Identification of the multivalent PDZ protein PDZK1 as a binding partner of sodium–coupled monocarboxylate transporter SMCT1 (SLC5A8) and SMCT2 (SLC5A12)

被引:0
作者
Sunena Srivastava
Kiyoshi Nakagawa
Xin He
Toru Kimura
Toshiyuki Fukutomi
Seiji Miyauchi
Hiroyuki Sakurai
Naohiko Anzai
机构
[1] Kyorin University School of Medicine,Department of Pharmacology and Toxicology
[2] Chiba University Graduate School of Medicine,Department of Pharmacology
[3] Tianjin University of Traditional Chinese Medicine,School of Chinese Materia Medica
[4] Toho University,Department of Pharmaceutics, Faculty of Pharmaceutical Sciences
来源
The Journal of Physiological Sciences | 2019年 / 69卷
关键词
Monocarboxylates; Monocarboxylate transporter; SMCT; Lactate; PDZ; PDZK1;
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摘要
Sodium-coupled monocarboxylate transporters SMCT1 (SLC5A8) and SMCT2 (SLC5A12) mediate the high- and low-affinity transport of lactate in the kidney, but their regulatory mechanism is still unknown. Since these two transporters have the PDZ-motif at their C-terminus, the function of SMCTs may be modulated by a protein–protein interaction. To investigate the binding partner(s) of SMCTs in the kidney, we performed yeast two-hybrid (Y2H) screenings of a human kidney cDNA library with the C-terminus of SMCT1 (SMCT1-CT) and SMCT2 (SMCT2-CT) as bait. PDZK1 was identified as a partner for SMCTs. PDZK1 coexpression in SMCT1-expressing HEK293 cells enhanced their nicotinate transport activity. PDZK1, SMCT1, and URAT1 in vitro assembled into a single tri-molecular complex and their colocalization was confirmed in the renal proximal tubule in vivo by immunohistochemistry. These results indicate that the SMCT1-PDZK1 interaction thus plays an important role in both lactate handling as well as urate reabsorption in the human kidney.
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页码:399 / 408
页数:9
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