Abstract
In the early days, Hammersmith campus was probably the leading medical research hospital in the UK, and enjoyed a reputation based on a fantastic multidisciplinary approach and spirit of collaboration, co-operation and clinical support. Nuclear medicine at the Hammersmith Hospital was established as a separate unit by Peter Lavender in the early seventies. It was called the Radioisotope Unit to distinguish it from the pre-existing Department of Medical Physics. As well as providing a clinical service, the unit, was active in clinical research complemented by the extensive academic activities of the MRC Cyclotron Unit. This chapter will enlighten us with the contributions from Hammersmith Hospitals’ to the science and practice of nuclear medicine in the UK and worldwide.
You have full access to this open access chapter, Download chapter PDF
Similar content being viewed by others
Keywords
These keywords were added by machine and not by the authors. This process is experimental and the keywords may be updated as the learning algorithm improves.
Nuclear medicine at the Hammersmith Hospital was established as a separate unit by Peter Lavender in the early seventies. It was called the Radioisotope Unit to distinguish it from the pre-existing Department of Medical Physics, headed by Harold Glass who was one of the early pioneers in medical radioisotope scanners [1]. As well as providing a clinical service, the unit, which only comprised two rooms, was active in clinical research complemented by the extensive academic activities of the MRC Cyclotron Unit. Two good examples of these activities that launched nuclear medicine at Hammersmith are firstly the development by Clark, Watson Fazio and Jones of Kr-81m for ventilation and perfusion studies [2], and secondly, cell labelling.
Kr-81m is a 13 s half-life radionuclide that is the metastable daughter of Rb-81, which has a half-life of 4.7 h. To obtain Kr-81m gas, oxygen is passed through the generator. There was an enthusiastic response to the generator across the UK, and, at one point, Kr-81m/Tc-99m ventilation/perfusion imaging was the second most frequently performed imaging procedure in the UK after bone scanning. Whilst Kr-81m remains the optimal ventilation agent for lung scanning, it is not so widely appreciated that Lavender and his colleagues also administered Kr-81 in solution to measure tissue perfusion. To obtain Kr-81m in solution, isotonic glucose is passed through the generator. For example, Harvey-Turner and Selwyn infused Kr-81m into the aortic root of dogs and continuously imaged regional changes in myocardial perfusion in response to transient coronary artery occlusion [3]. The distribution of pulmonary blood flow in humans was also imaged by continuous intravenous infusion [4]. Kr-81m was given both by inhalation and infusion to study ventilation-perfusion ratios and regional lung function in adults [4, 5] and children [6], When combined with the longer half-life Kr-85 (a lung gas volume marker), regional lung function per unit volume could be assessed. Lavender used Kr-81m/Tc-99m SPECT in the early eighties to study pulmonary physiology [7] but did not feel that it offered any great advantage over planar imaging for diagnosing pulmonary thrombo-embolic disease.
The second example of innovative collaboration between Hammersmith nuclear medicine and MRC Cyclotron Unit was the development of cell labelling by Thakur and McAfee. John McAfee came to the Hammersmith for a 6 month sabbatical with the specific aim of working with Matthew Thakur to develop cell labelling for clinical imaging. Cr-51 had already been developed for cell labelling but is not suitable for gamma camera imaging, only surface counting. Testing several combinations of lipophilic chelating agents and radiometals, Thakur and McAfee came up with In-111 and hydroxyquinoline (oxine). The first full paper on leucocyte scanning for sepsis, based on 15 patients, was published in 1977 ([8]; Fig. 12.1).
There was great hope for performing labelled lymphocyte studies too, until it was soon found that lymphocytes are radio-sensitive and destroyed by labelling with amounts of In-111 required for imaging. I arrived at the Hammersmith in 1979 to undertake a 3-year Cancer Research Campaign-funded project on labelled lymphocytes but with this discovery quickly turned my attention to labelled leucocytes and platelets. In those days, Amersham International was not selling In-111-oxine, so it had to be prepared in-house (by a radio-chemist, Malcolm Kensett, in the MRC Cyclotron Unit). Once a patient had been identified, I would order the In-111-oxine, go to the MRC to collect it, take the patient’s blood, go to the Haematology Isotope Unit to label it, then take it back to the Radioisotope Unit to inject it and image the patient. The Haematology isotope unit under the leadership of Mitchell Lewis, provided a tertiary service for ferrokinetics, using Fe-59 and Fe-52 (a positron emitter), and red cell survival and surface counting studies using Cr-51-labelled red cells. The unit also supported studies involving labelled cells, including In-111-labelled platelet kinetic studies by Klonikakis et al. [9], In-113m-labelled red cells and platelets, and studies on the clearance rates of labelled red cells modified by heating or antibody coating, undertaken by several workers from the Department of Medicine studying reticulo-endothelial (RE) function.
