Kinetics of Biomass Formation, Substrate Utilization and Product Formation in Cell Cultures

Kinetics of biomass formation, substrate utilization and
product formation in cell cultures
VIVEK R BITS Pilani, K K Birla Goa Campus

Biomass formation kinetics

Natural growth Vs Controlled growth
Animals, Plants  Eukaryotes  Difficult to tune up as a whole (-) (Climate dependent)
Animal and plant cells  tunable  controlled growth (+)

Growth in
Yeasts and moulds  lower eukaryotes  controlled growth ( + + )
Bioreactors
Bacteria prokaryotes  controlled growth ( + + + )

Simple-complex-simple

 Bacteria reproduce by binary fission, by asexual mode or by budding
 Binary fission one cell becomes two organisms
 The required time for each cell division is generation time ( can vary from days to less than 20 min)
 For example  if generation time is 30 min, one bacterium will form 224 = 16,777,216
after a period of 12 h
BITS Pilani, K K Birla Goa Campus

Batch growth
Also called log/exponential phase
𝟏 𝒅𝒙
µ=
𝒙 𝒅𝒕
x  biomass concentration
1) Exponential phase

Rate of cell growth in growth and decline phases
rx = µ. x = dx/dt rx in kg m-3 h-1

µ in h-1; x in g L -1
Integrating with x=x0 at t=0
𝑑𝑥
= 𝜇 𝑑𝑡
𝑥
ln 𝑥 = ln 𝑥0 + 𝜇 𝑡
𝒙 = 𝒙𝒐 𝒆𝝁𝒕

ln x and x vs t: use ln x vs t to calculate µ

Doubling time
Doubling time is the period of time required for the cells to double in weight/ number
When x0 is the starting concentration; at t=td x= 2x0
2𝑥0 = 𝑥0 𝑒 𝜇𝑡
𝐥𝐧 𝟐
𝒕𝒅 =
𝝁
Balanced growth
During balanced growth, the composition of the biomass remains constant.
rZ = µ z
where Z is a cellular constituent such as protein, RNA, polysaccharide, and so on, rZ is
the
volumetric rate of production of Z, and zVIVEK
is theR concentration of Z in the reactor volume
BITS Pilani, K K Birla Goa Campus
2) Stationary phase

Endogenous metabolism in stationary phase
Some times µ is expressed as µ net when endogenous metabolism is considered
𝟏 𝒅𝒙
𝝁𝒏𝒆𝒕 =
𝒙 𝒅𝒕 𝜇𝑛𝑒𝑡 = 𝑛𝑒𝑡 𝑠𝑝𝑒𝑐𝑖𝑓𝑖𝑐 𝑔𝑟𝑜𝑤𝑡ℎ 𝑟𝑎𝑡𝑒, ℎ−1
𝜇𝑔 = 𝑔𝑟𝑜𝑠𝑠 𝑠𝑝𝑒𝑐𝑖𝑓𝑖𝑐 𝑔𝑟𝑜𝑤𝑡ℎ 𝑟𝑎𝑡𝑒, ℎ−1
𝝁𝒏𝒆𝒕 = 𝝁𝒈 − 𝒌𝒅 𝑘𝑑 = 𝑟𝑎𝑡𝑒 𝑐𝑜𝑛𝑠𝑡𝑎𝑛𝑡 𝑓𝑜𝑟 𝑒𝑛𝑑𝑜𝑔𝑒𝑛𝑜𝑢𝑠, ℎ−
In stationary phase, cells catabolize their cellular reserves for new building blocks,
called endogenous metabolism
𝒅𝒙
= −𝒌𝒅 𝒙 or 𝒙 = 𝒙𝒔𝟎 𝒆−𝒌𝒅𝒕
𝒅𝒕
xso  the cell mass concentration at the beginning of the stationary
phase.
3) Death phase

Death phase
The rate of death usually follows first-order kinetics
𝑑𝑁
= −𝑘′𝑑 𝑁
𝑑𝑡
−𝒌′ 𝒕
𝑵 = 𝑵𝑺 𝒆 𝒅
where Ns number concentration of cells at the end of the stationary phase

k’d first order death-rate constant.

Batch growth
Also called log/exponential phase
𝟏 𝒅𝒙
µ=
𝒙 𝒅𝒕
x  biomass concentration
Effect of substrate concentration on specific growth rate

Effect of substrate concentration on specific growth rate
During balanced growth

Specific growth rate is related to the substrate concentration, often a rate limiting substrate
Monod Model 𝝁𝒎𝒂𝒙 𝑺

𝝁=
𝑲𝒔 + 𝑺
S  concentration of rate limiting substrate Zero order
Ks  substrate/ monod/saturation constant g/L or mg/L
𝝁𝒎𝒂𝒙  maximum specific growth rate T -1
First order
𝝁 independent of substrate concentration until S > 10 Ks
In batch growth, substrate concentration S >> Ks

KS Values for Several Organisms

Monod model limitations
The most frequently used expression relating growth rate to substrate concentration.
 Valid only for balanced growth and should not be applied when growth conditions
are changing rapidly
 Limited applicability at extremely low substrate levels.
Extra terms can be added to Monod expression when there is growth inhibition due to high
substrate and product concentration

