may then either undergo fur-ther testing in animal models or go straight intoclinical evaluation in humans. Abbreviated devel-opment may be possible in some cases becauseMMTs are synthesized from naturally occurringcarbohydrate monomers, are orally administeredwith limited systemic exposure and can be desig-nated as Generally Recognized as Safe (GRAS).

“Our model has the potential to be faster andmore cost efficient than traditional discovery anddevelopment,” according to Katharine Knobil,Kaleido’s CMO and head of R&D. It took just twoyears from conducting the first ex vivo screeningof Kaleido’s lead candidate for urea cycle disorders(UCD) to starting phase 2 trials, she pointed out.

Broad pipelineResearch initially focused on diseases targeting asingle metabolite, such as ammonia reduction inUCD (KB195) and hepatic encephalopathy (KB174).The portfolio has since expanded to encompassmultiple mechanisms on which MMTs can act, andKaleido is now advancing a pipeline of candidates

promoting immune homeostasis. Ongoing clinicalprograms include trials in ulcerative colitis (KB295)and in patients with mild-to-moderate COVID-19(KB109). Furthermore, expected delivery of multipleclinical-ready candidates in 2021 from preclinicalprograms include MMTs that reduce trimethyl-amine and inflammatory markers in metabolicconditions, and immune-potentiating MMTs foruse in immuno-oncology.

“There is a strong correlation between micro-biome profiles and successful treatment withcheckpoint inhibitors,” explained Knobil. “Weare currently assessing MMTs that can alter themicrobiome with the goal of helping more peoplerespond to checkpoint inhibitor therapy and withpotentially greater effect.”

Future outlookKaleido is already collaborating with the Johnson &Johnson subsidiary, Janssen, to explore the poten-tial for MMTs in childhood onset of atopic, immuneand metabolic conditions.

“Our MMTs are targeted and have broad appli-cability across a variety of conditions,” said vanHylckama Vlieg. “The gut microbiome is a largelyuntapped frontier in health care, and we areuniquely positioned to succeed in translating itspromise into solutions for patients.”

• Target enzymes across taxa rather thanonly in specific species, driving ecosystemand metabolic output changes

• Related to a class of compounds that isGenerally Recognized as Safe (GRAS),enabling rapid advancement into humanclinical studies

• Extensive intellectual property, NCEswhen developed as drugs

• Orally administered with limitedsystemic exposure

MICROBIOME METABOLIC THERAPIES (MMTs):Structurally diverse synthetic glycans that act as targetedand versatile modulators of microbiome communitycomposition and metabolic output

Chain lengthmono-oligo-poly-

saccharide

Our library of 1,500+ MMTs:

+ Multiplebond types

+ Branching

Starting monomers

Almost unlimiteddiversity ofchemical structuresin this class

Fig. 1 | Synthetic glycan chemistry enables extensive array of Microbiome Metabolic Therapies (MMTs).Using a chemistry-driven approach to systematically drive functional outputs of the microbiome, KaleidoBiosciences has built a proprietary product platform. NCEs, new chemical entities.

Norma Alonzo PalmaHead Scientific & Medical AffairsKaleido BiosciencesLexington, MA, USATel: +1-617-674-9000Email: norma.alonzo-palma@kaleido.com

CON

TACT

www.nature.com/biopharmdeal | December 2020 | B17