
The kappa chain primer is	[SEQ ID NO: 29]:
5′-CTAACACTCATTCCTGTTGAAGCTCTTGACAATGGG-3′
The gamma heavy chain primer is	[SEQ ID NO: 30]:
5′GTACATATGCAAGGCTTACAACCACAATC-3′.

The double stranded cDNA was cloned directly into plasmids pGEM7f+[Promega] that were then transformed into[0148]E. coliDH5-α[Bethesda Research Labs].

B. DNA Sequencing[0149]

Eight heavy and one light chain murine cDNA clones from Part A above were sequenced. The results of sequencing of the variable regions of these clones are shown in SEQ ID NO: 1 and 2 and 3 and 4. Each clone contained amino acids known to be conserved among mouse heavy chain variable regions or light chain variable regions, and murine signal sequences. The CDR amino acid sequences are listed below.[0150]

The CDR regions for the heavy chain are SEQ ID NO: 22, 24 and 26, (amino acids 50-56, 71-86 and 119-129 of SEQ ID NO: 4). See FIG. 2. These sequences are encoded by SEQ ID NO: 21, SEQ ID NO: 23, and SEQ ID NO: 25, respectively. The CDR regions for the light chain are SEQ ID NO: 16, 18 and 20 (amino acids 45-58, 74-80, and 113-121 of SEQ ID NO: 2). See FIG. 1. These sequences are encoded by SEQ ID NO: 15, 17, and 19, respectively.[0151]

C. Selection of Human Frameworks[0152]

Following the cloning of 3B9, the amino acid sequences of the variable region (amino acids 21-132 of SEQ ID NO: 2 and[0153]amino acids 20 to 140 of SEQ ID NO: 4) were compared with the human immunoglobulin sequence database using the KABAT® and the SWISS databases in order to identify a human framework for both the heavy and light chains which would most closely match the murine parent in sequence homology. In addition to these searches for sequence homology, the heavy and light chains were also evaluated against a positional database generated from structural models of the Fab domain to assess potential conflicts due to amino acid substitutions which might influence CDR presentation. For the present case, no obvious conflicts were detected in the structural search; hence, the DNA coding deduced from the amino acid sequence homology searches was used.

The heavy chain framework regions of an antibody obtained from a human myeloma immunoglobulin (COR) was used [E. M. Press and N. M. Hogg,[0154]Biochem. J.,117:641-660 (1970)]. This sequence was found to be approximately 77% homologous (69.4% identity) to the 3B9 variable chain region at the amino acid level.

For a suitable light chain variable framework region, the light chain variable framework sequence of the human antibody identified in H. G. Klobeck et al,[0155]Nucl. Acids Res.,13:6515-6529 (1985) was used. The human antibody sequence was found to be approximately 80.2% homologous (72.0% identity) to the murine 3B9 variable light chain region at the amino acid level.

Given the murine 3B9 CDRs [SEQ ID NO: 15-26] and the sequence of the human antibody, a synthetic heavy chain was made and PCR performed to fill in and amplify the DNA. These sequences were synthesized by the following overlapping oligonucleotides and amplified by PCR. SEQ ID NO: 31-37 provides five overlapping oligos and 2 PCR primers. Oligo 1 [SEQ ID NO: 31] is found spanning bases 5-121. Oligo 2 [SEQ ID NO: 32] is found spanning bases 122-241, and oligo 3 [SEQ ID NO: 33] is found spanning bases 242-361. The two bottom strand primers SEQ ID NO: 34 and SEQ ID NO: 35 span bases 134-110 and bases 253-230. Any errors in the mapped sequence which were inserted by PCR were corrected. PCR was again performed using as the 5′ primer nucleotides 1-25 SEQ ID NO: 36 and as the 3′ primer nucleotides 361-341 SEQ ID NO: 37.[0156]

The synthetic variable region was ligated into the expression vector pCD along with the synthetic signal sequence SEQ ID NO: 5 and 6 from the chimeric heavy chain construction along with an IgG[0157]₁human constant region. The synthetic V_Hand signal sequence nucleotide and amino acid sequences are provided in FIG. 4 [SEQ ID NOS: 11 and 12]. The amino acid sequences of the CDRs [SEQ ID NOS: 22, 24 and 26] are identical to the murine 3B9 CDRs. However, the coding sequences for these CDRs [SEQ ID NOS: 54, 55 and 56] differ from the murine 3B9 coding sequences [SEQ ID NOS: 21, 23 and 25]. The resulting expression vector, IL4hzhc1-l-Pcd is shown in FIG. 9.

The CDR gene regions of a pre-existing light chain framework were restriction digest removed and replaced with the following synthetic IL-4 CDR genes, which were synthetically made.[0158]


For CDR1:
SEQ ID NO: 38: 5′CTAGCTGTGTCTCTGGGCGAGAGGGCCACCATCAAC
TGCAAGG
3′
SEQ ID NO: 39: CCTTGCAGTTGATGGTGGCCCTCTCGCCCAGAGACACAG
SEQ ID NO: 40: TCGAGAGGCCTCCCAAAGTGTTGATTATGATGGTGATAG
TTATATGAACTGGTATCAGCAGAAACCC
SEQ ID NO: 41:
GGGTTTCTGCTGATACCAGTTCATATAACTATCACCATCATA
ATCAACACTTTGGGAGGCCTC
For CDR2:
SEQ ID NO: 44:
GGGCAGCCTCCTAAGTTGCTCATTTACGCTGCATCCAATCTA
GAATCTGGGGTAC
SEQ ID NO: 45:
CCCAGATTCTAGATTGGATGCAGCGTAAATGAGCAACTTAGG
AGGCTGCCC
For CDR3:
SEQ ID NO: 42:
ATACTACTGTCAGCAAAGTAATGAGGATCCTCCGAGGTTCGG
CGGAGGGAC
SEQ ID NO: 43:
CTTGGTCCCTCCGCCGAACCTCGGAGGATCCTCATTACTTTG
CTGACAGTAGT

