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NUTRACEUTICALS: An emerging field for metabolic engineering of Lactic Acid Bacteria MALVIKA MALIK 1 , RAVINDER NAGPAL 1 , MONICA PUNIYA 2 , ARTI BHARDWAJ 3 , SHALINI JAIN 4 and HARIOM YADAV 4* 1 Dairy Microbiology, 2 Dairy Cattle Nutrition, 4 Animal Biochemistry, National Dairy Research Institute, Karnal 132001, Haryana, Meerut Institute of Engineering and Technology, Meerut- 250002, U.P., India. *Email: [email protected]

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Page 1: An emerging field for metabolic engineering of Lactic Acid Bacterialibvolume2.xyz/biotechnology/semester8/metabolic... · 2015-01-14 · NUTRACEUTICALS: An emerging field for metabolic

NUTRACEUTICALS: An emerging field for metabolic engineering of Lactic Acid Bacteria

MALVIKA MALIK1, RAVINDER NAGPAL1, MONICA PUNIYA2, ARTI BHARDWAJ3, SHALINI JAIN4 and HARIOM YADAV4*

1Dairy Microbiology, 2Dairy Cattle Nutrition, 4Animal Biochemistry,

National Dairy Research Institute, Karnal 132001,

Haryana, Meerut Institute of Engineering and Technology, Meerut-250002, U.P., India.

*Email: [email protected]

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Nutraceuticals

• The term ‘Nutraceuticals’, launched by

Stephen De-Felici in the 1980s

• A food or part of a food that may provide

medicinal or health benefits, including the

prevention and treatment of disease.

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Metabolic Engineering

�Metabolic engineering is the practice of

optimizing genetic and regulatory

processes within cells to increase the cells'

production of a certain substance

� Controlled over expression of desired

genes

�Inactivation of undesired genes

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Examples of metabolic

engineering of LAB

• Increased production of diacetyl from

glucose and lactose

• Efficient production of L-alanine from sugar

• Production of non-metabolisable sugars

• Galactose and/or lactose removal from dairy

products

• Oligosaccharide production

• Vitamin production

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Lactic acid bacteria as cell-factories

• Lactic acid bacteria (LAB) are industrially important microbes, used in a large variety of food fermentations

• The NICE system for controlled heterologous and homologous gene expression in Lactic acid bacteria has been employed in many of the metabolic engineering strategies

(Boels et al. 2001; Sybesma et al. 2002)

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Why Lactic acid bacteria?

• The bacterium is food grade

• Plasmid selection mechanisms are available that are food

grade and self cloning

• No endotoxins or inclusion bodies are formed and

• Sophisticated genetic tools enable easy genetic handling

• Simple, non-aerated fermentation makes direct scale-up

from 1-L scale to 1000-L scale possible

• Nisin controlled gene expression can be effectively used

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NICE

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Increased Vitamins Production

• Folate

– Involved in biosynthesis of nucleotides

– Daily recommended intake for an adult is 200 µg

– Known to prevent neural-tube defect in infants

– Protect against some forms of cancer

• Main sources are vegetables and dairy products

• Milk is good source, fermented dairy products

like yoghurt are also important

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• Streptococcus thermophilus and Lactococcus lactis execute de novo biosynthesis of folates to secrete surplus folate

• Therefore can be used to make starter with increased folate levels

• In experimental yoghurt up to 150 µg/L folate has been reported

(Smid etal. 2001)

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Part of Folate gene cluster L. lactis

cloned behind strong promoter

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• The genes involved in folate biosynthesis have been

analysed completely.

• By genetic eng. several of these genes have been over

expressed in L.lactisNZ9000 using the NICE system

• Individual gene can be over expressed or in

combination

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• Folate normally synthesis as polyglutamyl-folate

derivatives intracellularly

• Absorbed in human guts as monoglutamyl folate

derivatives

• γ -glutamyl hydrolase cDNA introduced in L.

lactis

• Resulted in an inversion of folate spatial

distribution

(Sybesma et al. 2002)

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High production of folate by over

expression of whole fol gene cluster

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Folate production in engineered

Lb. gasseri

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Folate level in the organs of animals depleted

in folate and supplemented with LAB folate

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Riboflavin (B2)

• Riboflavin-deficiency can lead to:-

– Liver(Ross & Klein 1990) and skin-disorders

(Lakshimi 1998)

– Disturbed metabolism of the red blood cells

(Hassan & Thurnham 1977)

– Reduced performance during physical exercise

(Belko et al. 1983; Bates 1987)

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• In Bacillus subtilis first reaction in riboflavin

biosynthesis has been demonstrated to be

rate limiting (Humbelin et al. 1999)

• The gene coding for this enzyme, ribA, has

been brought to overexpression in L. lactis

using the NICE-system

• This resulted in a 3-fold overproduction of

riboflavin

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Production of non-metabolisable sugars

• Mannitol and sorbitol (polyols) and trehalose could

replace sucrose, lactose, glucose or fructose in

food products

• In colon they are fermented by micro-organisms to

short-chain fatty acids (mainly butyrate) which may

prevent colon cancer

• Trehalose is therapeutic against illnesses, such as

the Creutzfeld-Jakob disease

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• Mannitol and sorbitol have stool-bulking

properties and can be used as dietary fibers

• They are active as bifidogenic prebiotic

• Cholesterol lowering , immunomodulant

• They display equivalent sweetness and taste

(Dwivedi 1978)

• Mannitol can also serve as anti-oxidant in

biological cells

(Shen et al. 1997)

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Activation of Sorbitol production

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• Heterofermentative lactic acid bacteria such as

Leuconostoc mesenteroides are known to

produce mannitol in the fermentation of fructose

(Soetaert et al. 1995)

• homofermentative lactic acid bacteria can also

produce mannitol

• In both Lactobacillus plantarum (Ferain et al.

