Difference between revisions of "Sequence-based mutation analysis Gaucher Disease"
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− | ! Nr !! Mutation !! Score |
+ | ! Nr !! Mutation !! Score<br/>mutation !! Score<br/>min !! Score<br/>max !! Conservation |
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− | | colspan=6 style="border-collapse: separate; border-style: solid; border-spacing: 0; border-width: |
+ | | colspan=6 style="border-collapse: separate; border-style: solid; border-spacing: 0; border-width: 0 0 1px 0"| |
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− | | 1 || H99R || 0 || -4 || 2 |
+ | | 1 || H99R || 0 || -4 || 2 || [[File:subst_pssm_all_col99.png|150px]] |
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− | | 2 || V211I || 4 || -4 || 4 |
+ | | 2 || V211I || 4 || -4 || 4 || [[File:subst_pssm_all_col211.png|150px]] |
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− | | 3 || E150K || 0 || -4 || 5 |
+ | | 3 || E150K || 0 || -4 || 5 || [[File:subst_pssm_all_col150.png|150px]] |
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− | | 4 || L236P || 0 || -3 || 1 |
+ | | 4 || L236P || 0 || -3 || 1 || [[File:subst_pssm_all_col236.png|150px]] |
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− | | 5 || W248R || -2 || -3 || 4 |
+ | | 5 || W248R || -2 || -3 || 4 || [[File:subst_pssm_all_col248.png|150px]] |
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− | | 6 || L509P || -6 || -6 || 4 |
+ | | 6 || L509P || -6 || -6 || 4 || [[File:subst_pssm_all_col509.png|150px]] |
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− | | 7 || W351C || -3 || -6 || 9 |
+ | | 7 || W351C || -3 || -6 || 9 || [[File:subst_pssm_all_col351.png|150px]] |
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− | | 8 || A423D || -3 || -3 || 3 |
+ | | 8 || A423D || -3 || -3 || 3 || [[File:subst_pssm_all_col423.png|150px]] |
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− | | 9 || D482N || 4 || -4 || 4 |
+ | | 9 || D482N || 4 || -4 || 4 || [[File:subst_pssm_all_col482.png|150px]] |
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− | | 10 || R83S || 0 || -3 || 2 |
+ | | 10 || R83S || 0 || -3 || 2 || [[File:subst_pssm_all_col83.png|150px]] |
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<caption>Position specific substitution scores derived from all significant hits after 5 rounds PSI-BLAST.</caption> |
<caption>Position specific substitution scores derived from all significant hits after 5 rounds PSI-BLAST.</caption> |
Revision as of 07:52, 17 June 2012
The aim of this task was to carry out a thorough analysis of ten mutations and to classify them as disease-causing and non-disease causing. The mutations have been selected by another group from our [Researching SNPs Gaucher Disease|set of collected mutations] such that their impact had been unknown for us prior to this task. Technical details are reported in our protocol.
Contents
Mutations
<figtable id="tab:mutations">
Nr | Position | From | To |
---|---|---|---|
1 | 99 | H | R |
2 | 211 | V | I |
3 | 150 | E | K |
4 | 236 | L | P |
5 | 248 | W | R |
6 | 509 | L | P |
7 | 351 | W | C |
8 | 423 | A | D |
9 | 482 | D | N |
10 | 83 | R | S |
Randomly selected mutations from HGMD and dbSNP which were used for the sequence-based mutation analysis. </figtable>
Physicochemical properties
<figtable id="tab:props">
Nr | Wildtype | Mutant | Severe change | ||||||||
---|---|---|---|---|---|---|---|---|---|---|---|
AA | Charge | Polarity | Size | Aromatic | AA | Charge | Polarity | Size | Aromatic | ||
1 | H | negative | polar | large | no | R | negative | polar | large | no | no |
2 | V | neutral | unpolar | medium | no | I | neutral | unpolar | medium | no | no |
3 | E | positive | polar | large | no | K | negative | polar | large | no | yes |
4 | L | neutral | unpolar | medium | no | P | neutral | unpolar | medium | no | no |
5 | W | neutral | unpolar | large | yes | R | negative | polar | large | no | yes |
6 | L | neutral | unpolar | medium | no | P | neutral | unpolar | medium | no | no |
7 | W | neutral | unpolar | large | yes | C | neutral | polar | small | no | yes |
8 | A | neutral | unpolar | small | no | D | positive | polar | medium | no | yes |
9 | D | positive | polar | medium | no | N | neutral | polar | medium | no | no |
10 | R | negative | polar | large | no | S | neutral | polar | small | no | no |
Physicochemical properiets of the wildtype and mutatant amino acid which were used to classify the mutation as severe or non-severe. </figtable>
Structural analysis
<figtable id="tab:structure">
Location of mutations in 2nt0_A. Blue: wildtype; Red: mutant. </figtable>
<figure id="fig:structure_all">
</figure>
Substitution scores
BLOSUM62 scores
The scores were taken from the BLOSUM62 matrix.
