structural communications\(\def\hfill{\hskip 5em}\def\hfil{\hskip 3em}\def\eqno#1{\hfil {#1}}\)

Journal logoSTRUCTURAL BIOLOGY
COMMUNICATIONS
ISSN: 2053-230X
Volume 70| Part 9| September 2014| Pages 1127-1131

Chemical conversion of cisplatin and carboplatin with histidine in a model protein crystallized under sodium iodide conditions

CROSSMARK_Color_square_no_text.svg

aSchool of Chemistry, Faculty of Engineering and Physical Sciences, University of Manchester, Brunswick Street, Manchester M13 9PL, England
*Correspondence e-mail: john.helliwell@manchester.ac.uk

(Received 2 April 2014; accepted 14 June 2014; online 29 August 2014)

Cisplatin and carboplatin are platinum anticancer agents that are used to treat a variety of cancers. Previous X-ray crystallographic studies of carboplatin binding to histidine in hen egg-white lysozyme (HEWL) showed a partial chemical conversion of carboplatin to cisplatin owing to the high sodium chloride concentration used in the crystallization conditions. Also, the co-crystallization of HEWL with carboplatin in sodium bromide conditions resulted in the partial conversion of carboplatin to the transbromoplatin form, with a portion of the cyclobutanedicarboxylate (CBDC) moiety still present. The results of the co-crystallization of HEWL with cisplatin or carboplatin in sodium iodide conditions are now reported in order to determine whether the cisplatin and carboplatin converted to the iodo form, and whether this took place in a similar way to the partial conversion of carboplatin to cisplatin in NaCl conditions or to transbromoplatin in NaBr conditions as seen previously. It is reported here that a partial chemical transformation has taken place to a transplatin form for both ligands. The NaI-grown crystals belonged to the monoclinic space group P21 with two molecules in the asymmetric unit. The chemically transformed cisplatin and carboplatin bind to both His15 residues, i.e. in each asymmetric unit. The binding is only at the Nδ atom of His15. A third platinum species is also seen in both conditions bound in a crevice between symmetry-related molecules. Here, the platinum is bound to three I atoms identified based on their anomalous difference electron densities and their refined occupancies, with the fourth bound atom being a Cl atom (in the cisplatin case) or a portion of the CBDC moiety (in the carboplatin case).

1. Introduction

Cisplatin and carboplatin are platinum anticancer drugs that have long been used as cytostatics (https://www.cancerresearchuk.org/cancer-help/about-cancer/cancer-questions/what-are-cytostatic-drugs ) in the fight against cancer by targeting DNA. Our previous X-ray crystallographic studies of carboplatin with HEWL, a model protein, have shown partial chemical conversion to cisplatin owing to the high sodium chloride conditions used in the crystallization mixture, as confirmed by the presence of extra anomalous difference density in the binding site that is not attributable to the Pt atom (Tanley et al., 2013[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Schreurs, A. M. M. & Helliwell, J. R. (2013). J. Synchrotron Rad. 20, 880-883.]). Subsequently, we replaced sodium chloride with sodium bromide in the crystallization mixture to more easily observe the conversion of carboplatin to the bromo form (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]). In this condition, the observed chemical transformation which took place was to the transbromoplatin form, and contrasted with the sodium chloride case where cisplatin was seen (Tanley et al., 2013[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Schreurs, A. M. M. & Helliwell, J. R. (2013). J. Synchrotron Rad. 20, 880-883.]). Since a portion of the cyclobutanedicarboxylate (CBDC) moiety was still visible in the His15 ligand-binding site under the sodium bromide conditions, this confirmed that the chemical conversion of carboplatin to transbromoplatin was partial (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]).