The synthetic V[0159]_Land signal sequence nucleotide and amino acid sequences are provided in FIG. 5 [SEQ ID NOS: 13 and 14]. The amino acid sequences of the first two CDRs [SEQ ID NOS: 16 and 18] are identical to the corresponding murine 3B9 CDRs. However, the coding sequence for the first CDR [SEQ ID NO: 53] differs from the murine 3B9 coding sequence [SEQ ID NO: 15]. Further, in the last CDR, two humanized constructs of the 3B9 amino acid sequence were constructed. One, [SEQ ID NO: 28], differs by a single amino acid [SEQ ID NO: 20] from the native murine 3B9 sequence. SEQ ID NO: 28 is encoded by SEQ ID NO: 27. The synthetic variable light regions were ligated into the expression vector along with the signal sequence [SEQ ID NOS: 7 and 8]. One of the resulting expression vectors, IL4hzlc1-O-Pcn is illustrated in FIG. 10.

These synthetic variable light and/or heavy chain sequences are employed in the construction of a humanized antibody.[0160]

EXAMPLE 4

Expression of Humanized MAb in COS and CHO cells[0161]

pUC18 subclones for the V[0162]_Hwere made to add a signal sequence originally obtained from a human antibody SEQ ID NO: 5. For the V_L, pUC18 subclones were made to add a signal sequence SEQ ID NO: 7.

The humanized heavy chain, derived from an IgGl[0163]₁isotype, exhibits 89.3% homology (84.3% identity) at the amino acid level with the murine heavy chain from 3B9. This synthetic V_His provided in amino acids 20-141 of SEQ ID NOS: 11 and 12.

The humanized light chain, a human kappa chain, shows 92.0% homology (86.6% identity) with 3B9 at the amino acid level. This synthetic V[0164]_L[amino acids 21 to 131 of SEQ ID NOS: 13 and 14] containing the 3B9 CDRs was designed and synthesized as described above for the synthetic heavy chains.

The DNA fragments containing their respective signal linked to either the humanized heavy or light variable regions were inserted into pUC19-based mammalian cell expression plasmids containing CMV promoters and the human heavy chain or human light chain constant regions of the chimera produced in Example 5 below, by conventional methods [Maniatis et al., cited above] to yield the plasmids IL4hzhc1-lPcd (heavy chain) [FIG. 9] and IL4hzlc1-o-Pcn)(light chain) [FIG. 10]. The HZHC and HZLC plasmids are cotransfected into COS cells and supernatants assayed by the ELISA described immediately above for the presence of humanized antibody after three and five days. Another humanized antibody was constructed but with an IgG4 isotype.[0165]

The above example describes the preparation of an exemplary engineered antibody. Similar procedures may be followed for the development of other engineered antibodies, using other anti-IL4 antibodies (e.g., 6A1-Example 7) developed by conventional means.[0166]

EXAMPLE 5

Construction of Chimeric Antibody[0167]

A. A chimeric heavy chain was constructed by isolating the murine variable heavy chain region from the original mouse MAb 3B9 as an EcoRI-BstEII restriction fragment. A small DNA oligomer was designed and synthesized to link the mouse variable region with the human IgG1 constant region (BstEII-ApaI):[0168]


5′primer:	SEQ ID	GTCACCGTCTCCTCAGCTAGCACCAAGGGGC
	NO: 50:
3′primer:	SEQ ID	CTTGGTGCTAGCTGAGGAGACG
	NO: 51:

These two fragments were ligated into plasmid pCD (See FIG. 7)(digested with EcoRI and Apa1) that already encodes the human IgG1 constant region. This clone did not express; therefore, the wild-[0169]type 5′UTR and signal sequence were deleted and replaced with SEQ ID NO:5 and 6.

Because a convenient restriction endonuclease site was not available at the 3′ end of the signal sequence, a BstEII site was introduced (i.e., a silent mutation) via PCR. The following PCR primers were used:[0170]


SEQ ID NO: 48:	5′primer:	5′CAGGTTACCCTGAAAGAGTC 3′
SEQ ID NO: 49:	3′primer:	5′GAAGTAGTCCTTGACCAG 3′

A BstEII-PstI restriction fragment was then isolated from this plasmid. A new signal sequence and 5′UTR were then designed and synthesized having EcoRI and BstEII ends.[0171]


SEQ ID NO: 46:	5′primer:	AATTCGAGGACGCCAGCAACATGGT-
		GTTGCAGACCCAGGTCTTCATTTCT-
		CTGTTGCTCTGGACTCTGGTGCCTA-
		CGGGCAG
SEQ ID NO: 47:	3′primer:	GTAACCTGCCCGTAGGCACCAGAGA-
		TCCAGAGCAACAGAGAAATGAAGAC-
		CTGGGTCTGCAACACCATGTTGCTG-
		GCGTCCTCG

The chimeric light chain was constructed by applying the PCR technique to the original murine 3B9 light chain that was cloned into pGEM72f(+) [Promega]. The primers utilized were the commercially available pUC18 universal reverse primer at the 5′ end (EcoRI) and a 3′ primer that introduces a NarI site [5′CATCTAGATGGCG CCGCCACAGTACGTTTGATCTCCAGCTTGGTCCC3′ SEQ ID NO: 52], used to fuse the mouse variable region to the human constant region. This variable region was then ligated into the expression vector pCDN (EcoRI NarI) (FIG. 8) that already contains the human kappa region.[0172]