Exponential vs Logistic biomass growth

Exponential Vs logistic biomass growth
 Starts rapidly  Starts slowly

 Rate proportional to the cells  Rate begins to slow down when organisms
which already exist are in competition for limited space
The logistic equation
The sigmoidal shape of the growth curve can be predicted by combining Monod equation and
with the growth equation
𝜇𝑚𝑎𝑥 𝑆
𝜇= Eq 1
𝐾𝑠 + 𝑆
𝑑𝑥
= 𝜇𝑥 Eq 2
𝑑𝑡
𝑑𝑥 𝜇𝑚𝑎𝑥 𝑆
= 𝑥 Eq 3
𝑑𝑡 𝐾𝑆 + 𝑆

The relationship between microbial growth and substrate consumption is given by
𝑥 − 𝑥0
𝑌𝑋/𝑆 = Eq 4
𝑆0 − 𝑆
Substituting for S in Eq 3 from Eq 4
𝑑𝑥 𝜇𝑚 (𝑌𝑋/𝑆 𝑆0 + 𝑥0 − 𝑥)
= 𝑥 Eq 5
𝑑𝑡 (𝐾𝑆 𝑌𝑋/𝑆 + 𝑌𝑋/𝑆 𝑆0 + 𝑥0 − 𝑥)
The integrated form of rate expression is Eq 6
(𝑲𝑺 𝒀𝑿/𝑺 + 𝑺𝟎 𝒀𝑿/𝑺 + 𝒙𝟎 ) 𝒙 𝑲𝑺 𝒀𝑿/𝑺 𝒀𝑿/𝑺 𝑺𝟎 + 𝒙𝟎 − 𝒙

𝐥𝐧 − 𝐥𝐧 = 𝝁𝒎 𝒕
(𝒀𝑿/𝑺 𝑺𝟎 + 𝒙𝟎 ) 𝒙𝟎 (𝒀𝑿/𝑺 𝑺𝟎 + 𝒙𝟎 ) 𝒀𝑿/𝑺 𝑺𝟎

Eq 5 requires a predetermined knowledge about the maximum cell mass (x∞)
in a particular environment, also called as carrying capacity
Logistic equations are set of equation that characterize growth in terms of their carrying capacity
Usually the specific growth rate is related to the amount of unused carrying capacity
𝑥
𝜇 = 𝐾 (1 − ) Eq 7
𝑥∞
𝑑𝑥 𝑥 Eq 8
= 𝐾𝑥(1 − )
𝑑𝑡 𝑥∞
K  carrying capacity coefficient

Integrating with B.C: x(0) = x0
𝒙𝟎 𝒆𝒌𝒕
𝒙= 𝒙𝟎 Eq 9
𝟏− (𝟏 − 𝒆𝒌𝒕 )
𝒙∞
Eq 9 is represented by the growth curve

Cell mass concentration
Dry weight method Optical density
Centrifuge the broth Dilute the sample appropriately

using pre-weighed filter paper
Take optical density

Dry the paper in hot air over
OD 600 nm
At 80 °C till constant weight
(Vis spectrophotometer)
Calculate mass difference

Quantifying cell concentration
 Cell number density

Haemocytometer
Cell count by serial dilution
 Cell mass concentration

Dry cell weight/wet cell weight
Optical density

Cell counting using haemocytometer
Volume enclosed by the cover slip for each large square = 0.1 mm3

Viable cell count by serial dilution method

Kinetics of Biomass Formation, Substrate Utilization and Product Formation in Cell Cultures

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Kinetics of biomass formation, substrate utilization and

product formation in cell cultures

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

Animals, Plants  Eukaryotes  Difficult to tune up as a whole (-) (Climate dependent)

Animal and plant cells  tunable  controlled growth (+)

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

BITS Pilani, K K Birla Goa Campus

Also called log/exponential phase

VIVEK R BITS Pilani, K K Birla Goa Campus

rx = µ. x = dx/dt rx in kg m-3 h-1

Integrating with x=x0 at t=0

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

Some times µ is expressed as µ net when endogenous metabolism is considered

VIVEK R BITS Pilani, K K Birla Goa Campus

The rate of death usually follows first-order kinetics

where Ns number concentration of cells at the end of the stationary phase

VIVEK R BITS Pilani, K K Birla Goa Campus

Also called log/exponential phase

VIVEK R BITS Pilani, K K Birla Goa Campus

During balanced growth

Monod Model 𝝁𝒎𝒂𝒙 𝑺

In batch growth, substrate concentration S >> Ks

VIVEK R BITS Pilani, K K Birla Goa Campus

 Limited applicability at extremely low substrate levels.

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

 Starts rapidly  Starts slowly

VIVEK R BITS Pilani, K K Birla Goa Campus

The integrated form of rate expression is Eq 6

(𝑲𝑺 𝒀𝑿/𝑺 + 𝑺𝟎 𝒀𝑿/𝑺 + 𝒙𝟎 ) 𝒙 𝑲𝑺 𝒀𝑿/𝑺 𝒀𝑿/𝑺 𝑺𝟎 + 𝒙𝟎 − 𝒙

VIVEK R BITS Pilani, K K Birla Goa Campus

K  carrying capacity coefficient

Eq 9 is represented by the growth curve

VIVEK R BITS Pilani, K K Birla Goa Campus

Dry weight method Optical density

Centrifuge the broth Dilute the sample appropriately

Take optical density

Calculate mass difference

VIVEK R BITS Pilani, K K Birla Goa Campus

 Cell number density

 Cell mass concentration

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

VIVEK R BITS Pilani, K K Birla Goa Campus

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