In the study reported here, cisplatin or carboplatin was co-crystallized with HEWL under sodium iodide conditions. The motivation for this new study is twofold. Firstly, to again confirm whether a chemical conversion occurs, and specifically whether it is to the trans-platinated or cis-platinated form and whether it is a partial or a full chemical conversion. Secondly, if an iodinated platinated species is observed then it would suggest the prospect of undertaking a dual K-edge (platinum and iodine) targeted radiation therapy experiment against a tumour. Cisplatin administration has previously been studied in the case of radiation therapy using a synchrotron source and the Pt K edge alone (Biston et al., 2004[Biston, M.-C., Joubert, A., Adam, J.-F., Elleaume, H., Bohic, S., Charvet, A.-M., Estève, F., Foray, N. & Balosso, J. (2004). Cancer Res. 64, 2317-2323.]; see also https://www.esrf.eu/UsersAndScience/Publications/Highlights/2004/Imaging/Ima10/ ). Sodium iodide has been used previously to crystallize native HEWL and in these conditions HEWL crystallizes in space group P21 with two protein molecules in the asymmetric unit (Alderton & Fevold, 1946[Alderton, G. & Fevold, H. L. (1946). J. Biol. Chem. 164, 1-5.]; Steinrauf, 1959[Steinrauf, L. K. (1959). Acta Cryst. 12, 77-79.], 1998[Steinrauf, L. K. (1998). Acta Cryst. D54, 767-779.]).

2. Methods

2.1. Crystallization conditions

Co-crystallization of HEWL with cisplatin in NaI solution was carried out under similar conditions as published in Alderton & Fevold (1946[Alderton, G. & Fevold, H. L. (1946). J. Biol. Chem. 164, 1-5.]) and Steinrauf (1959[Steinrauf, L. K. (1959). Acta Cryst. 12, 77-79.], 1998[Steinrauf, L. K. (1998). Acta Cryst. D54, 767-779.]) but with 20 mg HEWL co-crystallized with 1.2 mg cisplatin in 75 µl DMSO, 462.5 µl 0.1 M sodium acetate, 462.5 µl 1 M NaI solution. The conditions were identical for carboplatin but used 1.4 mg carboplatin.

2.2. X-ray diffraction data collection, structure solution and model refinement

A crystal of HEWL with cisplatin or carboplatin was scooped into a loop with silicone oil used as the cryoprotectant. All X-ray diffraction (XRD) data were measured on a Bruker APEX II home-source diffractometer at an X-ray wavelength of 1.5418 Å at a fixed temperature of 100 K (Table 1[link]), using an XRD data-collection strategy to obtain generally good data sets, i.e. high completeness of unique data, high anomalous difference completeness and good data redundancy. XRD data from both crystals were processed using the SAINT software package (v.2; Bruker AXS Inc., Madison, WI, USA).

Table 1
X-ray crystallographic data and final protein plus ligand model-refinement statistics for both the cisplatin and carboplatin crystals

Values in parentheses are for the last shell.

  Cisplatin/NaI Carboplatin/NaI
PDB code 4ow9 4owa
Data-collection temperature (K) 100 100
Data reduction
 Space group P21 P21
 Unit-cell parameters (Å, °) a = 27.25, b = 62.54, c = 58.98, β = 90.92 a = 27.14, b = 62.28, c = 58.05, β = 92.59
 Molecules per asymmetric unit 2 2
 Observed reflections 110261 104255
 Unique reflections 11636 20257
 Resolution (Å) 31.27–2.10 (2.15–2.10) 29.04–1.80 (1.90–1.80)
 Completeness (%) 90.1 (55.7) 94.3 (78.0)
Rmerge (%) 0.130 (0.229) 0.099 (0.340)
 〈I/σ(I)〉 11.7 (3.5) 11.7 (1.9)
 Multiplicity 6.9 (1.6) 5.7 (1.4)
Refinement
 Cruickshank DPI (Å) 0.11 0.18
 No. of atoms
  Protein 2002 2002
  Water molecules 39 147
  Pt and halogen atoms 34 42
  Other bound atoms 28 28
 Average B factor (Å2)    
  Protein atoms 21.1 12.2
  Water molecules 18.8 19.2
  Pt and halogen atoms 29.1 20.9
  Other bound atoms 24.8 18.4
  R factor/Rfree (%) 19.7/27.1 18.4/24.0
  R.m.s.d., bonds (Å)/angles (°) 0.010/1.5 0.015/1.6
 Ramachandran values (%)
  Most favoured 94.1 96.5
  Additional allowed 5.2 3.1
  Disallowed 0.8 0.4
†The PDB validation report includes phenix.xtriage statistics; subsequent use of DETWIN in CCP4 suggested that the data were 6% twinned. To our knowledge, no twinning has been reported for this form of HEWL in NaI conditions before. Turning on amplitude twin refinement in REFMAC improved the R/Rfree from 19.7/27.5% to 19.7/27.1%. The electron-density maps at the His binding sites as well as in general were the same with and without using twin refinement, presumably owing to the rather small twin fraction.
‡The disallowed residues are Asp18, Ser72 and Arg73 and are part of a loop/turn region.