Media supernatants were collected three and five days later and assayed by the ELISA described as follows: ELISA plates were coated with 0.1 μg of a goat antibody specific for the Fc region of human antibodies. The media supernatants were added for one hour. A horseradish peroxidase conjugated goat antibody specific for an entire human IgG antibody was added. This was followed by addition of ABTS peroxidase substrate (Kirkegaard & Perry Laboratories Inc., Gaithersburg, Md.) for one hour. Expression of the chimeric antibody was detected. In a second ELISA the COS cell supernatants containing the chimeric antibody bound specifically to recombinant human IL4 protein. This result confirmed that genes coding for an antibody specific for IL4 had been cloned.[0173]

B. A humanized heavy chain can also be obtained from this chimeric heavy chain. The humanized heavy chain was designed from by inserting the murine CDRs into a human framework. The chosen human framework was as described above, the most homologous protein sequence in the Swiss protein data based to the murine 3B9 V[0174]_H(amino acids 20-140 of SEQ ID NO: 4). This humanized heavy chain sequence (EcoRI ApaI) was made synthetically and PCR performed to fill in and amplify DNA as described above. This synthetic variable region was ligated into the the expression vector pCD (EcoRI ApaI) together with the synthetic signal sequence SEQ ID NOS: 5 and 6 from the chimeric heavy chain construction and an IgG₁human constant region.

EXAMPLE 6

Purification and Thermodynamics—Humanized MAb[0176]

Purification of CHO expressed chimeric and humanized 3B9 can be achieved by conventional protein A (or G) affinity chromatography followed by ion exchange and molecular sieve chromatography. Similar processes have been successfully employed for the purification to >95% purity of other MAbs (e.g., to respiratory syncytial virus and malaria circumsporozoite antigens).[0177]

The affinity and detailed thermodynamics of IL4 binding to humanized MAb 3B9 and murine 3B9 (Example 1) were determined by titration microcalorimetry. This method measures binding reactions by virtue of their intrisic heats of reaction (see, e.g., Wiseman et al.,[0178]Anal. Biochem,179:131-137 (1989). The affinity of both MAbs was found to be too tight to measure directly at ambient temperature. Thus, a thermodynamic approach was taken: i) the affinity was measured at 60° C., where it is weak enough to be measured directly; and (ii) the temperature-dependence of the binding enthalpy was measured from 30-60° C. Together, these data allow calculation of the affinity over a wide range of temperautes using the Gibbs-Helmholz equation.

A summary of the IL4 binding thermodynamics of the humanized and murine 3B9 antibodies are presented in Table 1. Based upon the changes in free energy, enthalpy, entropy and heat capacity of the two MAbs, the binding thermodymanics are indistinguishable.[0179]

TABLE 1


Thermodynamics of hIL-4 binding to Humanzied 3B9 and Murine 3B9 at
pH 7.4, 150 mM NaCl, and 25° C..

		ΔG	ΔH	−TΔS	ΔC
	K_d	kcal/	kcal/	kcal/	cal/mol
mAB	picomolar	mol IL4	mol IL4	mol IL4	IL4/° K.

human-	11	−13.6 ± 0.6	−21.8 ± 2	8.2 ± 2.1	−580 ± 160
ized
3B9
murine	19	−13.3 ± 0.6	−20.5 ± 1	7.2 ± 1.2	−660 ± 200
3B9

EXAMPLE 7

Production and Characterization of Rat MAb[0180]

MAb 6A1, chosen for high affinity binding, was derived from an immunized rat, using the same immunization protocol as described for the mouse in Example 1. 6A1 was selected from hybridomas (specifically, hybridoma 3426A11C1B9) prepared from rats immunized with human IL4.[0181]

The K[0182]_dfor 6A1 was calculated as described in Beatty et alJ. Immunol. Methods,100:173-179 (1987) to be 2×10⁻¹⁰M.

Hybridoma 3426A11C1B9 was deposited Oct. 6, 1993 with the European Collection of Animal Cell Cultures (ECACC), Public Health Laboratory Service Centre for Applied Microbiology & Research, Porton Down, Salisbury, Wiltshire, SP4 0JG, United Kingdom, under accession number 93100620, and has been accepted as a patent deposit, in accordance with the Budapest Treaty of 1977 governing the deposit of microorganisms for the purposes of patent procedure.[0183]

EXAMPLE 8

Biological Activity of MAbs: 3B9 (humanized), 3B9 (Murine) and 6A1[0184]

The following assays were performed using the procedures described below.[0185]

A. Binding to Glycosylated rhIL4[0186]

The above-identified antibodies were raised to non-glycosylated recombinant human IL4 (rhIL4) which was produced in[0187]E. coli.Because native human IL4 is glycosylated, it was important to confirm binding to material secreted by a mammalian cell line. 3B9 binds equally well to both glycosylated and non-glycosylated human recombinant IL4, and is not therefore directed to an epitope that would be masked on natural human IL4.

B. Inhibition of IL4 Binding to Receptor[0188]

The ability of 3B9 to inhibit the binding of IL4 to its receptor was studied using[0189]¹²⁵I-rhIL4 binding to the gibbon cell line, MLA [ATCC TIB201], that bears approximately 6000 receptors per cell, MLA cells were incubated with¹²⁵I-IL4 for 30 minutes at 37° C. Uptake of radioactivity was determined in a gamma counter after separation of cell bound¹²⁵I-IL4 by centrifugation through an oil-gradient. Non-sic binding was determined by incubating in the presence of a 100-fold molar excess of unlabelled IL4 [Park et al,J. Exp. Med.,166:476-488 (1987)]. The IC₅₀value for unlabeled IL4 in this assay was 22 pM when the amount of (added) IL4 was 83 pM. For intact murine (IgG) 3B9 the IC₅₀was 63 pM, and 93 pM for the Fab fragment. At another concentration of IL4 (218 pM), the assay amount for murine (IgG) 3B9 was 109 pM.

