Nucleation rate and Gibbs free energy of nucleation of APIs, large molecule, amino acid and inorganic materials in solution at different cooling rates

Abstract

We propose a new mathematical model based on the classical nucleation theory to predict the nucleation rate, kinetic constant, and Gibbs free energy of nucleation using metastable zone width (MSZW) data as a function of solubility temperature. Unlike widely used models by Nývlt, Kubota, and Sangwal, which are limited in capturing the impact of varying cooling rates, the proposed model allows direct estimation of nucleation rates from MSZW data obtained under different cooling conditions. This is particularly advantageous for continuous or semi-batch crystallisation design, where cooling rate is a critical variable. The model has been successfully validated using experimental data from 22 solute–solvent systems, including 10 APIs, one API intermediate, lysozyme, and glycine, as well as 8 inorganic compounds. Predicted nucleation rates span from 10²⁰ to 10²⁴ molecules per m³ s for APIs, and up to 10³⁴ molecules per m³ s for lysozyme, the largest molecule studied. Gibbs free energy of nucleation varies from 4 to 49 kJ mol⁻¹ for most compounds, reaching 87 kJ mol⁻¹ for lysozyme. The model also enables accurate prediction of induction time and key thermodynamic parameters such as surface free energy, critical nucleus size, and number of unit cells—based solely on MSZW data obtained at different cooling rates.

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In this communication, we propose a useful mathematical model to predict the nucleation rate and Gibbs free energy of nucleation from metastable zone width (MSZW) values measured at different cooling rates. The model is validated using a broad dataset comprising 11 different active pharmaceutical ingredients (APIs)/solvent combinations involving 10 active pharmaceutical ingredients (APIs), 8 inorganic compound–solvent systems, one API intermediate, one amino acid, and one large molecule. The MSZW is crucial in crystallization processes because it defines the range of supersaturation where no spontaneous nucleation occurs, but crystal growth is possible.^1–4 MSZW helps to determine the precise supersaturation levels to avoid spontaneous nucleation, which can lead to undesirable crystal sizes or polymorphs.^5–7 Operating within the MSZW allows controlled crystal growth, ensuring consistent size and quality of the crystals. On the theoretical side, MSZW allows to calculate the nucleation rate which is a key factor in understanding and optimising the crystallisation.⁵ Theoretically the nucleation rate is obtained using the MSZW measured at different cooling rates using theoretical models that includes the one developed by Nývlt,⁸ Sangwal,⁹ and Kubota.¹ These models allow to theoretically calculate the nucleation rate kinetic constant and the order of nucleation.^1,8–21 Moreover, these models relate the MSZW obtained at fixed saturation temperature with the rate of cooling. It will be useful to develop a theoretical model that can theoretically determine the nucleation rate at different cooling rates. Thus, to complement the established model of Nývlt, Sangwal and Kubota, we present a new mathematical model based on the classical nucleation theory that allows to calculate nucleation rate at different cooling rates using the MSZW data collected from different solubility onset temperature. Unlike existing models, which do not explicitly account for cooling rate, our approach directly incorporates its influence, enabling accurate prediction of nucleation rates across varying cooling conditions. Furthermore, as the model rely on the classical nucleation theory, it immediately allows to theoretically calculate the Gibbs free energy of nucleation as a function of temperature and supersaturation at the point of nucleation. From the Gibbs free energy, it is possible to calculate the surface free energy or the interfacial tension and the radius of the critical nucleus as a function of the operating variables that mainly include the supersaturation and the temperature at which the nucleation is observed. To demonstrate the usefulness and universality of the proposed model, it was applied to experimental MSZW data from 22 different solute–solvent combinations. This dataset includes 10 different APIs across 11 API–solvent systems, eight inorganic compound–solvent combinations, as well as one API intermediate (L-arabinose), one amino acid (glycine), and one large biomolecule (lysozyme). The MSZW data, reported at different cooling rates, were used to extract key nucleation parameters, including the nucleation rate kinetic constant, Gibbs free energy of nucleation (ΔG), surface energy, and the critical nucleus radius, all evaluated as functions of supersaturation and nucleation temperature.

The metastable zone widths (MSZW) of solutions containing these single-component compounds, experimentally measured using the polythermal method, were obtained from the literature.^22–32 This method involves changing the temperature of the solution from a reference solubility temperature at a predefined cooling rate and detecting the onset of nucleation at T_nuc.⁹ The relationship between the reference solution temperature, temperature at which nucleation can be observed or detected is shown in Fig. 1. In Fig. 1, we also showed the line of supersolubility concentration, solubility concentration and their relationship with the MSZW, ΔT_max and the supersaturation at the MSZW, ΔC_max.

