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Query: UMLS:C0153690 (
bone metastases
)
6,382
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Combined Tc-99m MDP skeletal imaging and Tc-99m(V)
DMSA
whole body scans to detect metastases were performed during the follow-up of 30 patients who underwent surgery for breast carcinoma. Eight patients had normal Tc-99m MDP and Tc-99m(V)
DMSA
scans and were declared free of metastatic disease, further confirmed by no change in symptomatology over a 1-year follow-up period. Twenty-two patients had positive Tc-99m MDP scans with varied skeletal involvement. Tc-99m(V)
DMSA
scans showed matched areas of increased radiotracer concentration in bony metastases in 20 of these patients. Tc-99m(V)
DMSA
concentration was not seen in traumatic vertebral collapse or in coexistent osteoarthritic disease in vertebral metastatic involvement. Interestingly, Tc-99m(V)
DMSA
showed increased concentration in brain and liver metastases. Pentavalent Tc-99m(V)
DMSA
appears useful for detecting skeletal and soft-tissue metastases in breast carcinoma, and can improve the specificity of Tc-99m MDP bone scans in screening for
bone metastases
.
...
PMID:Tc-99m(V) DMSA imaging. A new approach to studying metastases from breast carcinoma. 131 48
The purpose of this investigation was to characterise the in vivo chemistry and binding mechanisms of technetium-99m dimercaptosuccinic acid [99mTc(V)
DMSA
]. Biodistribution was studied in mice by frozen section whole-body autoradiography and microautoradiography in selected tissues. Binding to bone mineral analogues was studied in vitro using various forms of calcium phosphate and hydroxyapatite under varied conditions. Similar studies with 99mTc-hydroxymethylene diphosphonate (HDP) were also carried out for comparison. The in vivo stability of 99mTc(V)
DMSA
was monitored by high-performance liquid chromatographic analysis of blood and urine samples taken over 24 h from patients injected with the tracer. Whole-body autoradiography shows that 99mTc(V)
DMSA
has highest affinity for bone (cortical rather than medullary) in mice. Substantial uptake of the tracer was also observed in the kidney (cytoplasm of cortical renal tubular cells). No specific localisation was observed in the liver at either the microscopic or the macroscopic level. While 99mTc-HDP bound strongly to calcium phosphates under all conditions, 99mTc(V)
DMSA
binding was inhibited in the presence of phosphate and was stronger at pH 6.0 than at pH 7. 4. In non-phosphate buffers, however, the binding of 99mTc(V)
DMSA
remained high across the pH range 4-7.4. 99mTc(V)
DMSA
binds to calcium phosphates chemically unaltered, and no radioactive species other than the three isomers of 99mTc(V)
DMSA
were detected in blood or urine samples taken from patients up to 24 h after injection. 99mTc(V)
DMSA
is stable in vivo, and no conversion of the complex to other chemical species needs to be invoked to explain its uptake in
bone metastases
or soft tissue tumour. Bone affinity may be due to reversible binding of the unaltered complex to the mineral phase of bone.
...
PMID:In vitro and in vivo studies with pentavalent technetium-99m dimercaptosuccinic acid. 892 10
Pentavalent 99Tcm-dimercaptosuccinic acid (99Tcm-(V)
DMSA
) has an established role in imaging medullary thyroid carcinoma. There have been case reports of uptake in
bone metastases
. Our aims were to compare 99Tcm-(V)
DMSA
with 99Tcm-hydroxymethylene diphosphonate (99Tcm-HDP) in
bone metastases
, to assess its value in imaging of
bone metastases
, and to assess the prospects of the beta-emitting analogues 186/188Re-(V)
DMSA
as palliative agents for painful
bone metastases
. Ten patients confirmed by a 99Tcm-HDP bone scan to have
bone metastases
secondary to carcinoma of the prostate, lung or breast were injected with 99Tcm-(V)
DMSA
(600 MBq). Whole-body scans acquired at 3 and 24 h were compared with the 99Tcm-HDP bone scans. 99Tcm-(V)
DMSA
showed high soft tissue background, kidney retention and avid uptake in most
bone metastases
: 86% of bone lesions identified on bone scans were detected with 99Tcm-(V)
DMSA
. The lesion-to-normal ratios were comparable to or lower than those for 99Tcm-HDP at 3 h, but increased by 24 h. Instances of abnormal uptake in liver, primary lung tumour, lymph nodes and pleural effusion were observed. We conclude that 99Tcm-(V)
DMSA
is a tracer for
bone metastases
(with lower sensitivity than 99Tcm-HDP) and soft tissue tumours. If 186/188Re-(V)
DMSA
behave similarly, they may find use in therapy for soft tissue tumours and bony metastases.