The crystal structures were solved using molecular replacement with Phaser (McCoy et al., 2007[McCoy, A. J., Grosse-Kunstleve, R. W., Adams, P. D., Winn, M. D., Storoni, L. C. & Read, R. J. (2007). J. Appl. Cryst. 40, 658-674.]) followed by rigid-body refinement with REFMAC5 from CCP4 (Murshudov et al., 2011[Murshudov, G. N., Skubák, P., Lebedev, A. A., Pannu, N. S., Steiner, R. A., Nicholls, R. A., Winn, M. D., Long, F. & Vagin, A. A. (2011). Acta Cryst. D67, 355-367.]) using the reported monoclinic lysozyme structure with PDB code 1lkr as the molecular search model (Steinrauf, 1998[Steinrauf, L. K. (1998). Acta Cryst. D54, 767-779.]). Amplitude twin refinement was carried out for the cisplatin data set. Anomalous difference maps were generated using calculated phases with the ligands omitted from the model. These maps allowed a check for and identification of the I-atom positions. Model building, adjustment and restrained refinement were carried out using Coot (Emsley & Cowtan, 2004[Emsley, P. & Cowtan, K. (2004). Acta Cryst. D60, 2126-2132.]) and REFMAC5 (Murshudov et al., 2011[Murshudov, G. N., Skubák, P., Lebedev, A. A., Pannu, N. S., Steiner, R. A., Nicholls, R. A., Winn, M. D., Long, F. & Vagin, A. A. (2011). Acta Cryst. D67, 355-367.]) in CCP4. Ligand-binding occupancies were calculated using SHELXTL (Sheldrick, 2008[Sheldrick, G. M. (2008). Acta Cryst. A64, 112-122.]). The platinum-to-ligand distances were not restrained during refinement. The crystallographic and molecular model-refinement parameters are summarized in Table 1[link]. Figures were prepared with CCP4mg (McNicholas et al., 2011[McNicholas, S., Potterton, E., Wilson, K. S. & Noble, M. E. M. (2011). Acta Cryst. D67, 386-394.])

3. Results

3.1. Cisplatin study

Ligand binding is seen at His15 residue of both molecules A and B of HEWL in this monoclinic crystal form, i.e. with two molecules per asymmetric unit. In molecule A platinum binding is only seen at the Nδ binding site (Fig. 1[link]), with an anomalous difference electron-density peak height of 9.8σ and an occupancy value of 80% (Table 2[link]). Besides the platinum peak, there are two large anomalous difference electron-density peaks of 11.1σ and 8.8σ in the trans positions which are readily assignable as I atoms at distances of 2.6 Å (±0.1 Å) from the Pt atom, confirming that cisplatin has converted to the trans iodo-platinated form (transiodoplatin). The angle between these three atoms is 176°, which is close to linearity. A third 2Fo − Fc electron-density peak is seen bound to the Pt atom. However, no anomalous difference electron density is observed here and so a third I atom is ruled out. Modelling in an N atom from cisplatin gave a B factor of 2.0 Å2, which is physically unrealistic, and therefore a Cl atom was modelled in. This Cl atom has an occupancy of 100% as calculated by SHELX and a quite reasonable B factor of 21.3 Å2. The distance between the platinum and this chlorine is 2.4 Å (±0.1 Å) and can be compared with the usual platinum–chlorine distance of 2.35 Å; as this distance is well within the error of the bond-distance estimate (0.1 Å), this atom assignment seems reasonable. In molecule B, the identification of the compound bound to the Nδ atom of His15 (Supplementary Fig. S11) is more difficult than in molecule A described above (Fig. 1[link]) and the figure is given in the Supporting Information for completeness. Platinum binding is again only seen at the Nδ binding site (Fig. 1[link]), with an anomalous difference electron-density peak height of 6.7σ and an occupancy of 67% (Table 2[link]). There are also two other anomalous difference electron-density peaks in the binding site (7.2 and 4σ) in the trans position to the Pt atom and these are therefore assigned as I atoms bound to the platinum, each at a distance of 2.6 Å (±0.2 Å). The angle between these three atoms is 169°, showing signs of some distortion from linearity. In molecule B there are also two extra 2FoFc density peaks close to the Pt and I atoms. Modelling in an N atom from cisplatin again gave a B factor of 2.0 Å2. Owing to this, a mixture of cisplatin and transiodoplatin appears to be bound to this Nδ atom. The distance between platinum and chlorine 1 is 2.4 Å (±0.3 Å) and the platinum–chlorine 2 distance is 2.8 Å (±0.1 Å). The occupancies of each molecule as a whole, estimated using SHELX, gave values of 51% for the transiodoplatin molecule and 49% for the cisplatin molecule. A third 2FoFc electron-density peak is also seen, with no anomalous difference electron density observed at this position. An Na ion with 100% occupancy has been modelled in with a B factor of 33 Å2.

