. Author manuscript; available in PMC: 2021 Dec 23.

Published in final edited form as: Nature. 2021 Jun 16;594(7863):385–390. doi: 10.1038/s41586-021-03551-x

Table 1|.

Set of available PDB structures of CLC-ec1 at various conditions. The RMSD values are calculated for backbone atoms with respect to the PDB 1OTS structure as reference.

PDB ID	PH	Mutations	Ions	BB RMSD (Å)
1OTS	9.5		NaCI	reference
1KPK	8.5		Na₂SO₄ / Li₂SO₄	0.785
1KPL^*	4.6	M26L/C264V	Na₂SO₄ / Li₂SO₄	1.169
1OTT	9.5	E148A	NaCI	0.465
1OTU	9.5	E148Q	NaCI	0.589
2EXY	8.5	E148Q	TART	0.646
2EZ0	9.5	S107A/E148Q/Y445A	NaBr	0.722
2FEC	7.5	E203Q	NaBr	0.425
2FED	7.5	E203Q	NaCI	0.427
2FEE	7.5		NaBr	0.362
2H2P	7.5		KSCN	0.515
2H2S	7.5	E148A	KSeCN	0.491
2HLF	9.5	Y445E	NaBr	0.378
2HT2	8.5	Y445H	TART	0.654
2HT3	7.5	Y445L	TART	0.581
2HT4	8.0	Y445W	NaBr	0.533
2HTK	8.5	Y445A	TART	0.378
2R9H	9.5	Q207C	NaCI / TART	0.558
3DET	5.5	E148A / Y445A	KCI	0.415
3EJY	9.5		NaBr	0.425
3EJZ	8.5	E203V	NaBr	0.426
3NMO^†	9.5		LiNO₃	0.565
4ENE	8.5		CaCI₂	0.442
4FTP	9.5	E202Y		0.877
4KJP	9.5			0.412
4KK5	9.0		NaF / NaBr	0.282
4KK8	8.5	E148Q	NaF	0.422
4KKB	7.0	E148A	NaF / NaBr	0.454
4KKC	9.0	E148A	NaBr	0.679
5HD8	9.0	D417C	TART	0.597

Denotes a low-pH structure of CLC from Salmonella typhimurium.

^†

Denotes structures of monomers. All CLC X-ray structures exhibited essentially identical conformations. However, NMR, computational and biochemical studies have suggested larger-scale movements. A recent X-ray structure of a ClC-ec1 triple mutant (E148Q/E203Q/E113Q) that mimics the protonation of essential glutamates at low pH, reports global conformational changes that lead to opening of the extracellular permeation pathway.⁴⁵ Thus, under the assumption that the displacements of surface features are signatures of movements in the underlying helices, our LAFM maps suggest motions that could result in changes in the region of the extracellular gate.