1996) and Lactococus lactis (Neves et al. 2000),

disruption of lactate dehydrogenase (LDH)

resulted in production mannitol along with other

metabolites

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• Overproduction of the mannitol-P dehydrogenase (MPDH) in a LDH-deficient L. lactis strain has resulted in strong increase in intracellular mannitol production

• Similar results were obtained when MPDH was overproduced in a strain with decreased phosphofructokinase (PFK) activity

• Production of mannitol by Lactococcus lactis can be increased if excretion of this polyol is facilitated, by introducing the mannitol-transporter present in Leuconostoc mesenteroides.

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Increasing Mannitol production

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Effect of pH on the production of mannitol and sorbitol

by

Lb. plantarum VL202

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Tagatose production

• A potential sucrose replacement.

• Higher sweetening power than similar components

such as mannitol, sorbitol and erythritol

• Much lower caloric value

(Zehner 1988)

• Recently been launched on the food market as low

calorie sugar, as prebiotic

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Calorific values of different

sugars

• Glucose 4.0 cal/gm

• Mannitol 1.5 cal/gm

• Sorbitol 2.5 cal/gm

• Erythritol 0.2 cal/gm

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• Chosen strategy is to disrupt the lacC and/or lacD genes resulting in production of either tagatose-6-P or tagatose-1,6-diphosphate

• Disruption of lacD was accomplished via a two step procedure

– recombination process, involving integration of an erythromycin-resistance plasmid containing only the lacC and lacF genes via single crossing-over

– removal of lacD (or reversion to the wild-type) in a second, spontaneous, recombination event

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Production of polysaccharides

• Exopolysaccharides (EPS)

– Some polysaccharides produced by lactic

acid bacteria have prebiotic

(Gibson & Roberfroid 1995)

– Immunostimulatory

(Hosono et al. 1997)

– Antitumoral

(Kitazawa et al. 1991)

– Cholesterol-lowering activity

(Nakajima et al. 1992a)

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• The specific eps genes are encoded on

large plasmids

• Conjugally transferred from one

lactococcal strain to the next, thereby

introducing the EPS-producing capacity in

the recipient strain

( van Kranenburg et al. 1997)

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Polysaccharide gene cluster in various

LAB

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Improving sugar conversion

• In cow’s milk 4–4.5% (w/v) of lactose

present

• In liquid fermented dairy products, such

as yoghurt or buttermilk, usually less than

half is fermented to lactic acid

• These products are unsuitable for lactose

intolerant persons

• The lactose is converted to galactose and

later to galactitol

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• For most lactic acid bacteria, galactose is a

poor substrate

• The efficiency lactose utilization by L.lactis

can be increased by metabolic engineering

• Secondly lactose metabolism in L. lactis can

be modified in such a way that the glucose

moiety will end up in the product, while

galactose will be fully used for growth, in this

way providing a natural sweetening process

for dairy products

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Galactose of Lactose being fully utilized and

Glucose ends up in the product

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• Free galactose is accumulated intracellularly as a

result of the absence of galactokinase activity in

these strains

• Streptococcus thermophilus, gene for

galactokinase is completely intact, but that one or

more point mutations have taken place leading to a

‘silent’ phenotype (Vaughan et al. 2001).

• Sometimes these mutations may revert back

spontaneously

• To enhance the galactose utilization these

mutations can be reverted deliberately

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αααα- Galactosides and their hydrolytic

enzymes

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Removal of raffinose

• Soy- and pulse-derived food products contain

high levels of α-galactosides such as stachyose

and raffinose

• These are not metabolized in human gut due to

lack of α- galactosidase

• These undigested α- galactosides accumulate in

the lower gut and induce gastric problems like

flatulence

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• By applying metabolic engineering strategies, lactic

acid bacteria can be constructed with high α-

galactosidase activities

• Starters for removal of α-galactosides during soy

fermentation

• Possible probiotics to deliver α-galactosidase

activity in the gut for prevention of flatulence

• In Lactobacillus plantarum gene (melA) code for

α-galactosidase

(Silvestroni et al. 2002)

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• For construction of starter and probiotic bacteria

with high α-galactosidase activity, the melA is

cloned in L. lactis in three different constructions

resulting in

– expression of the enzyme in the cytoplasm for

maximum protection of enzyme activity

– expression as a secreted enzyme for maximum

exposure to the sugar substrate

– expression on the surface but anchored to the

surface of the cell

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Conclusion

• Metabolic engineering has provided a powerful

and effective tool for production of nutraceuticals

• Metabolic engineering approach can also be

applied for production of more benificial product.

• With increasing knowledge of the genomic

analysis metabolic engineering can further be

explored for more nutraceutical production.