Table 2
Occupancy values of the Pt and I atoms for both the cisplatin and carboplatin cases calculated using SHELX

  Cisplatin study Carboplatin study
    Anomalous peak height (σ) Occupancy (%) Anomalous peak height (σ) Occupancy (%)
Pt His15 Nδ binding site, molecule A 9.8 80 ± 12 9.8 77 ± 5
I1 11.1 86 10.8 70
I2 8.8 89 7.8 86
Pt His15 Nδ binding site, molecule B 6.7 67 ± 11 12.2 68 ± 4
I1 7.2 77 12.1 70
I2 4.0 67 11.3 77
Pt In a crevice between two symmetry-related molecules near Asn106 6.7 57 8.8 68
I1 9.4 60 5.4 70
I2 8.2 74 5.9 77
I3 7.8 62 9.2 69
[Figure 1]
Figure 1
Binding to His15 shows a chemically transformed cisplatin, namely transiodoplatin. (a, b) The molecule A binding site shown in two different views. The 2FoFc electron-density map (blue) is contoured at 1.5 r.m.s. and the anomalous difference electron-density map (orange) is contoured at 3σ. The Pt atom is shown in purple, the iodines are in yellow, the chlorine is in grey, C atoms are in green and N atoms are in blue.

At the His15 N binding sites in molecules A and B, an anomalous difference electron-density peak of 4.1σ and 4.0σ is seen, respectively, at 3.9 (±0.2) and 5.0 Å (±0.2 Å) from the N atom, too distant to be a Pt atom. This peak is instead assigned as an I atom in both cases, which is 3.9 Å (±0.2 Å) from the NH backbone group of Ile88, which is in the correct distance range for a halogen hydrogen bond. This is the same situation as previously seen in the NaBr crystallization conditions case (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]), where a Br atom was assigned at this position.

3.2. Carboplatin study

Ligand binding is seen at the His15 Nδ atoms in both molecule A and molecule B. In molecule A, a platinum peak with an anomalous difference electron density of 9.8σ is seen which refines to an occupancy of 77% (Supplementary Fig. S2 and Table 2[link]). Two further anomalous difference electron-density peaks are seen (10.8σ and 7.8σ) in the trans position to the Pt atom and these are assigned as I atoms bound to the Pt atom with a distance of 2.6 Å (±0.3 Å) (Supplementary Fig. S2). A third 2FoFc electron-density peak is seen at a binding distance from the Pt atom, but no anomalous difference electron density is observed here. Owing to the lack of anomalous difference density, a portion of the CBDC moiety was modelled in. Thus, similar to the carboplatin in NaBr conditions (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]), a portion of the CBDC moiety must still be present at this binding position.