C. Inhibition of Lymphocyte Proliferation[0190]

Using the method described in Spits et al,[0191]J. Immunol.,139:1142-1147 (1987), human peripheral blood lymphocytes are incubated for three days with phytohemagglutinin, a T cell mitogen, to upregulate the IL4 receptor. The resultant blast cells are then stimulated for three days further with IL4. Proliferation is measured by the incorporation of³H thymidine. B cell proliferation was measured by the assay of Callard et al, inLymphokines and Interferons, A Practical Approach,Ch. 19, p. 345, modified as follows. Purified human tonsillar B cells are stimulated for 3 days with IL4 and immobilized anti-IgM. Proliferation is measured by the incorporation of³H thymidine.

3B9 (murine) inhibited[0192]³H-thymidine incorporation by human peripheral blood T lymphocytes stimulated with 133 pM IL4 and human tonsillar B lymphocytes stimulated by 167 pM IL4. IL2-stimulated T lymphocytes were not affected. The IC₅₀for inhibition of T cell proliferation was 30 pM, and for B cell proliferation 103 pM. The corresponding values for the Fab fragment of 3B9 (murine) were 108 and 393 pM.

D. Inhibition of CD23 Induction[0193]

CD23 is the low affinity receptor for IgE (FcERII) and is induced on the membrane of resting B lymphocytes by low concentrations of IL4 as a necessary prerequisite for IgE production. Purified human tonsillar B cells are stimulated for 2 days with IL4. The percentage of cells expressing the CD23 receptor are determined by flow cytometry [Defrance et al,[0194]J. Exp. Med.,165:1459-1467 (1987)]. 3B9 (murine) inhibited CD23 expression on human tonsil B lymphocytes stimulated with 8.3 pM IL4 with an IC₅₀value of 136 pM.

E. Inhibition of IgE Secretion[0195]

Unlike other assays where IL4 was added at EC[0196]₅₀concentrations [Pere et al,Proc. Natl. Acad. Sci.,85:6880-6884 (1989)], IgE secretion was investigated in the presence of concentrations of IL4 giving maximal secretion in order to reduce the variability inherent in this system. T cell proliferation was measured as follows. Human peripheral blood lymphocytes are incubated with IL4 for between 10-18, preferably 12, days. The concentration of IgE in the culture supernatant is determined by ELISA.

IgE secretion was inhibited by 3B9 (murine), and the Fab fragment of 3B9, in the presence of 1.7 nM IL4 giving IC[0197]₅₀values of 1.9 and 5.0 nM respectively. The experiment was repeated using a lower concentration of IL4, 667 pM, which reduced the IC₅₀value to 0.65 nM for 3B9 (murine). The molar ratio of antibody (IgG) to IL4 remained unchanged (1:1) over the concentration ranges examined.

F. Summary and Interpretation of Data[0198]

The molar ratios of IL4 to various MAbs required for 50% inhibition of function in bioassays is given in Table 2.[0199]

TABLE 2


Comparative activity of mAbs 3B9, 6A1 and Humanized 3B9
[IgG1 and IgG4 variants] in IL-4 dependent bioassays

IC50 (pM) [range]_n

		Murine		Humanized
	Murine	3B9		3B9
Assay	3B9	(Fab)	Rat 6A1	IgG1	IgG4*

RBA	63	93	>50000
	[17-109]₂
T cell	30	108	87	44 [30-56]₃	40
	[10-40]₄
B cell	103	393	187	47 [10-80]₃	79
	[79-120]₃
CD23	136	216	80	333
induc-	[53-272]₄
tion
IgE	658	1170	623 [412-833]₂	54 [35-83]₃	406
synthe-	[370-1070]₆
sis

In all assays, except IgE secretion, IL4 was added at approximate ED[0200]₅₀concentrations. The molar ratios of antibody to IL-4 required for 50% inhibition were similar for humanized 3B9, murine 3B9, and 6A1 in the two lymphocyte proliferation assays, but higher for humanized 3B9 in the CD23 induction assay. The latter is a particularly sensitive assay apparently requiring very low (˜5%) receptor occupancy (Kruse et al.,EMBO J,12:5121 1993) and, as is evident from the results obtained with murine 3B9, subject to inter assay variation.

A comparison of the activities of rat 6A1 and murine 3B9 demonstrated a similar profile of functional effects, but an unexpected failure of 6A1 to fully inhibit the binding of radioiodinated IL4 to its receptor. The radioiodinated IL4 used in the receptor binding assay is thought to be iodinated at the accessible tyrosine, residue 124. When the ability of 6A1 to inhibit CD23 expression induced by either unlabelled or iodinated IL4 was compared, it was found that inhibition was less efficient against iodinated ligand. These results indicate that 6A1 binds to IL4 in the region of, but not specifically to, tyrosine 124.[0201]

Thus on current data, 6A1 is a neutralizing antibody of high affinity, binding to a very different region of IL4 than 3B9.[0202]

EXAMPLE 9

Pharmacokinetics[0203]

The pharmacokinetics of humanized 3B9 was investigated in the male Sprague Dawley rat. Humanized 3B9 was administered to four animals as an iv bolus dose at 1 mg/kg, blood sampling was continued for 5 weeks post dosing. Plasma humanized 3B9 concentrations were determined using an IL4/anti-human IgG sandwich ELISA designed to confirm not only the presence of circulating human IgG but also its ability to bind to recombinant human IL4.[0204]

Results from this study are summarized in Table 3.[0205]

TABLE 3


Pharmacokinetics of Humanized 3B9 in male Sprague-Dawley Rats
(dose: 1 mg/kg iv bolus)

	Clp
	(mL/h/kg)

