Table 1 Peptide sequences of the validated NES motifs or false positives used in the structure-based modeling.

From: Structural prerequisites for CRM1-dependent nuclear export signaling peptides: accessibility, adapting conformation, and the stability at the binding site

Protein

Class

NES sequence

KD (nM)§

ref.

MVM NS2

1a

77STVDEMTKKFGTLTIHD93

2

31

*super PKI

1a

34NLNELALKLAGLDINK49

4

31

PKI

1a

34NSNELALKLAGLDINK49

34

31

ADAR1

1a

121RGVDCLSSHFQELSIYQ137

69

31

MEK1

1a

28TNLEALQKKLEELELDE44

70

31

Pax

1a

264RELDELMASLSDFKFMA280

700

31

*CPEB4-R

1a

395RMIDILSSELSHMDFTR379

710

31

NPMmutA

1a

278MTDQEAIQDLCLAVEEVSLRK298

790

31

HDAC5

1a

1081EAETVSAMALLSVG1095

1600

31

p73

1a

364NFEILMKLKESLELMELVP382

2000

31

*hRio2-R

1a

405GKIEELAQNFETMEFSR389

2600

31

Stradα

1a

413GIFGLVTNLEELEVD427

10300

31

*FMRP-1b

1b

YLKEVDQLRALERLQID

3000

14

SNUPN

1c

1MEELSQALASSFSVSQDLNS20

12500

31

HPV E7

1c

73HVDIRTLEDLLMGTLGIVC91

34000

31

HIV Rev

2

73LQLPPLERLTLDC85

1180

31

FMRP

2

424LKEVDQLRLERLQID438

2000

31

SMAD4

2

134ERVVSPGIDLSGLTLQ149

4600

31

mDia2

3

1157SVPEVEALLARLRAL1171

1600

31

CDC7

3

456QDLRKLCERLRGMDSSTP473

20000

31

X11L2

4

55SSLQELVQQFEALPGDLV72

1500

31

CPEB4

1a-R

379RTFDMHSLESSLIDIMR395

800

31

hRio2

1a-R

389RSFEMTEFNQALEEIKG405

2800

31

*PKImut1 (I47A)

34NSNELALKLAGLDANK49

150000

31

*PKImut2 (L42A/L45A)

34NSNELALKAAGADINK49

900000

31

APC

1a

163AQLQNLTKRIDSLPL174

(−)

33

Cyclin D1

1a

281VDLACTPTDVRDVDI295

(−)

APRIL

1b

106LEPLKKLECLKSLDL120

(−)

33

hTERT

1c

965KAGRNMRRKLFGVLRLKC982

(−)

DcpS

1c

136TEKHLQKYLRQDLRL150

(−)

33

Cdk5

2

133LINRNGELKLADFGL147

(−)

33

FGF1

2

138THYGQKAILFLPLPV152

(−)

33

COMMD1

3

171ILKTLSEVEESISTL185

(−)

20

DEAF1

1a-R

452SWLYLEEMVNSLLNTAQQ469

(−)

13

SGN5

1a-R

221YALEVSYFKSSLDRKLL238

(−)

13

COMMD1–2

1a-R

164DEVKVNQILKTLSEVEES181

(−)

13

ELF3

1a-R

111RLVFGPLGDQLHAQLR126

(−)

13

  1. *Engineered or mutated (underscored residues are the ones inserted or mutated).
  2. Do not fit the consensus in Fig. 1 (due to Pro or do not have a bulky residue at Φ3/4 in the class 1a-R).
  3. Unpublished data.
  4. §(−) means no binding determined by pull-down binding assay.
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