In molecule B, a platinum anomalous difference electron-density peak of 12.2σ is observed which refines to an occupancy of 68% (Fig. 2[link] and Table 2[link]). Two anomalous difference density peaks are seen (12.1σ and 11.3σ) in trans positions to the Pt atom and these are assigned as I atoms bound to the Pt atom at a distance of 2.6 Å (±0.2 Å). A third 2FoFc electron-density peak is seen at a binding distance to the Pt atom, with a weak anomalous difference electron-density peak of 2.6σ. Owing to the weakness of the peak it was not assigned to an atom type, but the 2FoFc density is more elongated than in the trans iodo positions at this site and could correspond to a mixture of an I atom and a portion of the CBDC moiety (Fig. 2[link]). Modelling in a mixture of an I atom and a portion of the CBDC moiety gives occupancies of 52% for the I atom and 48% for the CBDC moiety. Thus, the carboplatin has partially converted to the trans iodo-platinated form, with some evidence that a portion of the carboplatin molecule is still present. Molecule B is shown in Fig. 2[link] and molecule A in Supplementary Fig. S2 as they are very similar and the electron density around the carboplatin is slightly better for molecule B.

[Figure 2]
Figure 2
Binding of carboplatin chemically transformed to transiodoplatin to His15. (ab) The molecule B binding site shown in two different views. The 2FoFc electron-density map (blue) is contoured at 1.5 r.m.s. and the anomalous difference electron-density map (orange) is contoured at 3σ. The Pt atom is shown in purple, the iodines are in yellow, C atoms are in green, O atoms are in red and N atoms are in blue.

At the N binding site in molecules A and B anomalous difference electron-density peaks of 3.4σ and 5.5σ are seen 5.1 (±0.4) and 5.5 Å (±0.2 Å) from the N atom, too distant and too weak to be assignable as a Pt atom. This peak is assigned as an I atom in both cases which is 3.5 Å (±0.4 Å) and 3.9 Å (±0.2 Å) from the NH backbone group of Ile88, which is in the correct distance range for a halogen hydrogen bond.

3.3. A third Pt ligand-binding site in a crevice between two symmetry-related molecules

For both the cisplatin and carboplatin HEWL NaI crystal studies, a third platinum binding site is seen where a PtI3 moiety is identified bound in a crevice between two symmetry-related molecules near Asn106, Arg112, Pro70, Asn65 and Asn103 of molecule A, and Arg128, Cys6, Glu7 and Ala10 of a symmetry-related molecule. However, this binding is not seen at the same residues in molecule B. In the cisplatin case, three anomalous difference electron-density peaks of 9.4σ, 8.2σ and 7.8σ are seen (Table 2[link]) at distances of 2.7 (±0.1), 2.5 (±0.1) and 2.5 Å (±0.1 Å) from the Pt atom, respectively. A fourth 2FoFc electron-density peak is found at a distance of 2.4 Å (± 0.2 Å) from the Pt atom (Fig. 3[link]a). A Cl atom is assigned at this fourth position. In the carboplatin study, three anomalous difference electron-density peaks of 5.4σ, 5.9σ and 9.2σ are seen (Table 2[link]) at distances of 2.7 (±0.3), 2.5 (±0.3) and 2.7 Å (±0.3 Å) from the Pt atom, respectively. A fourth 2FoFc electron-density peak within binding distance of the Pt atom has elongated density (Fig. 3[link]b). We interpret this as a portion of the CBDC moiety of carboplatin bound at this fourth position.

[Figure 3]
Figure 3
A PtI3X complex bound in a crevice between two symmetry-related molecules. (a, b) Complex derived from cisplatin with a Pt atom bound to three I atoms and a Cl atom bound near Arg128, Cys6, Glu7 and Ala10 of molecule A and Asn106, Arg112, Pro70 and Asn65 of a symmetry-related molecule. (c, d) Complex derived from carboplatin with platinum bound to three I atoms and a portion of the CBDC moiety bound near Asn106, Arg112, Pro70, Asn65 of molecule A and Arg128, Cys6, Glu7 and Ala10 of a symmetry-related molecule (a). The 2FoFc electron-density map (blue) is contoured at 1.5σ and the anomalous difference electron-density map (orange) is contoured at 3σ. The Pt atom is shown in purple, the iodines are in yellow, the chlorine is grey, C atoms are green and O atoms are red.

