Titrations

Introduction

1.) Buret Evolution

 Primary tool for titration
Gay-Lussac (1824)
Blow out liquid
Mohr (1855)
Compression clip
Used for 100 years

Descroizilles (1806) Henry (1846) Mohr (1855)

Pour out liquid Copper stopcock Glass stopcock
 Titrations
Introduction

2.) Volumetric analysis

 Procedures in which we measure the volume of
reagent needed to react with an analyte

3.) Titration
 Increments of reagent solution (titrant) are added
to analyte until reaction is complete.
- Usually using a buret

 Calculate quantity of analyte from the amount of

titrant added.

 Requires large equilibrium constant

 Requires rapid reaction
- Titrant is rapidly consumed by analyte

Controlled Chemical Reaction

 Titrations

Introduction

4.) Equivalence point

 Quantity of added titrant is the exact amount necessary for stoichiometric
reaction with the analyte
- Ideal theoretical result

Analyte Titrant (colorless) (colorless)

Oxalic acid (purple)
(colorless)

Equivalence point occurs when 2 moles of MnO4- is added to 5 moles of Oxalic acid
 Titrations

Introduction

5.) End point

 What we actually measure
- Marked by a sudden change in the physical property of the solution
- Change in color, pH, voltage, current, absorbance of light,
presence/absence ppt.

CuCl Titration with NaOH

Before any addition of NaOH After the addition of End Point

8 drops of NaOH
 Titrations

Introduction

5.) End point

 Occurs from the addition of a slight excess of titrant
- Endpoint does not equal equivalence point

Analyte Titrant (colorless) (colorless)

Oxalic acid (purple)
(colorless)

After equivalence point occurs, excess MnO4- turns solution purple  Endpoint
 Titrations

Introduction

5.) End point

 Titration Error
- Difference between endpoint and equivalence point
- Corrected by a blank titration
i. repeat procedure without analyte
ii. Determine amount of titrant needed to observe change
iii. subtract blank volume from titration

 Primary Standard
- Accuracy of titration requires knowing precisely the
quantity of titrant added.
- 99.9% pure or better  accurately measure concentration

Analyte Titrant
Oxalic acid (purple)
(colorless)
 Titrations

Introduction

6.) Standardization
 Required when a non-primary titrant is used
- Prepare titrant with approximately the desired concentration
- Use it to titrate a primary standard
- Determine the concentration of the titrant
- Reverse of the normal titration process!!!

Titration Standardization

titrant known titrant unknown

concentration concentration

analyte unknown
analyte known
concentration
concentration
 Titrations

Introduction

7.) Back Titration

 Add excess of one standard reagent (known concentration)
- Completely react all the analyte
- Add enough MnO4- so all oxalic acid is converted to product

Analyte Titrant (colorless) (colorless)

Oxalic acid (purple)
(colorless)

 Titrate excess standard reagent to determine how much is left

- Titrate Fe2+ to determine the amount of MnO4- that did not react with oxalic acid
- Differences is related to amount of analyte
- Useful if better/easier to detect endpoint
 Titrations

Titration Calculations

1.) Key – relate moles of titrant to moles of analyte

2.) Standardization of Titrant Followed by Analysis of Unknown

Calculation of ascorbic acid in Vitamin C tablet:

(i) Starch is used as an indicator: starch + I3-  starch-I3- complex

(clear) (deep blue)

(ii) Titrate ascorbic acid with I3-:

1 mole ascorbic acid  1 mole I3-

 Titrations

Titration Calculations

2.) Standardization of Titrant Followed by Analysis of Unknown

Standardization: Suppose 29.41 mL of I3- solution is required to react with 0.1970 g of

pure ascorbic acid, what is the molarity of the I3- solution?
 Titrations

Titration Calculations

2.) Standardization of Titrant Followed by Analysis of Unknown

Analysis of Unknown: A vitamin C tablet containing ascorbic acid plus an inert binder
was ground to a powder, and 0.4242g was titrated by 31.63 mL of I3-. Find the weight
percent of ascorbic acid in the tablet.
 Titrations

Spectrophotometric Titrations

1.) Use Absorbance of Light to Follow Progress of Titration

 Example:
- Titrate a protein with Fe3+ where product (complex) has red color
- Product has an absorbance maximum at 465 nm
- Absorbance is proportional to the concentration of iron bound to protein

Analyte titrant (red)

(colorless) (colorless)

As Fe3+ binds protein

solution turns red

 Titrations

Spectrophotometric Titrations

1.) Use Absorbance of Light to Follow Progress of Titration

 Example:
- As more Fe3+ is added, red color and absorbance increases,
- When the protein is saturated with iron, no further color can form
- End point – intersection of two lines (titrant has some absorbance at 465nm)

When all the protein is bound to Fe3+,

no further increase in absorbance.

As Fe3+ continues to bind protein

red color and absorbance increases.
 Titrations

Spectrophotometric Titrations

1.) Use Absorbance of Light to Follow Progress of Titration

 Example:
- As more Fe3+ is added, concentration changes due to dilution
- Need to correct absorbance for dilution.

 total volume 
Corrected absorbance   observed absorbance 
 initial volume 

Total volume changes after each addition

 Titrations

Precipitation Titration Curve

1.) Graph showing how the concentration of one of the reactants varies as titrant
is added.

Sharpness determined
by titration condition

Monitor pH, voltage,

current, color,
absorbance, ppt.