The Medical Research Council funded the building of a medical cyclotron on the Hammersmith site in 1954 (Fig. 12.2). This stimulated much research into cardiopulmonary physiology and neuro-pathophysiology in collaboration with the clinical staff of the Hospital. Pairs of scintillation detectors (front and back) were used first (with coincidence counting of positron emission), then planar gamma camera imaging, and finally positron emission tomography. The first studies were carried out in the late 1950s by West and his colleagues [10–12] using the short-lived positron emitting isotope, oxygen-15 (half life 2.1 min) as C15O2 and C15O. Lung water distribution was studied with H2 15O [13, 14], pulmonary perfusion with infused 13N2 in solution [15], pulmonary haemorrhage with inhaled 11CO [16], and ventilation with neon-19 [17]. Rhodes and Hughes [18] summarized pulmonary studies using the positron camera. There was also much interest in studies of inflammatory conditions using F-18-fluorodeoxyglucose (18FDG) [19, 20], and in imaging beta-agonist receptors in the heart and lung [21, 22].
Research activity elsewhere in the MRC Cyclotron Unit included the development of 18FDG for imaging the brain (Terry Jones and Richard Frackowiak) and myocardium. Camici et al. were one of the first groups to image Rb-82 uptake in the myocardium of patients with coronary disease and show increased FDG uptake in ischaemic regions [23].
Many pioneers in nuclear medicine worked at Hammersmith. One of the earliest was Charles Galasko who in bone scintigraphy showed in 1968 that 12 of 50 patients with apparently ‘early’ breast cancer on clinical, radiological and biochemical grounds had positive scintigraphy and developed metastatic disease in the first 5 years following mastectomy [24]. Joseph Pflug was a pioneer in lymphatic function studies and was one of the first to use lymphoscintigraphy. Aga Epenetos, an oncologist, was one of the first to develop radiolabelled monocloncal antibodies for imaging cancer. Having worked with Keith Britton at St Bartholomew’s and Walter Bodmer from the then ICRF, Epenetos continued his work at the Hammersmith. Also collaborating with ICRF, Lavender used a very effective monoclonal antibody to the platelet fibrinogen receptor for imaging thrombus ([25]; Fig. 12.3).
Dominic Haskard came to Hammersmith from Guy’s Hospital around 1990 and developed very effective monocloncal antibodies to vascular adhesion molecules for imaging inflammation [26]. Sadly, however, none of these labelled antibodies made it into regular nuclear medicine practice.
Having developed In-111-oxine cell labelling, workers at the Hammersmith, again in collaboration with the MRC Cyclotron Unit (Danpure and Osman), then explored other chelating agents and discovered tropolone [27], which, now that GE do not offer In-111-oxine, is the standard agent for In-111 cell labelling. We then went on to develop Tc-99m-HMPAO for leucocyte labelling [28]. Saverymuttu demonstrated the extraordinary ability of In-111 and Tc-99m-labelled leucocyte scintigraphy to quantify and image inflammatory bowel disease (Fig. 12.4) and published numerous papers on its applications in gastroenterology.
Other, generally unfunded work, on patient volunteers established the normal whole body kinetics and physiological margination sites of granulocytes, and, in particular, dismantled the erroneous notion that the vast majority of intravascular granulocytes are pooled in the lungs [29]. It was clearly demonstrated how in systemic inflammatory diseases, such as pancreatitis, IBD and vasculitis, circulating granulocytes become primed, lose deformability and undergo prolonged transit through the pulmonary vasculature. This is in contrast to hold-up in the lungs of granulocytes artificially activated by the labelling procedure and associated with very low intravascular recovery. This work led to quality control guidelines for leucocyte labelling.