	Rat 1	0.442
	Rat 2	0.655
	Rat 3	0.555
	Rat 4	0.447
	Mean	0.525
	SD	0.101

Data indicated that inter-animal variability was relatively small and disappearance of humanized 3B9 from plasma appeared to be biphasic. The apparent plasma clearance was low (0.5 mL/h/kg). The half-life appeared to be 11 days. Thus, the pharmacokinetic characteristics of the CHO cell-derived humanized 3B9 are consistent with other humanized monoclonal antibodies in rats. The long circulating half life of humanized 3B9 in the rat also suggests that when administered to man, humanized 3B9 is likely to be effective over an extended period of time.[0206]

Numerous modifications and variations of the present invention are included in the above-identified specification and are expected to be obvious to one of skill in the art. For example, human framework legions or modifications thereof, other than the exemplary antibodies described above, may be used in the construction of humanized antibodies. Such modifications and alterations to the compositions and processes of the present invention are believed to be encompassed in the scope of the claims appended hereto.[0207]

1 ATG GAG ACA GAC ACA ATC CTG CTA TGG GTG CTG CTG CTC TGG GTT CCA 48 Met Glu Thr Asp Thr Ile Leu Leu Trp Val Leu Leu Leu Trp Val Pro 1 5 10 15 GGC TCC ACT GGT GAC ATT GTG CTG ACC CAA TCT CCA GCT TCT TTG GCT 96 Gly Ser Thr Gly Asp Ile Val Leu Thr Gln Ser Pro Ala Ser Leu Ala 20 25 30 GTG TCT CTA GGG CAG AGG GCC ACC ATC TCC TGC AAG GCC AGC CAA AGT 144 Val Ser Leu Gly Gln Arg Ala Thr Ile Ser Cys Lys Ala Ser Gln Ser 35 40 45 GTT GAT TAT GAT GGT GAT AGT TAT ATG AAC TGG TAC CAA CAG AAA CCA 192 Val Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro 50 55 60 GGA CAG CCA CCC AAA CTC CTC ATC TAT GCT GCA TCC AAT CTA GAA TCT 240 Gly Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser 65 70 75 80 GGG ATC CCA GCC AGG TTT AGT GGC AGT GGG TCT GGG ACA GAC TTC ACC 288 Gly Ile Pro Ala Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr 85 90 95 CTC AAC ATC CAT CCT GTG GAG GAG GAG GAT GCT GCA ACC TAT TAC TGT 336 Leu Asn Ile His Pro Val Glu Glu Glu Asp Ala Ala Thr Tyr Tyr Cys 100 105 110 CAG CAA AGT AAT GAG GAT CCT CCG ACG TTC GGT GGA GGC ACC AAG CTG 384 Gln Gln Ser Asn Glu Asp Pro Pro Thr Phe Gly Gly Gly Thr Lys Leu 115 120 125 GAA ATC AAA CGG 396 Glu Ile Lys Arg 130

2 Met Glu Thr Asp Thr Ile Leu Leu Trp Val Leu Leu Leu Trp Val Pro 1 5 10 15 Gly Ser Thr Gly Asp Ile Val Leu Thr Gln Ser Pro Ala Ser Leu Ala 20 25 30 Val Ser Leu Gly Gln Arg Ala Thr Ile Ser Cys Lys Ala Ser Gln Ser 35 40 45 Val Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro 50 55 60 Gly Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser 65 70 75 80 Gly Ile Pro Ala Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr 85 90 95 Leu Asn Ile His Pro Val Glu Glu Glu Asp Ala Ala Thr Tyr Tyr Cys 100 105 110 Gln Gln Ser Asn Glu Asp Pro Pro Thr Phe Gly Gly Gly Thr Lys Leu 115 120 125 Glu Ile Lys Arg 130

3 GAATTCGCGG CCGCTATGCA GGGACAATCA GCAGCAGCAA TGAGGAAGTA AGCCTGTGCA 60 GAT ATG AAC AGG CTT ACT TCC TCA TTG CTG CTG CTG ATT GTC CCT GCA 108 Met Asn Arg Leu Thr Ser Ser Leu Leu Leu Leu Ile Val Pro Ala 1 5 10 15 TAT GTC CTG TCC CAG GTT ACT CTG AAA GAG TCT GGC CCT GGG ATA TTG 156 Tyr Val Leu Ser Gln Val Thr Leu Lys Glu Ser Gly Pro Gly Ile Leu 20 25 30 CAG CCC TCC CAG ACC CTC AGT CTG ACT TGT TCT TTC TCT GGG TTT TCA 204 Gln Pro Ser Gln Thr Leu Ser Leu Thr Cys Ser Phe Ser Gly Phe Ser 35 40 45 CTG AGC ACT TCT GGT ATG GGT GTG AGC TGG ATT CGT CAG CCT TCA GGA 252 Leu Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Ser Gly 50 55 60 AAG GGT CTG GAG TGG CTG GCA CAC ATT TAC TGG GAT GAT GAC AAG CGC 300 Lys Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg 65 70 75 TAT AAC CCA TCC CTG AAG AGC CGG CTC ACA ATC TCC AAG GAT ACC TCC 348 Tyr Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser 80 85 90 95 AGC AAC CAG GTA TTC CTC AAG ATC ACC AGT GTG GAC ACT GCA GAT ACT 396 Ser Asn Gln Val Phe Leu Lys Ile Thr Ser Val Asp Thr Ala Asp Thr 100 105 110 GCC ACA TAC TAC TGT GCT CGA AGA GAG ACT GTG TTC TAC TGG TAC TTC 444 Ala Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe 115 120 125 GAT GTC TGG GGC GCA GGG ACC ACG GTC ACC GTC TCC TCA 483 Asp Val Trp Gly Ala Gly Thr Thr Val Thr Val Ser Ser 130 135 140