...
PMID:Pentavalent 99Tcm-DMSA imaging in patients with bone metastases. 939 90
Pentavalent rhenium-188 dimercaptosuccinic acid [188Re(V)
DMSA
] is a beta-emitting analogue of 99mTc(V)
DMSA
, a tracer that is taken up in a variety of tumours and
bone metastases
. The aim of this study was to develop the kit-based synthesis of the agent on a therapeutic scale, to assess its stability in vivo, and to obtain preliminary biodistribution and dosimetry estimates, prior to evaluation of its potential as a targeted radiotherapy agent. The organ distribution of 188Re in mice was determined 2 h after injection of 3 MBq 188Re(V)
DMSA
prepared from eluate from a 188W/188Re generator. Three patients with cancer of the prostate and three with cancer of the bronchus, all with
bone metastases
confirmed with a standard 99mTc-hydroxymethylene diphosphonate (99mTc-HDP) scan, were given 370 MBq 188Re(V)
DMSA
and imaged at 3 h and 24 h using the 155-keV gamma-photon (15%). Blood and urine samples were collected to determine clearance and to analyse the speciation of 188Re. Organ residence times were estimated from the scans, and used to estimate radiation doses using MIRDOSE 3. In mice, 188Re(V)
DMSA
was selective for bone and kidney. In patients, it showed selectivity for
bone metastases
(particularly those from prostate carcinoma) and kidney, but uptake in normal bone was not significantly greater than in surrounding soft tissues. Of the normal tissues the kidneys received the highest radiation dose (0.5-1.3 mGy/MBq). The images were strongly reminiscent of 99mTc(V)
DMSA
scans in similar patients. High-performance liquid chromatography analysis of blood and urine showed no evidence of 188Re in any chemical form other than 188Re(V)
DMSA
up to 24 h. In conclusion, 188Re(V)
DMSA
and its 186Re analogue warrant further clinical assessment as generator/kit-derived agents for treatment of painful
bone metastases
. These agents should also be assessed in medullary thyroid carcinoma and other soft tissue tumours which have been shown to accumulate 99mTc(V)
DMSA
.
...
PMID:Pentavalent rhenium-188 dimercaptosuccinic acid for targeted radiotherapy: synthesis and preliminary animal and human studies. 961 76
The aim of this study was to establish the value of 99Tcm(V)-
DMSA
scintigraphy in the detection of metastatic bone lesions and compare the results to 99Tcm-MDP bone scintigraphy. Thirty-four patients presenting with metastatic bone disease (Group 1) and 12 controls with degenerative skeletal lesions (Group 2) were studied. Conventional bone scanning and 99Tcm(V)-
DMSA
whole-body scanning were performed on all patients. All scans were interpreted visually. Furthermore, lesion-to-normal bone ratios (L/N) in vertebral metastases on the 4 and 24 h bone scans were obtained in 58 lesions of cancer patients and in 23 benign (degenerative) vertebral lesions of the control group. 99Tcm-MDP L/N ratios at 24 h (3.08 +/- 0.32) were significantly higher than those at 4 h (2.48 +/- 0.24) in the malignant foci (P < 0.001). No significant difference was observed in benign lesions (P > 0.05). In 167 (164 metastatic, 3 traumatic) of 186 99Tcm-MDP positive lesions (90%) of Group 1, 99Tcm(V)-
DMSA
uptake was observed. The remaining 19 lesions (10%) were 99Tcm(V)-
DMSA
negative. Fourteen of these 19 sites were diagnosed as benign. The remaining five foci were malignant. In four lung cancer metastases showing no 99Tcm-MDP uptake, 99Tcm(V)-
DMSA
uptake was observed. There was no 99Tcm(V)-
DMSA
accumulation in any of the 99Tcm-MDP positive degenerative lesions of Group 2. All quantitatively evaluated (n = 42) vertebral metastatic foci and two compression fractures in Group 1 showed 99Tcm(V)-
DMSA
accumulation and an increased 99Tcm-MDP L/N ratio at 24 h. A total of 36 degenerative lesions (Groups 1 and 2) and one compression fracture (Group 1) showed neither 99Tcm(V)-
DMSA
uptake nor an increased 99Tcm-MDP L/N ratio at 24 h. Our results indicate that quantitative 4/24 h analysis of vertebral lesions on 99Tcm-MDP scans has a similar diagnostic value to 99Tcm(V)-
DMSA
imaging in the detection of
bone metastases
. However, the accumulation of 99Tcm(V)-
DMSA
in four lung cancer metastases showing no 99Tcm-MDP uptake is encouraging and justifies further research in patients with proven
bone metastases
and negative bone scans.