4. Discussion

Our studies have investigated whether co-crystallizing cisplatin or carboplatin with HEWL in NaI conditions, rather than using NaCl, would result in partial or full chemical conversion of these compounds to the iodo form. Previous results with carboplatin in NaCl crystallization conditions showed partial conversion to cisplatin (Tanley et al., 2013[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Schreurs, A. M. M. & Helliwell, J. R. (2013). J. Synchrotron Rad. 20, 880-883.]), whereas in sodium bromide conditions the carboplatin was partially converted to the trans bromo form with a portion of the CBDC moiety still being present (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]). Obviously, cisplatin with HEWL under sodium chloride conditions would simply preserve chlorinated platinum in the cisplatin.

The results presented here for both cisplatin and carboplatin indeed showed partial conversion to the trans iodo form with a portion of a Cl or CBDC moiety still seen in the binding site (Figs. 1[link] and 2[link]), which is similar to the results using NaBr as the crystallization high-salt component (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]). Tanley, Diederichs et al. (2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]) describe carboplatin binding to HEWL in NaBr crystallization conditions as well as in non-NaCl and non-NaBr conditions, the latter being in order to see a chemically unmodified carboplatin. A study of cisplatin binding to HEWL in NaBr conditions has also been carried out, and for completeness those results are given in the Supporting Information to this paper. The results are very similar to the carboplatin study in NaBr conditions, in which the cisplatin is also seen to be converted to a transbromoplatin form with a Cl atom also bound to the platinum centre at the Nδ binding site. Similar to the carboplatin study, the N binding site shows less detail, with a weakly occupied Pt atom (20%) bound to a Br atom.

Previously, under NaCl conditions at pH 4.7, we have seen clear binding at both the Nδ and N sites of His15. This was attributed to the chlorine extracting a His15 H atom, creating an imidazolyl ion (Tanley et al., 2012[Tanley, S. W. M., Schreurs, A. M. M., Kroon-Batenburg, L. M. J., Meredith, J., Prendergast, R., Walsh, D., Bryant, P., Levy, C. & Helliwell, J. R. (2012). Acta Cryst. D68, 601-612.]). In the bromo case (Tanley, Diederichs et al., 2014[Tanley, S. W. M., Diederichs, K., Kroon-Batenburg, L. M. J., Levy, C., Schreurs, A. M. M. & Helliwell, J. R. (2014). Acta Cryst. F70, 1135-1142.]) binding at both sides was still seen, but with a much weaker occupancy (up to 20%) for the N binding site. We rationalize this as being owing to bromine ions being weaker than chloride ions at extracting the last His H atom to generate the imidazolyl ion. Another possibility is tautomeric forms; see Tanley et al. (2012[Tanley, S. W. M., Schreurs, A. M. M., Kroon-Batenburg, L. M. J., Meredith, J., Prendergast, R., Walsh, D., Bryant, P., Levy, C. & Helliwell, J. R. (2012). Acta Cryst. D68, 601-612.]) for a full discussion. Where binding is seen at only one histidine N atom we are obviously not seeing a tautomeric pair or an imidazolyl anion. In the iodo case, the hydrogen-abstracting effectiveness is worse than for bromide ions and this is a likely reason why the binding of a platinum ligand is seen only at one His15 N atom, at least at pH 4.7, in the NaI case. A further difference between the NaI conditions and the NaCl or NaBr conditions was the fact that the crystals are monoclinic, rather than tetragonal, and thereby had two protein molecules in the asymmetric unit. In both monoclinic asymmetric units we note that binding only occurs to the Nδ atom of His15.

Recently, Messori et al. (2013[Messori, L., Marzo, T., Gabbiani, C., Valdes, A. A., Quiroga, A. G. & Merlino, A. (2013). Inorg. Chem. 52, 13827-13829.]) soaked PtI2(NH3)2 into pre-grown HEWL crystals and the Pt atom was seen to be bound to the Nδ atom of His15 but, as they described it, showed `peculiar features' involving

the presence of three peaks of anomalous electron density close to a Pt atom suggesting the presence of two alternative modes of binding of the [PtI2NH3] moiety.