<figtable id="tab:subst_blosum">
Nr | Mutation | Score mutation | Score min | Score max |
---|---|---|---|---|
1 | H99R | 0 | -3 | 8 |
2 | V211I | 3 | -3 | 4 |
3 | E150K | 1 | -4 | 5 |
4 | L236P | -3 | -4 | 4 |
5 | W248R | -3 | -4 | 11 |
6 | L509P | -3 | -4 | 4 |
7 | W351C | -2 | -4 | 11 |
8 | A423D | -2 | -3 | 4 |
9 | D482N | 1 | -4 | 6 |
10 | R83S | -1 | -3 | 5 |
BLOSUM62 scores of the selected mutations </figtable>
PSSM of all hits
PSSM.
<figtable id="tab:subst_pssm_all">
Position specific substitution scores derived from all significant hits after 5 rounds PSI-BLAST. </figtable>
Scoring Mutants
SIFT
The predicted results from SIFT Blink is shown here:
Substitution at pos 83 from R to S is predicted to be TOLERATED with a score of 0.17. Median sequence conservation: 2.12 Sequences represented at this position:77 Substitution at pos 99 from H to R is predicted to be TOLERATED with a score of 0.64. Median sequence conservation: 2.14 Sequences represented at this position:80 Substitution at pos 150 from E to K is predicted to be TOLERATED with a score of 0.76. Median sequence conservation: 2.10 Sequences represented at this position:86 Substitution at pos 211 from V to I is predicted to be TOLERATED with a score of 0.56. Median sequence conservation: 2.09 Sequences represented at this position:86 Substitution at pos 236 from L to P is predicted to AFFECT PROTEIN FUNCTION with a score of 0.02. Median sequence conservation: 2.09 Sequences represented at this position:86 Substitution at pos 248 from W to R is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 2.09 Sequences represented at this position:86 Substitution at pos 351 from W to C is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 2.10 Sequences represented at this position:87 Substitution at pos 423 from A to D is predicted to AFFECT PROTEIN FUNCTION with a score of 0.01. Median sequence conservation: 2.10 Sequences represented at this position:85 Substitution at pos 482 from D to N is predicted to be TOLERATED with a score of 0.69. Median sequence conservation: 2.18 Sequences represented at this position:66 Substitution at pos 509 from L to P is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 2.10 Sequences represented at this position:79
The predicted results from SIFT is shown here:
Substitution at pos 83 from R to S is predicted to AFFECT PROTEIN FUNCTION with a score of 0.05. Median sequence conservation: 3.10 Sequences represented at this position:15 Substitution at pos 99 from H to R is predicted to be TOLERATED with a score of 0.74. Median sequence conservation: 3.11 Sequences represented at this position:14 Substitution at pos 150 from E to K is predicted to be TOLERATED with a score of 0.44. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 211 from V to I is predicted to be TOLERATED with a score of 1.00. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 236 from L to P is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 248 from W to R is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 351 from W to C is predicted to AFFECT PROTEIN FUNCTION with a score of 0.00. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 423 from A to D is predicted to AFFECT PROTEIN FUNCTION with a score of 0.01. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 482 from D to N is predicted to be TOLERATED with a score of 0.77. Median sequence conservation: 3.10 Sequences represented at this position:16 Substitution at pos 509 from L to P is predicted to AFFECT PROTEIN FUNCTION with a score of 0.01. Median sequence conservation: 3.11 Sequences represented at this position:14
Polyphen2
H99R This mutation is predicted to be benign with a score of 0.000 (sensitivity: 1.00; specificity: 0.00) This mutation is predicted to be benign with a score of 0.000 (sensitivity: 1.00; specificity: 0.00) V211I This mutation is predicted to be benign with a score of 0.000 (sensitivity: 1.00; specificity: 0.00) This mutation is predicted to be benign with a score of 0.001 (sensitivity: 0.99; specificity: 0.09) E150K This mutation is predicted to be benign with a score of 0.000 (sensitivity: 1.00; specificity: 0.00) This mutation is predicted to be benign with a score of 0.001 (sensitivity: 0.99; specificity: 0.09) L236P This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) W248R This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) This mutation is predicted to be probably damaging with a score of 0.999 (sensitivity: 0.09; specificity: 0.99) L509P This mutation is predicted to be probably damaging with a score of 0.992 (sensitivity: 0.70; specificity: 0.97) This mutation is predicted to be probably damaging with a score of 0.988 (sensitivity: 0.53; specificity: 0.95) W351C This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) A423D This mutation is predicted to be probably damaging with a score of 1.000 (sensitivity: 0.00; specificity: 1.00) This mutation is predicted to be probably damaging with a score of 0.996 (sensitivity: 0.36; specificity: 0.97) D482N This mutation is predicted to be benign with a score of 0.000 (sensitivity: 1.00; specificity: 0.00) his mutation is predicted to be benign with a score of 0.002 (sensitivity: 0.99; specificity: 0.18) R83S This mutation is predicted to be benign with a score of 0.007 (sensitivity: 0.96; specificity: 0.75) This mutation is predicted to be benign with a score of 0.019 (sensitivity: 0.95; specificity: 0.55)