 Understand the chemistry that occurs during titration

 Learn how experimental control can be exerted to influence the quality of
an analytical titration
- No end point at wrong pH
- Concentration of analyte and titrant and size of Ksp influence end point
- Help choose indicator for acid/base and oxidation/reduction titrations
 Titrations

Precipitation Titration Curve

2.) Because concentration varies over many orders of magnitude, plot p function

p function: pX   log 10 [ X ]
where [X] is concentration of X

3.) Example:
Consider the titration of 25.00 mL of 0.1000M I- with 0.05000M Ag+

K sp  [ Ag  ][ I  ]  8.3  10 17

Since Ksp is so small, each addition of Ag+ reacts completely with I-

 Titrations

Precipitation Titration Curve

3.) Example:
At equivalence point, sudden increase in Ag+ concentration.
- All I- has been consumed

What volume (Ve) of Ag+ titrant is need to reach the equivalence point?

0.02500 L   0.1000 mol I  / L   Ve   0.05000 mol Ag  / L 

mol I- mol Ag+

 Ve  0.05000  50.00 mL

One mole of Ag+ reacts with one mol I-

 Titrations

Precipitation Titration Curve

4.) Three distinct regions in titration curve

 Before, at and after the equivalence point.
after

at
before

 Before the Equivalence Point

- All titrant [Ag+] is consumed, free [I-] is [I-] that has not been precipitated.
- Negligible I- from AgI(s) (Ksp)

Moles of I- = original moles of I- - moles of Ag+ added

 Titrations

Precipitation Titration Curve

4.) Three distinct regions in titration curve

 Before the Equivalence Point
- Concentration of Ag+ is governed by Ksp

Consider the titration of 25.00 mL of 0.1000M I- with 10 mL of 0.05000M Ag+

Moles of I- = original moles of I- - moles of Ag+ added

Moles of I   0.02500 L   0.100 mol / L   0.01000 L   0.05000 mol / L   0.002000 mol I 

Volume is 0.3500 L ( 25.00 mL + 10.00 mL)

0.00200 mol I 

Molarity of I   0.05714 M
0.03500 L

Concentration of Ag+ in equilibrium with this much I-

Ag 
 K sp
  
[I ]
8.3  10 17
0.05714
 1.5  10 15 M
 Titrations

Precipitation Titration Curve

4.) Three distinct regions in titration curve

 Before the Equivalence Point
- Concentration of Ag+ is governed by Ksp

p function

pAg    log [ Ag  ]  - log ( 1.5  10 -15 )  14 .84

2 sig. fig.  2 sig. fig. in
the mantissa of p function
 At Equivalence Point
- added exactly enough Ag+ to react with all I-
- [Ag+] independent of the original concentrations
- [Ag+] dependent on Ksp

K sp  [ Ag  ][ I  ]  8.3  10 17

( x )( x )  8.3  10 17  x  9.1  10 9  pAg    log x  8.04

 Titrations

Precipitation Titration Curve

4.) Three distinct regions in titration curve

 After Equivalence Point
- All Ag+ added before equivalence point has ppt.
- [Ag+] is determined by Ag+ added after the equivalence point.
> volume after equivalence point

For 2 mL of Ag+ added past equivalence point

 
Moles of Ag   0.00200 L   0.05000 mol Ag  / L  0.000100 mol Ag 
[ Ag  ]  ( 0 .000100 mol)/( 0 .07700 L)  1.30  10 - 3 M  pAg   2.89
 Titrations

Shape of Titration Curve

1.) Equivalence point is the steepest point of the curve.

 Point of maximum slope  inflection point  second derivative is zero

dy
Steepest slope : reaches greatest value
dx
d2y
Inflection po int : 0
dx 2
 Titrations

Shape of Titration Curve

2.) Affect of Ksp on Titration Curve.

 Lowest solubility gives steepest change at equivalence point

Magnitude of concentration
change and ease of identifying
equivalence point increases
with Ksp
 Titrations

Titration of a Mixture

1.) Product with the Smaller Ksp Precipitates First

 Two Stage Titration Curve
- Assumes significant difference in Ksp

First, AgI ppt.

Titrate Mixture of KI and KCl
with AgNO3

Then, AgCl ppt.

Ksp(AgI) << Ksp(AgCl)

AgI ppt. not complete

at midpoint
 Titrations

End-Point Detection

1.) Precipitation Titration

 End points detected with electrode or indicator
- Electrode – converts concentration of specific ion into measurable current or
potential.

pH electrode responds to [H+]

- Indicators:
Volhard titration: formation of a soluble, colored complex at the end point

Fajans titration: adsorption of a colored indicator on the precipitate at the end

point
 Titrations

End-Point Detection

1.) Precipitation Titration

 Volhard titration (First Published in 1874)

Determine [Cl-]:

First ppt. Cl- by titration with Ag+ and filter off solid

Titrate excess Ag+ with thiocyanate (SCN-)

When all Ag+ is consumed, thiocyanate binds

Fe3+. Appearance of Red color is endpoint

Total amount of Ag+ is known, so amount consumed by Cl- can be calculated

Subtract excess [Ag+] from total [Ag+] used to ppt. Cl-
 Titrations AgCl ppt.

End-Point Detection

1.) Precipitation Titration

 Fajans titration
- Uses an adsorption indicator

Precipitate surface is initially

negatively charged due to excess Cl-
AgCl ppt.

After equivalence point (end point), have

excess Ag+ so surface is now positively
charged.

Anionic dye is attracted to positive charged

surface. Adsorption of dye causes color change
 Titrations

End-Point Detection

1.) Precipitation Titration

 Fajans titration
 Anionic dyes
- Maximize surface area  higher binding stronger color change
- small particle size  low concentration
- must use appropriate pH to maintain negative charge

Sharper color transition, binds to tightly to Cl-

Changes from greenish yellow to pink
 Titrations
End-Point Detection

2.) Typical Applications

 Also indicates potential sources of interference
- other ions/analytes may be present in sample