...
PMID:Evaluation of metastatic bone disease with pentavalent 99Tc(m)-dimercaptosuccinic acid: a comparison with whole-body scanning and 4/24 hour quantitation of vertebral lesions. 1082 27
Rhenium-188 dimercaptosuccinic acid complex [188Re(V)
DMSA
], a potential therapeutic analogue of the tumour imaging agent 99mTc(V)
DMSA
, is selectively taken up in
bone metastases
in patients with prostate cancer. It would be helpful in planning palliative radionuclide therapy if 99mTc(V)
DMSA
could be used to predict tumour and kidney retention of 188Re(V)
DMSA
. The aim of this study was to determine the correlation between tumour-to-normal tissue ratios and kidney-to-soft tissue ratios of 99mTc(V)
DMSA
and 188Re(V)
DMSA
. This would determine whether a scan with 99mTc(V)
DMSA
could be used to identify patients for whom 188Re(V)
DMSA
treatment would be contra-indicated, and enable prediction of relative kidney and tumour radiation absorbed dose in 188Re(V)
DMSA
treatment. Ten patients with prostate carcinoma were recruited following observation of disseminated
bone metastases
on a recent 99mTc-hydroxydiphosphonate bone scan. Whole-body planar scans were obtained at ca. 4 h and 24 h after hydration and injection of 600 MBq 99mTc(V)
DMSA
, and a week later, at similar times after hydration and injection of 370 MBq 188Re(V)
DMSA
. A triple-energy window (TEW) scatter correction was applied to the 188Re scans. Counts per pixel were determined in regions of interest drawn over metastatic sites, kidneys and normal soft tissue. Tumour-to-soft tissue ratios were significantly lower (by a factor of approximately 0.8 after the TEW was applied) on 188Re scans than on 99mTc scans, but the two were highly linearly correlated both in all individual patients and in tumours pooled from all patients together both at 4 h and at 24 h. Kidney-to-soft tissue ratios were similarly correlated and were lower for 188Re than for 99mTc by a similar factor. Both tumour- and kidney-to-soft tissue ratios increased between 4 and 24 h but the latter increased more. In conclusion, only minor differences were seen between 99mTc and 188Re scans, and kidney-to-background ratios on 188Re scans were not higher than on 99mTc scans. These differences are insufficient to infer that they are due to a real difference in biodistribution, and they may be due only to different physical imaging characteristics. Thus 99mTc(V)
DMSA
scans are predictive of 188Re(V)
DMSA
biodistribution and could be used to estimate tumour and renal dosimetry and assess suitability of patients for 188Re(V)
DMSA
treatment.
...
PMID:99mTc(V)DMSA quantitatively predicts 188Re(V)DMSA distribution in patients with prostate cancer metastatic to bone. 1100 25
Starting from our previous finding that 99mTc(V) dimercaptosuccinic acid (99mTc(V)-
DMSA
), a useful agent for the localization of osteosarcoma and
bone metastases
, loses its bone affinity when one ester group is introduced into the complex we studied the impact of esterification in more detail. This paper reports on the evaluation of various ester complexes of 99mTc(V)-
DMSA
in rats and tumour-bearing nude mice with regard to their tumour retention and improvement of the tumour to tissue ratios. The distribution patterns of the complexes [99mTcO(
DMSA
)2]- (A), [99mTcO(
DMSA
/DMSEt)]- (B) and [99mTcO(DMSEt)2]- (C) are gradually changed with the number of ester groups in the anionic complex. However, the asymmetric diester complex [99mTcO(
DMSA
/DMSEt2)]- (D) is very slowly cleared, especially from the blood of nude mice. Moreover, this complex differs significantly from the symmetrical complex C in its elimination behaviour from the liver and kidneys. The tumour uptake is maintained with complexes that contain one or two non-hydrolysable ester functions. Preliminary biodistribution studies of the monoethyl and diethyl ester complexes B, C and D in comparison with A in tumour-bearing nude mice showed similar uptake into the human squamous cell carcinoma (FaDu) as well as into the human colonic cell carcinoma (HT29) of nude mice. The low bone accumulation of B, C and D results in excellent tumour-to-bone ratios, e.g., approx. 3:1 for the ester complex B compared to approx. 1:2 for complex A. Differences were observed in the accumulation and elimination behaviour of the complexes A and B in various bone structures of rats. The age-dependent uptake of A and B was compared in long bone (femur) and in cranial bone of rats. The results suggest that 99mTc(V)-
DMSA
complexes that contain a functional ester, and their 188Re analogues, may be superior to 99mTc(V)/188Re(V)-
DMSA
in diagnostic and therapeutic nuclear medicine.