Another major nuclear medicine landmark in the history of the Hammersmith radioisotope unit was the development by Mark Pepys and Philip Hawkins of I-123-labelled serum amyloid protein (SAP) for imaging amyloidosis [30]. This work was dramatically successful and led to the establishment of a separate unit in the hospital with its own gamma camera and technical staff, such was the weight of referrals from all over the country. So, at one time, there were five separate nuclear medicine units on the Hammersmith site! I remember Pepys and Hawkins opening champagne in the Radioisotope Unit when they had just witnessed heavy hepatic uptake of labelled SAP in a patient with amyloidosis (Fig. 12.5). I wondered if the celebrations might be premature, having learned that in general when a tracer is not functioning properly it is liable to end up in the liver, but this was clearly not the case!
The spirit of research collaboration at the Hammersmith Hospital fuelled many interesting research projects using radionuclides. For example, the early advances in interventional radiology allowed us to inject In-111-labelled platelets directly into the splenic artery of patients having arterial catheterization and show conclusively that platelets pool in the spleen and are released after a mean residence time of about 10 min. Plasma exchange for the treatment of immune complex disease was shown to be associated with improved RE function as measured by the splenic extraction efficiency of radiolabelled antibody-coated red cells, using simultaneously injected In-111-labelled platelets to measure splenic blood flow [31]. Before then, it had been thought that RE function could be quantified by the clearance rate of heat-damaged red cells until we showed that the clearance rate reflected splenic pooling and was therefore, like platelet equilibration between blood and spleen, a measure of splenic blood flow. Early studies on pulmonary epithelial permeability using inhaled Tc-99m-DTPA [32] and pulmonary endothelial permeability using intravenous In-111-transferrin [33] were performed by Royston and his co-workers. Davies and Walport demonstrated for the first time the whole body kinetics of I-123-labelled immune complexes [34].
In the mid-nineties, rotaPET was acquired by what had now been re-named the ‘Nuclear Medicine Department’. This was a partial ring detector consisting of two separate segments and was used predominantly for FDG imaging of cancer but also clinical F-18-DOPA brain imaging. The department was involved in early clinical work with In-111-pentetriotide and showed how amino acid infusion blocked renal tubular uptake of the agent [35]. In research, Harrington and Stewart demonstrated the targeting of tumours by In-111-labelled stealth liposomes containing chemotherapeutic agents [36]. In collaboration with ‘Tiny’ Maini from the Institute of Rheumatology, the therapeutic effect of TNFα blockade was shown to reduce dramatically leucocyte uptake in rheumatoid joints [37]. Muhammad Mubashar was one of the first workers to image P-glycoprotein expression in breast cancer [38]. As one of the first centres in the UK to develop interventional radiology, the Hammersmith Hospital was a referral centre for conditions such as pulmonary arterio-venous shunts and much work with the Department of Respiratory Medicine [39] was performed to quantify these shunts before and after therapeutic embolization. Finally, elegant work performed in collaboration with George Hall, an anaesthetist with an interest in exercise physiology, demonstrated in trained athletes undergoing maximal brief exercise how platelets and all leucocyte subtypes pool in the spleen with similar residence times [40]. Contrasting the behaviour of red cells versus leucocytes and platelets in response to exercise, he showed that the spleen is essentially an erectile organ – permanently erect!
In the time I was at Hammersmith Hospital (1979–1999), the Hammersmith campus was probably the leading medical research hospital in the UK, and enjoyed a reputation based on a fantastic multidisciplinary approach and spirit of collaboration, co-operation and clinical support. Clinical research in nuclear medicine that goes beyond the evaluation of the latest novel radiopharmaceutical or imaging hardware critically depends on support from the clinicians, and this support was second-to-none at the Hammersmith.
References
Glass HI, Hudson FR, French MT. A 70 mm diameter germanium detector medical radioisotope scanner. Medical Radioisotope Scintigraphy. Vienna: IAEA; 1973.
Fazio F, Jones T. Assessment of regional ventilation by continuous inhalation of radioactive krypton-81m. Br Med J. 1975;3(5985):673–6.
Turner JH, Selwyn AP, Jones T, et al. Continuous imaging of regional myocardial blood flow in dogs using krypton-81m. Cardiovasc Res. 1976;10:398–404.
