A biokinetic and dosimetric model for ionic indium in humans

Andersson, Martin; Mattsson, Sören; Johansson, Lennart; Leide-Svegborn, Sigrid

A biokinetic and dosimetric model for ionic indium in humans

Mark

Andersson, Martin ^LU ; Mattsson, Sören ^LU ; Johansson, Lennart and Leide-Svegborn, Sigrid ^LU (2017) In Physics in Medicine and Biology 62(16). p.6397-6407

Abstract: This paper reviews biokinetic data for ionic indium, and proposes a biokinetic model for systemic indium in adult humans. The development of parameter values focuses on human data and indium in the form of ionic indium(III), as indium chloride and indium arsenide. The model presented for systemic indium is defined by five different pools: plasma, bone marrow, liver, kidneys and other soft tissues. The model is based on two subsystems: one corresponding to indium bound to transferrin and one where indium is transported back to the plasma, binds to red blood cell transferrin and is then excreted through the kidneys to the urinary bladder. Absorbed doses to several organs and the effective dose are calculated for ¹¹¹In- and... (More); This paper reviews biokinetic data for ionic indium, and proposes a biokinetic model for systemic indium in adult humans. The development of parameter values focuses on human data and indium in the form of ionic indium(III), as indium chloride and indium arsenide. The model presented for systemic indium is defined by five different pools: plasma, bone marrow, liver, kidneys and other soft tissues. The model is based on two subsystems: one corresponding to indium bound to transferrin and one where indium is transported back to the plasma, binds to red blood cell transferrin and is then excreted through the kidneys to the urinary bladder. Absorbed doses to several organs and the effective dose are calculated for ¹¹¹In- and ^113mIn-ions. The proposed biokinetic model is compared with previously published biokinetic indium models published by the ICRP. The absorbed doses are calculated using the ICRP/ICRU adult reference phantoms and the effective dose is estimated according to ICRP Publication 103. The effective doses for ¹¹¹In and ^113mIn are 0.25 mSv MBq^-1 and 0.013 mSv MBq^-1 respectively. The updated biokinetic and dosimetric models presented in this paper take into account human data and new animal data, which represent more detailed and presumably more accurate dosimetric data than that underlying previous models for indium.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/e8e4b816-b8fa-4b39-96f6-1084dd952507

author

Andersson, Martin ^LU ; Mattsson, Sören ^LU ; Johansson, Lennart and Leide-Svegborn, Sigrid ^LU

organization

publishing date

2017-07-20

type

Contribution to journal

publication status

published

subject

keywords

absorbed dsoe, biokinetic model, effective dose, indium

in

Physics in Medicine and Biology

volume

62

issue

16

pages

11 pages

publisher

IOP Publishing

external identifiers

pmid:28726676
scopus:85026788703

ISSN

0031-9155

DOI

10.1088/1361-6560/aa779f

language

English

LU publication?

yes

id

e8e4b816-b8fa-4b39-96f6-1084dd952507

date added to LUP

2017-08-25 15:45:54

date last changed

2024-02-29 20:32:58

@article{e8e4b816-b8fa-4b39-96f6-1084dd952507,
  abstract     = {{<p>This paper reviews biokinetic data for ionic indium, and proposes a biokinetic model for systemic indium in adult humans. The development of parameter values focuses on human data and indium in the form of ionic indium(III), as indium chloride and indium arsenide. The model presented for systemic indium is defined by five different pools: plasma, bone marrow, liver, kidneys and other soft tissues. The model is based on two subsystems: one corresponding to indium bound to transferrin and one where indium is transported back to the plasma, binds to red blood cell transferrin and is then excreted through the kidneys to the urinary bladder. Absorbed doses to several organs and the effective dose are calculated for <sup>111</sup>In- and <sup>113m</sup>In-ions. The proposed biokinetic model is compared with previously published biokinetic indium models published by the ICRP. The absorbed doses are calculated using the ICRP/ICRU adult reference phantoms and the effective dose is estimated according to ICRP Publication 103. The effective doses for <sup>111</sup>In and <sup>113m</sup>In are 0.25 mSv MBq<sup>-1</sup> and 0.013 mSv MBq<sup>-1</sup> respectively. The updated biokinetic and dosimetric models presented in this paper take into account human data and new animal data, which represent more detailed and presumably more accurate dosimetric data than that underlying previous models for indium.</p>}},
  author       = {{Andersson, Martin and Mattsson, Sören and Johansson, Lennart and Leide-Svegborn, Sigrid}},
  issn         = {{0031-9155}},
  keywords     = {{absorbed dsoe; biokinetic model; effective dose; indium}},
  language     = {{eng}},
  month        = {{07}},
  number       = {{16}},
  pages        = {{6397--6407}},
  publisher    = {{IOP Publishing}},
  series       = {{Physics in Medicine and Biology}},
  title        = {{A biokinetic and dosimetric model for ionic indium in humans}},
  url          = {{http://dx.doi.org/10.1088/1361-6560/aa779f}},
  doi          = {{10.1088/1361-6560/aa779f}},
  volume       = {{62}},
  year         = {{2017}},
}

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A biokinetic and dosimetric model for ionic indium in humans