...
PMID:Novel tumortropic ester derivatives of 99mTc(V) mesodimercapto succinic acid with low affinity for bone tissue. 1456 72
In order to find the conditions under which Tc-99m-methylenediphosphonate (Tc-99m-MDP) and Tc-99m(V)-dimercaptosuccinate (Tc-99m(V)-
DMSA
) may become tumour-seeking agents, leaving healthy organs free from the radionuclide uptake, the solution chemistry of these radiopharmaceuticals was studied by paper chromatography and paper electrophoresis in distilled water, in physiological saline, in NAHCO3, and ascorbic acid solutions. Both radiopharmaceuticals are anionic in the radiopharmaceutical solution but get easily hydrolysed to form cationic Tc-99m species which concentrates in healthy bone and in some
bone metastases
. Tc-99m (V)-
DMSA
being more stable remains long in the blood pool giving undesirable presence of the radionuclide in lung, heart and kidneys, in addition to its reduced uptake in
bone metastases
and in some primaries. We are trying to eliminate these drawbacks of healthy organ uptake of Tc-99-m(V)-
DMSA
not only to get a clean scintigraphic image of the tumour with this radiopharmaceutical but to extend its formulation, thus obtained, to prepare radiopharmaceutical with Re-188, which is the higher homologue of Tc-99m, for systemic therapy of cancer. Essentially similar solution chemistry of both radiopharmaceuticals suggests that like Tc-99m-MDP, technetium-99m-dimercaptosuccinate is also a complex of tetravalent Tc-99m and not of pentavalent Tc-99m as so far supposed to be.
...
PMID:Paper chromatographic and paper elettrophoretic study of the solution chemistry of Tc-99m-methylendiphosphonate and of Tc-99m-dimercaptosuccinate for improving the tumour-affinity of Tc-99m during scintigraphic imaging of cancer. 1550 27
We report a patient with DTPA and
DMSA
uptake on unsuspected
bone metastases
. He had severe pain due to grade 3 hydronephrosis of his left kidney. When Tc-99m DTPA and
DMSA
renal scanning were performed for preoperative evaluation, abnormal radiopharmaceutical uptake on the iliac area was noted. Pancreatic adenocarcinoma metastases to bone were subsequently defined. This patient is a very demonstrative case in respect of having all DTPA,
DMSA
and HDP uptakes in
bone metastases
. The type of the tumor has to be added to the list of extrarenal uptake of DTPA and
DMSA
as a rare cause.
...
PMID:Incidental DTPA and DMSA uptake during renal scanning in unknown bone metastases. 1687 10
Scintigraphy of the skeletal system is performed mainly with the use of 99mTc-MDP. There are other radiopharmaceuticals showing affinity to bone lesions: 99mTc-MIBG, 201Tl, 131I (in the case of papillary or follicular thyroid cancers), and 99mTc (V)
DMSA
(in the case of medullary cancer). Currently, positron emitted radioisotopes are also used in clinical practice. It seems that 18F-NaF/PET is a highly sensitive and specific modality for detection of metastases and other bone lesions. Certain data concerning the role of 18F-FDG, 18F-choline, or 68Ga-DOTATATE can be found. The aim of this article is to review the role of 18F-NaF and 18F-FDG in diagnosis of
bone metastases
.
...
PMID:Bone metastases diagnosis possibilities in studies with the use of 18F-NaF and 18F-FDG. 2221 51
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