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. 2018 Oct 2;9(77):34641. doi: 10.18632/oncotarget.26214

Correction: Screening of cancer tissue arrays identifies CXCR4 on adrenocortical carcinoma: correlates with expression and quantification on metastases using 64Cu-plerixafor PET

Ido D Weiss 1, Lyn M Huff 2, Moses O Evbuomwan 3, Xin Xu 1, Hong Duc Dang 1, Daniel S Velez 1, Satya P Singh 1, Hongwei H Zhang 1, Paul J Gardina 4, Jae-Ho Lee 5, Liza Lindenberg 6, Timothy G Myers 4, Chang H Paik 5, David S Schrump 7, Stefania Pittaluga 3, Peter L Choyke 6, Tito Fojo 2, Joshua M Farber 1
PMCID: PMC6195380  PMID: 30349656

This article has been corrected: On page 73395, the following sentences have been updated to read, “Dosimetry for 64Cu-plerixafor calculated from this single patient gave an Effective Dose of 0.283 rem/mCi, and a total of 2.43 rem from the dose of 8.6 mCi. The organs that contributed the most to the Effective Dose were the liver and bone marrow (0.0606 and 0.0760 rem/mCi, respectively)”.

Similar to results in mice, the liver had the highest uptake of the tracer, with unbound tracer excreted through the kidneys [31, 32]. Significant uptake was also seen in organs of the immune system, including spleen, vertebral bodies (bone marrow), and lymph nodes (Figure 4 and Supplementary Figure 6). Of additional interest, uptake of 64Cu-plerixafor was absent from a number of vertebral bodies in the thoracolumbar spine that were within the region of prior radiation therapy (Figure 4 and Supplementary Figure 6). Dosimetry for 64Cu-plerixafor calculated from this single patient gave an Effective Dose of 0.283 rem/mCi, and a total of 2.43 rem from the dose of 8.6 mCi. The organs that contributed the most to the Effective Dose were the liver and bone marrow (0.0606 and 0.0760 rem/mCi, respectively). PET/CT sections (Figure 4B) showed variable uptake in the multiple pulmonary nodules.

Original article: Oncotarget. 2017; 8:73387-73406. https://doi.org/10.18632/oncotarget.19945


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