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	Figure 1. Schematic topology of the HCN4 and MiRP1 proteins. The HCN4 α-subunit has six transmembrane segments (S1–S6), a pore-forming loop (P) and intracellular N- and C-termini. The voltage sensor of the channel is formed by the positively-charged S4 helix. The C-terminus comprises the C-linker (dotted line) and the cyclic nucleotide-binding domain (cNBD), which is known to mediate cyclic AMP (cAMP)-dependent changes in HCN channel gating. The MiRP1 β-subunit has a single transmembrane segment with an extracellular N-terminus and intracellular C-terminus. Red dots indicate the location of the 23 known HCN4 and MiRP1 mutation sites associated with clinically established or potential sinus node dysfunction. The split dots indicate the truncations resulting from the 573X and 695X non-sense (truncating) mutations.
	Figure 2. Membrane currents of a human sinoatrial node (SAN) pacemaker cell assessed by a simulated action potential clamp. (A) Action potentials recorded from a human SAN pacemaker cell used for the action potential clamp; (B) associated rate of change of the membrane potential (dVm/dt); (C) global intracellular calcium concentration ([Ca2+]i) in a different cell with a highly similar cycle length; and (D) numerically reconstructed membrane current (Im): L-type calcium current (ICa,L), If, delayed rectifier potassium current (IKr) and net membrane current (Inet). See the text for details.
	Figure 3. Effect of mutations in HCN4 on If in a human SAN pacemaker cell assessed by simulated action potential clamp. (A) Action potentials recorded from a human SAN pacemaker cell used for action potential clamp; (B) computed wild-type (WT) If of a human SAN pacemaker cell during the action potentials of (A) under control conditions (“control”, blue line) and upon adrenergic stimulation (“cAMP”, red line); (C–H) computed If of a human SAN pacemaker cell carrying heterozygous mutation in HCN4, as indicated, during the action potentials of (A) under control conditions (solid blue line) and upon adrenergic stimulation (solid red line). Wild-type If of (B) under control conditions (dashed blue line) and upon adrenergic stimulation (dashed red line) are shown for reference. G482R traces, labelled “a” and “b”, are based on data from Milano et al. [27] and Schweizer et al. [28], respectively.
	Figure 4. Contribution of If to diastolic depolarization for each of the heterozygous mutations in HCN4 or KCNE2. The charge carried by If (Qf) during the 25-mV, 550-ms spontaneous depolarization from the maximum diastolic potential of −63 mV of the human SAN action potential is as indicated in Figure 3A. The blue bars are computed from the If traces under control conditions (“control”). The red bars are computed from the If traces upon adrenergic stimulation (“cAMP”). The dashed grey line indicates the charge of 0.025 pC/pF carried by the net membrane current (Qnet) during the 25-mV depolarization. (A) Mutations of Figure 3; (B) mutations assessed in previous publication [30].

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