Harf A, Pratt T, Hughes JMB. Regional distribution of VA/Q in man at rest and on exercise measured with krypton-81m. J Appl Physiol. 1978;44:115–23.
Amis TC, Jones HA, Hughes JMB. Effect of posture on interregional distribution of pulmonary perfusion and VA/Q ratios in man. Respir Physiol. 1984;56:169–82.
Ciofetta G, Silverman M, Hughes JMB. Quantitative approach to the study of regional lung function in children using Krypton-81m. Br J Radiol. 1980;53:950–9.
Lavender JP, Al-Nahhas AM, Myers MJ. Ventilation perfusion ratios of the normal supine lung using emission tomography. Br J Radiol. 1984;57:141–6.
Thakur ML, Lavender JP, Arnot RN, et al. Indium-111-labeled autologous leukocytes in man. J Nucl Med. 1977;18:1014–21.
Klonizakis I, Peters AM, Fitzpatrick ML, et al. Radionuclide distribution following injection of indium-111 labelled platelets. Br J Haematol. 1980;46:595–602.
West JB, Dollery CT. Distribution of blood flow and ventilation-perfusion ratio in the lung, measured with radioactive CO2. J Appl Physiol. 1960;15:405–10.
West JB, Dollery CT. Absorption of inhaled radioactive water vapour. Nature. 1961;189:588.
West JB, Dollery CT, Hugh-Jones P. The use of radioactive carbon dioxide to measure regional blood flow in the lungs of patients with pulmonary disease. J Clin Invest. 1961;40:1–12.
Jones T, Jones HA, Rhodes CG, et al. Distribution of extravascular fluid volumes in isolated perfused lungs measured with H2 15O. J Clin Invest. 1976;57:706–13.
Swinburne AJ, MacArthur CGC, Rhodes CG, et al. Measurement of lung water in dog lobes using inhaled C15O2 and injected H2 15O. J Appl Physiol Respir Environ Exercise Physiol. 1982;52:1535–44.
Ewan PW, Jones HA, Nosil J, et al. Uneven perfusion and ventilation within lung regions studied with nitrogen-13. Respir Physiol. 1976;34:45–60.
Ewan PW, Jones HA, Rhodes CG, et al. Detection of intrapulmonary haemorrhage with carbon monoxide uptake: application in Goodpasture’s Syndrome. N Engl J Med. 1976;295:1391–6.
Valind SO, Rhodes CG, Brudin LH, et al. Measurements of regional ventilation pulmonary gas volume: theory and error analysis with special reference to positron emission tomography. J Nucl Med. 1991;32:1937–44.
Rhodes CG, Hughes JMB. Pulmonary studies using positron emission tomography. Eur Respir J. 1995;8:1001–17.
Jones HA, Clark RJ, Rhodes CG, et al. In vivo measurement of neutrophil activity in experimental lung inflammation. Am J Respir Crit Care Med. 1994;149:1635–9.
Jones HA. Inflammation imaging. Proc Am Thorac Soc. 2005;513–4:545–8.
Ueki J, Rhodes CG, Hughes JMB, et al. In vivo quantification of pulmonary beta-adrenoceptor density in man u sing S[11C]CGP12177 and positron emission tomography. J Appl Physiol. 1993;75:559–65.
Hayes MJ, Qing F, Rhodes CG, et al. In vivo quantification of human pulmonary β-adrenoceptors with PET: effect of β-agonist therapy. Am J Resp Crit Care Med. 1996;154:1277–83.
Camici P, Araujo LI, Spinks T, et al. Increased uptake of 18F-fluorodeoxyglucose in postischemic myocardium of patients with exercise-induced angina. Circulation. 1986;74:81–8.
Galasko CS, Westerman B, Sellwood RA, et al. Use of the gamma camera for early detection of osseous metastases from mammary cancer. Br J Surg. 1968;55:613–5.
Peters AM, Lavender JP, Needham SG, et al. Imaging thrombus with a radiolabelled monoclonal antibody to platelets. Br Med J. 1986;293:1525–7.
Jamar F, Chapman PT, Harrison AA, et al. Inflammatory arthritis: imaging of endothelial cell activation with an In-111 labeled F(ab’)2 fragment of anti-E-selectin monoclonal antibody. Radiology. 1995;194:843–50.