4 Met Asn Arg Leu Thr Ser Ser Leu Leu Leu Leu Ile Val Pro Ala Tyr 1 5 10 15 Val Leu Ser Gln Val Thr Leu Lys Glu Ser Gly Pro Gly Ile Leu Gln 20 25 30 Pro Ser Gln Thr Leu Ser Leu Thr Cys Ser Phe Ser Gly Phe Ser Leu 35 40 45 Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Ser Gly Lys 50 55 60 Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg Tyr 65 70 75 80 Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser Ser 85 90 95 Asn Gln Val Phe Leu Lys Ile Thr Ser Val Asp Thr Ala Asp Thr Ala 100 105 110 Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe Asp 115 120 125 Val Trp Gly Ala Gly Thr Thr Val Thr Val Ser Ser 130 135 140

5 ATG GTG TTG CAG ACC CAG GTC TTC ATT TCT CTG TTG CTC TGG ATC TCT 48 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 GGT GCC TAC GGG 60 Gly Ala Tyr Gly 20

6 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 Gly Ala Tyr Gly 20

7 ATG GGA TGG AGC TGT ATC ATC CTC TTC TTG GTA GCA ACA GCT ACA GGT 48 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 GTC CAC TCC 57 Val His Ser

8 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 Val His Ser

9 ATG GTG TTG CAG ACC CAG GTC TTC ATT TCT CTG TTG CTC TGG ATC TCT 48 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 GGT GCC TAC GGG CAG GTT ACC CTG AAA GAG TCT GGC CCT GGG ATA TTG 96 Gly Ala Tyr Gly Gln Val Thr Leu Lys Glu Ser Gly Pro Gly Ile Leu 20 25 30 CAG CCC TCC CAG ACC CTC AGT CTG ACT TGT TCT TTC TCT GGG TTT TCA 144 Gln Pro Ser Gln Thr Leu Ser Leu Thr Cys Ser Phe Ser Gly Phe Ser 35 40 45 CTG AGC ACT TCT GGT ATG GGT GTG AGC TGG ATT CGT CAG CCT TCA GGA 192 Leu Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Ser Gly 50 55 60 AAG GGT CTG GAG TGG CTG GCA CAC ATT TAC TGG GAT GAT GAC AAG CGC 240 Lys Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg 65 70 75 80 TAT AAC CCA TCC CTG AAG AGC CGG CTC ACA ATC TCC AAG GAT ACC TCC 288 Tyr Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser 85 90 95 AGC AAC CAG GTA TTC CTC AAG ATC ACC AGT GTG GAC ACT GCA GAT ACT 336 Ser Asn Gln Val Phe Leu Lys Ile Thr Ser Val Asp Thr Ala Asp Thr 100 105 110 GCC ACA TAC TAC TGT GCT CGA AGA GAG ACT GTG TTC TAC TGG TAC TTC 384 Ala Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe 115 120 125 GAT GTC TGG GGC GCA GGG ACC ACG GTC ACC GTC TCC TCA 423 Asp Val Trp Gly Ala Gly Thr Thr Val Thr Val Ser Ser 130 135 140

10 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 Gly Ala Tyr Gly Gln Val Thr Leu Lys Glu Ser Gly Pro Gly Ile Leu 20 25 30 Gln Pro Ser Gln Thr Leu Ser Leu Thr Cys Ser Phe Ser Gly Phe Ser 35 40 45 Leu Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Ser Gly 50 55 60 Lys Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg 65 70 75 80 Tyr Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser 85 90 95 Ser Asn Gln Val Phe Leu Lys Ile Thr Ser Val Asp Thr Ala Asp Thr 100 105 110 Ala Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe 115 120 125 Asp Val Trp Gly Ala Gly Thr Thr Val Thr Val Ser Ser 130 135 140

11 ATG GTG TTG CAG ACC CAG GTC TTC ATT TCT CTG TTG CTC TGG ATC TCT 48 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 GGT GCC TAC GGG CAG GTT ACC CTG CGT GAA TCC GGT CCG GCA CTA GTT 96 Gly Ala Tyr Gly Gln Val Thr Leu Arg Glu Ser Gly Pro Ala Leu Val 20 25 30 AAA CCG ACC CAG ACC CTG ACG TTA ACC TGC ACC TTC TCC GGT TTC TCC 144 Lys Pro Thr Gln Thr Leu Thr Leu Thr Cys Thr Phe Ser Gly Phe Ser 35 40 45 CTG TCG ACC TCC GGT ATG GGT GTT TCC TGG ATC CGT CAG CCG CCG GGT 192 Leu Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Pro Gly 50 55 60 AAA GGT CTA GAA TGG CTG GCT CAC ATC TAC TGG GAC GAC GAC AAA CGT 240 Lys Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg 65 70 75 80 TAC AAC CCG AGC CTG AAA TCC CGT CTG ACG ATA TCC AAA GAC ACC TCC 288 Tyr Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser 85 90 95 CGT AAC CAG GTT GTT CTG ACC ATG ACT AAC ATG GAC CCG GTT GAC ACC 336 Arg Asn Gln Val Val Leu Thr Met Thr Asn Met Asp Pro Val Asp Thr 100 105 110 GCT ACC TAC TAC TGC GCT CGA CGC GAA ACC GTT TTC TAC TGG TAC TTC 384 Ala Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe 115 120 125 GAC GTT TGG GGT CGT GGT ACC CCA GTT ACC GTG AGC TCA 423 Asp Val Trp Gly Arg Gly Thr Pro Val Thr Val Ser Ser 130 135 140