In our studies reported here, by using NaI in the crystallization mixture we examined whether the cisplatin or carboplatin was converted to an iodo form with I atoms bound to the platinum centre. For our NaI co-crystallization conditions we see a PtI2X2 species at His15, i.e. transiodoplatin bound to the His15 N atom. In addition, though, we also see a third platinum moiety, a PtI3X species, which is bound in a crevice between molecules A through residues Asn106, Arg112, Pro70, Asn65 and Asn103, and Arg128, Cys6, Glu7 and Ala10 of a symmetry-related molecule. This binding is not seen at the same residues for molecule B. The evidence that a platinum is seen bound to three I atoms is based on the presence of anomalous difference electron-density peaks (Fig. 3[link]) and then on their refined occupancies. The fourth bound atom, i.e. the X in PtI3X, is interpreted as a Cl atom (cisplatin) or a portion of the CBDC moiety (carboplatin). This is reminiscent of Zeise's salt PtCl3C2H4 (Black et al., 1969[Black, M., Mais, R. H. B. & Owston, P. G. (1969). Acta Cryst. B25, 1753-1759.]).

Finally, we note that in our companion paper on HEWL with Pt hexahalides we see a PtI3 species bound to the His15 N atom (Tanley, Starkey et al., 2014[Tanley, S. W. M., Starkey, L.-V., Lamplough, L., Kaenket, S. & Helliwell, J. R. (2014). Acta Cryst. F70, 1132-1134.]).

5. Conclusions

Co-crystallization of HEWL with cisplatin and carboplatin in NaI was carried out, with the XRD results showing that both platinum compounds indeed underwent a partial chemical conversion. In both cases this was to transiodoplatin (i.e. PtI2X2) bound to the His15 N atom, with either a Cl atom (cisplatin) or a portion of the CBDC moiety (carboplatin) bound at the fourth Pt ligand atom position. These results are similar to our previous results using NaBr crystallization conditions. In the NaI conditions, only binding to the Nδ atom of His15 is seen; this is attributed to the inability of iodide ions to produce an imidazolyl ion, at least at the pH used in these experiments.

A PtI3X species is seen bound in a crevice between symmetry-related protein molecules; here the platinum is bound to three I atoms based on the presence of anomalous difference electron density and their refined occupancies, with the fourth bound atom being a Cl atom (cisplatin) or a portion of the CBDC moiety (carboplatin). The observation of these iodinated platinum species suggests the prospect of undertaking a dual K-edge (platinum and iodine) targeted radiation therapy experiment against a tumour. Cisplatin administration has previously been studied in this way involving radiation therapy using a synchrotron source and the Pt K edge alone (Biston et al., 2004[Biston, M.-C., Joubert, A., Adam, J.-F., Elleaume, H., Bohic, S., Charvet, A.-M., Estève, F., Foray, N. & Balosso, J. (2004). Cancer Res. 64, 2317-2323.]; see also https://www.esrf.eu/UsersAndScience/Publications/Highlights/2004/Imaging/Ima10/ ). To undertake such a dual K-edge radiation therapy involving iodinated cisplatin or carboplatin under patient conditions would build upon experiments such as are already under way at the ESRF with cisplatin as cited above.

6. Related literature

The following reference is cited in the Supporting Information for this article: Cianci et al. (2008[Cianci, M., Helliwell, J. R. & Suzuki, A. (2008). Acta Cryst. D64, 1196-1209.]).

Supporting information


Footnotes

1Supporting information has been deposited in the IUCr electronic archive (Reference: NO5053 ).

Acknowledgements

JRH is grateful to the University of Manchester for general support, to the EPSRC for a PhD studentship to SWMT and to the School of Chemistry for crystallization, computing and X-ray facilities. We are grateful to Dr Chris Muryn of the School of Chemistry for his stewardship of the APEX II CCD X-ray diffractometer.

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Volume 70| Part 9| September 2014| Pages 1127-1131
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