Peters AM, Saverymuttu SH, Reavy HJ, et al. Imaging inflammation with 111-indium tropolonate labeled leukocytes. J Nucl Med. 1983;24:39–44.
Peters AM, Danpure HJ, Osman S, et al. Preliminary clinical experience with Tc-99m-HMPAO for labelling leucocytes and imaging inflammation. Lancet. 1986;2:946–9.
Peters AM. Just how big is the pulmonary granulocyte pool? Clin Sci. 1998;94:7–19.
Hawkins PN, Myers MJ, Lavender JP, et al. Diagnostic radionuclide imaging of amyloid: biological targeting by circulating human serum amyloid P component. Lancet. 1988;1(8600):1413–8.
Walport MJ, Peters AM, Elkon KB, et al. The splenic extraction ratio of antibody coated erythrocytes and its response to plasma exchange and pulse methy-lprednisolone. Clin Exp Immunol. 1985;65:465–73.
Nolop KB, Maxwell DL, Fleming JS, et al. A comparison of 99mTc-DTPA and 113mIn-DTPA aerosol clearances in humans. Effects of smoking, hyperinflation and in vitro oxidation. Am Rev Respir Dis. 1987;136:1112–6.
Braude S, Nolop KB, Hughes JMB, et al. Comparison of lung vascular and epithelial permeability indices in the Adult Respiratory Distress Syndrome. Am Rev Respir Dis. 1986;133:1002–5.
Davies KA, Peters AM, Beynon HLC, et al. Immune complex processing in patients with sysytemic lupus erythematosus – in vivo imaging and clearance studies. J Clin Invest. 1992;90:2075–83.
Hammond PJ, Wade AF, Gwilliam ME, et al. Amino acid infusion blocks renal tubular uptake of an indium-labelled somatostatin analogue. Br J Cancer. 1993;67:1437–9.
Harrington KJ, Mohammadtaghi S, Uster PS, et al. Effective targeting of solid tumours in patients with locally advanced cancers by radiolabelled pegylated liposomes. Clin Cancer Res. 2001;7:243–54.
Taylor PC, Paleolog E, Chapman PT, et al. TNFα blockade in patients with rheumatoid arthritis reduces chemokines and leukocyte traffic to joints. Arthr Rheum. 2000;43:38–47.
Mubashar M, Harrington KJ, Chaudhary KS, et al. Tc-99m-sestamibi imaging in the assessment of toremifene as a modulator of multidrug resistance in patients with breast cancer. J Nucl Med. 2002;43:519–25.
Whyte MKB, Peters AM, Hughes JMB, et al. Quantification of right-to-left shunt at rest and during exercise in patients with pulmonary arteriovenous malformations. Thorax. 1992;47:790–6.
Allsop P, Peters AM, Arnot RN, et al. Intrasplenic blood cell kinetics in man before and after brief maximal exercise. Clin Sci. 1992;83:47–54.
Acknowledgements
The author would like to thank Prof Mike Hughes and Prof Peter Lavender for advice regarding the work described in this article.
Author information
Authors and Affiliations
Editor information
Editors and Affiliations
Rights and permissions
Open Access This chapter is distributed under the terms of the Creative Commons Attribution-Noncommercial 2.5 License (http://creativecommons.org/licenses/by-nc/2.5/) which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
The images or other third party material in this chapter are included in the work’s Creative Commons license, unless indicated otherwise in the credit line; if such material is not included in the work’s Creative Commons license and the respective action is not permitted by statutory regulation, users will need to obtain permission from the license holder to duplicate, adapt or reproduce the material.
Copyright information
© 2016 The Author(s)
About this chapter
Cite this chapter
Peters, M. (2016). Nuclear Medicine at the Hammersmith Hospital. In: McCready, R., Gnanasegaran, G., Bomanji, J. (eds) A History of Radionuclide Studies in the UK. Springer, Cham. https://doi.org/10.1007/978-3-319-28624-2_12
Download citation
DOI: https://doi.org/10.1007/978-3-319-28624-2_12
Published:
Publisher Name: Springer, Cham
Print ISBN: 978-3-319-28623-5
Online ISBN: 978-3-319-28624-2
eBook Packages: MedicineMedicine (R0)