12 Met Val Leu Gln Thr Gln Val Phe Ile Ser Leu Leu Leu Trp Ile Ser 1 5 10 15 Gly Ala Tyr Gly Gln Val Thr Leu Arg Glu Ser Gly Pro Ala Leu Val 20 25 30 Lys Pro Thr Gln Thr Leu Thr Leu Thr Cys Thr Phe Ser Gly Phe Ser 35 40 45 Leu Ser Thr Ser Gly Met Gly Val Ser Trp Ile Arg Gln Pro Pro Gly 50 55 60 Lys Gly Leu Glu Trp Leu Ala His Ile Tyr Trp Asp Asp Asp Lys Arg 65 70 75 80 Tyr Asn Pro Ser Leu Lys Ser Arg Leu Thr Ile Ser Lys Asp Thr Ser 85 90 95 Arg Asn Gln Val Val Leu Thr Met Thr Asn Met Asp Pro Val Asp Thr 100 105 110 Ala Thr Tyr Tyr Cys Ala Arg Arg Glu Thr Val Phe Tyr Trp Tyr Phe 115 120 125 Asp Val Trp Gly Arg Gly Thr Pro Val Thr Val Ser Ser 130 135 140

13 ATG GGA TGG AGC TGT ATC ATC CTC TTC TTG GTA GCA ACA GCT ACA GGT 48 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 GTC CAC TCC GAT ATC GTG ATG ACC CAG TCT CCA GAC TCG CTA GCT GTG 96 Val His Ser Asp Ile Val Met Thr Gln Ser Pro Asp Ser Leu Ala Val 20 25 30 TCT CTG GGC GAG AGG GCC ACC ATC AAC TGC AAG GCC TCC CAA AGT GTT 144 Ser Leu Gly Glu Arg Ala Thr Ile Asn Cys Lys Ala Ser Gln Ser Val 35 40 45 GAT TAT GAT GGT GAT AGT TAT ATG AAC TGG TAT CAG CAG AAA CCC GGG 192 Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro Gly 50 55 60 CAG CCT CCT AAG TTG CTC ATT TAC GCT GCA TCC AAT CTA GAA TCT GGG 240 Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser Gly 65 70 75 80 GTA CCT GAC CGA TTC AGT GGC AGC GGG TCT GGG ACA GAT TTC ACT CTC 288 Val Pro Asp Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr Leu 85 90 95 ACC ATC AGC AGC CTG CAG GCT GAA GAT GTG GCA GTA TAC TAC TGT CAG 336 Thr Ile Ser Ser Leu Gln Ala Glu Asp Val Ala Val Tyr Tyr Cys Gln 100 105 110 CAA AGT AAT GAG GAT CCT CCG AGG TTC GGC GGA GGG ACC AAG GTG GAG 384 Gln Ser Asn Glu Asp Pro Pro Arg Phe Gly Gly Gly Thr Lys Val Glu 115 120 125 ATC AAA CGT 393 Ile Lys Arg 130

14 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 Val His Ser Asp Ile Val Met Thr Gln Ser Pro Asp Ser Leu Ala Val 20 25 30 Ser Leu Gly Glu Arg Ala Thr Ile Asn Cys Lys Ala Ser Gln Ser Val 35 40 45 Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro Gly 50 55 60 Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser Gly 65 70 75 80 Val Pro Asp Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr Leu 85 90 95 Thr Ile Ser Ser Leu Gln Ala Glu Asp Val Ala Val Tyr Tyr Cys Gln 100 105 110 Gln Ser Asn Glu Asp Pro Pro Arg Phe Gly Gly Gly Thr Lys Val Glu 115 120 125 Ile Lys Arg 130

15 AAG GCC AGC CAA AGT GTT GAT TAT GAT GGT GAT AGT TAT ATG AAC 45 Lys Ala Ser Gln Ser Val Asp Tyr Asp Gly Asp Ser Tyr Met Asn 1 5 10 15

16 Lys Ala Ser Gln Ser Val Asp Tyr Asp Gly Asp Ser Tyr Met Asn 1 5 10 15

17 GCT GCA TCC AAT CTA GAA TCT 21 Ala Ala Ser Asn Leu Glu Ser 1 5

18 Ala Ala Ser Asn Leu Glu Ser 1 5

19 CAG CAA AGT AAT GAG GAT CCT CCG ACG 27 Gln Gln Ser Asn Glu Asp Pro Pro Thr 1 5

20 Gln Gln Ser Asn Glu Asp Pro Pro Thr 1 5

21 ACT TCT GGT ATG GGT GTG AGC 21 Thr Ser Gly Met Gly Val Ser 1 5

22 Thr Ser Gly Met Gly Val Ser 1 5

23 CAC ATT TAC TGG GAT GAT GAC AAG CGC TAT AAC CCA TCC CTG AAG AGC 48 His Ile Tyr Trp Asp Asp Asp Lys Arg Tyr Asn Pro Ser Leu Lys Ser 1 5 10 15

24 His Ile Tyr Trp Asp Asp Asp Lys Arg Tyr Asn Pro Ser Leu Lys Ser 1 5 10 15

25 AGA GAG ACT GTG TTC TAC TGG TAC TTC GAT GTC 33 Arg Glu Thr Val Phe Tyr Trp Tyr Phe Asp Val 1 5 10

26 Arg Glu Thr Val Phe Tyr Trp Tyr Phe Asp Val 1 5 10

27 CAG CAA AGT AAT GAG GAT CCT CCG AGG 27 Gln Gln Ser Asn Glu Asp Pro Pro Arg 1 5

28 Gln Gln Ser Asn Glu Asp Pro Pro Arg 1 5

29 CTAACACTCA TTCCTGTTGA AGCTCTTGAC AATGGG 36

30 GTACATATGC AAGGCTTACA ACCACAATC 29

31 GGTTACCCTG CGTGAATCCG GTCCGGCACT AGTTAAACCG ACCCAGACCC TGACGTTAAC 60 CTGCACCTTC TCCGGTTTCT CCCTGTCGAC CTCCGGTATG GGTGTTTCCT GGATCCG 117

32 TCAGCCGCCG GGTAAAGGTC TAGAATGGCT GGCTCACATC TACTGGGACG ACGACAAACG 60 TTACAACCCG AGCCTGAAAT CCCGTCTGAC GATATCCAAA GACACCTCCC GTAACCAGG 120

33 TGTTCTGACC ATGGACCCGG TTGACACCGC TACCTACTAC TGCGCTCGTC GCGAAACCGT 60 TTTCTACTGG TACTTCGACG TTTGGGGTCG TGGTACCCCA GTTACCGTGA GCTCCCAAC 120

34 ACCCGGCGGC TGACGGATCC AGGAA 25

35 ATGGTCAGAA CAACCTGGTT ACGG 24

36 TTCGGGTTAC CCTGCGTGAA TCCGG 25

37 CCAACCCTCG AGTGCCATTG A 21

38 CTAGCTGTGT CTCTGGGCGA GAGGGCCACC ATCAACTGCA AGG 43

39 CCTTGCAGTT GATGGTGGCC CTCTCGCCCA GAGACACAG 39

40 TCGAGAGGCC TCCCAAAGTG TTGATTATGA TGGTGATAGT TATATGAACT GGTATCAGCA 60 GAAACCC 67

41 GGGTTTCTGC TGATACCAGT TCATATAACT ATCACCATCA TAATCAACAC TTTGGGAGGC 60 CTC 63

42 ATACTACTGT CAGCAAAGTA ATGAGGATCC TCCGAGGTTC GGCGGAGGGA C 51

43 CTTGGTCCCT CCGCCGAACC TCGGAGGATC CTCATTACTT TGCTGACAGT AGT 53

44 GGGCAGCCTC CTAAGTTGCT CATTTACGCT GCATCCAATC TAGAATCTGG GGTAC 55

45 CCCAGATTCT AGATTGGATG CAGCGTAAAT GAGCAACTTA GGAGGCTGCC C 51

46 AATTCGAGGA CGCCAGCAAC ATGGTGTTGC AGACCCAGGT CTTCATTTCT CTGTTGCTCT 60 GGATCTCTGG TGCCTACGGG CAG 83

47 GTAACCTGCC CGTAGGCACC AGAGATCCAG AGCAACAGAG AAATGAAGAC CTGGGTCTGC 60 AACACCATGT TGCTGGCGTC CTCG 84

48 CAGGTTACCC TGAAAGAGTC 20

49 GAAGTAGTCC TTGACCAG 18

50 GTCACCGTCT CCTCAGCTAG CACCAAGGGG C 31

51 CTTGGTGCTA GCTGAGGAGA CG 22

52 CATCTAGATG GCGCCGCCAC AGTACGTTTG ATCTCCAGCT TGGTCCC 47

53 AAGGCCTCCC AAAGTGTTGA TTATGATGGT GATAGTTATA TGAAC 45

54 ACCTCCGGTA TGGGTGTTTC C 21

55 CACATCTACT GGGACGACGA CAAACGTTAC AACCCGAGCC TGAAATCC 48

56 CGCGAAACCG TTTTCTACTG GTACTTCGAC GTT 33

57 ATG GGA TGG AGC TGT ATC ATC CTC TTC TTG GTA GCA ACA GCT ACA GGT 48 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 GTC CAC TCC GAT ATC GTG ATG ACC CAG TCT CCA GAC TCG CTA GCT GTG 96 Val His Ser Asp Ile Val Met Thr Gln Ser Pro Asp Ser Leu Ala Val 20 25 30 TCT CTG GGC GAG AGG GCC ACC ATC AAC TGC AAG GCC TCC CAA AGT GTT 144 Ser Leu Gly Glu Arg Ala Thr Ile Asn Cys Lys Ala Ser Gln Ser Val 35 40 45 GAT TAT GAT GGT GAT AGT TAT ATG AAC TGG TAT CAG CAG AAA CCC GGG 192 Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro Gly 50 55 60 CAG CCT CCT AAG TTG CTC ATT TAC GCT GCA TCC AAT CTA GAA TCT GGG 240 Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser Gly 65 70 75 80 GTA CCT GAC CGA TTC AGT GGC AGC GGG TCT GGG ACA GAT TTC ACT CTC 288 Val Pro Asp Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr Leu 85 90 95 ACC ATC AGC AGC CTG CAG GCT GAA GAT GTG GCA GTA TAC TAC TGT CAG 336 Thr Ile Ser Ser Leu Gln Ala Glu Asp Val Ala Val Tyr Tyr Cys Gln 100 105 110 CAA AGT AAT GAG GAT CCT CCG ACG TTC GGC GGA GGG ACC AAA GTG GAG 384 Gln Ser Asn Glu Asp Pro Pro Thr Phe Gly Gly Gly Thr Lys Val Glu 115 120 125 ATC AAA CGT 393 Ile Lys Arg 130

58 Met Gly Trp Ser Cys Ile Ile Leu Phe Leu Val Ala Thr Ala Thr Gly 1 5 10 15 Val His Ser Asp Ile Val Met Thr Gln Ser Pro Asp Ser Leu Ala Val 20 25 30 Ser Leu Gly Glu Arg Ala Thr Ile Asn Cys Lys Ala Ser Gln Ser Val 35 40 45 Asp Tyr Asp Gly Asp Ser Tyr Met Asn Trp Tyr Gln Gln Lys Pro Gly 50 55 60 Gln Pro Pro Lys Leu Leu Ile Tyr Ala Ala Ser Asn Leu Glu Ser Gly 65 70 75 80 Val Pro Asp Arg Phe Ser Gly Ser Gly Ser Gly Thr Asp Phe Thr Leu 85 90 95 Thr Ile Ser Ser Leu Gln Ala Glu Asp Val Ala Val Tyr Tyr Cys Gln 100 105 110 Gln Ser Asn Glu Asp Pro Pro Thr Phe Gly Gly Gly Thr Lys Val Glu 115 120 125 Ile Lys Arg 130