Fig. 1 The relationship between solubility concentration, c* and solubility temperature, T*. Also shown in the figures are the different parameters that can be experimentally fixed or obtained and their relationship between the MSZW (or ΔT_max = − T_nuc) and the supersaturation (or ) at the MSZW.

According to the classical nucleation theory, the nucleation rate is defined as

J = k_n exp(−ΔG/RT) (1)

During the cooling the crystallization, the undersaturated solution will be cooled from approximately + 5 °C at a fixed cooling rate of dT*/dt until the nucleation or the phase change is observed or can be experimentally detected measured in the solution. The temperature where the nucleation is observed is T_nuc. So, at the point of nucleation, T = T_nuc and thus eqn (1) becomes:

J = k_n exp(−ΔG/RT_nuc) (2)

The nucleation rate can be defined in terms of cooling rate, and the slope of solubility curve as followsFrom eqn (2) and (3), it is possible to write thatAt the point of nucleation,where, is the MSZW and Δc_max is the supersaturation (or the driving force required for crystallization) achieved at T_nuc, where primary nucleation is most likely to occur. The relationship between the solubility concentration c* and the parameters that include T*, , T_nuc, and MSZW (i.e., ΔT_max) and the supersaturation concentration at ΔT_max (i.e., Δc_max) are given in Fig. 1.

Substituting eqn (5) in (4), we get

Eqn (6) can be linearized as follows:From eqn (7), it is immediately evident that the model explicitly incorporates the cooling rate, along with the metastable zone width (ΔT_max), supersaturation at ΔT_max, and the nucleation temperature, to predict the nucleation rate constant (k_n) and related parameters under varying experimental conditions. Importantly, eqn (7) establishes a direct link between key nucleation parameters such as the nucleation rate constant (k_n), Gibbs free energy of nucleation (ΔG), and induction time (as later shown in eqn (12)) and experimentally measurable quantities. Theoretically, a plot of ln(ΔC_max/ΔT_max) versus 1/T_nuc should be linear with a negative slope whose value will be equal to ΔG/R with an intercept equal to ln(k_n). Once the nucleation kinetic constant, k_n and the ΔG is determined, then mathematically it is possible to estimate at the nucleation rate J using eqn (2) at a fixed cooling rate R′ and the MSZW measured at different (and the corresponding T_nuc). Furthermore, from the classical nucleation theory, it is also possible to calculate the surface energy, or the interfacial tension associated with the formation of stable nucleus using the expression:⁹Once the surface energy is calculated using eqn (8), we can mathematically calculate the radius of the critical nucleus using the expression:⁹In Fig. 2a and b, we showed the plot of ln(ΔC_max/ΔT_max) versus 1/T_nuc for 11 different combinations of APIs and solvents. In Fig. 2c and d we showed the plot of ln(ΔC_max/ΔT_max) versus 1/T_nuc for 8 combinations of inorganic compounds and solvents, as well as for one API intermediate (L-arabinose), one amino acid (glycine) and a large biomolecule (lysozyme). The ΔC_max, ΔT_max, and the corresponding nucleation temperature during the crystallization of these different compounds from their solution and the solvents involved are given in Table 1. All the experimental values were obtained from literature (see Table 1). From Fig. 2, it is evident that the proposed model provides an excellent fit to the experimental data across all systems studied, regardless of the nature of the solutes (APIs, inorganic compounds, or biomolecules), the solvents used, or the specific experimental conditions, including the studied cooling rates. From Fig. 2 and using eqn (7) we calculated the nucleation rate kinetic constant, k_n and the Gibbs free energy of nucleation, ΔG. The calculated k_n, ΔG and the corresponding r² values are given in Table 1. In most cases the coefficient of determination was always greater than 0.97, indicating the proposed model provides an excellent representation of the experimental data across systems studied including API/solvent combinations, inorganic compounds, the API intermediate, the amino acid (glycine) and lysozyme. While some systems, such as lysozyme/NaCl, demonstrate a very high coefficient of determination (r² = 0.9952), others, like NaNO₃/NaCl–H₂O, show relatively lower but still acceptable values (e.g., r² = 0.8911 – see Table 1). In crystallisation studies, particularly those relying on thermodynamic or kinetic parameters derived from indirect measurements such as MSZW, an r² ≥ 0.9 is generally considered indicative of a strong model fit. The observed variation in r² across different systems does not point to a fundamental limitation of the proposed model but rather reflects statistical constraints inherent to linear regression when applied over narrow MSZW or solubility ranges. Specifically, systems with limited experimental variability, where MSZW data span only a small solubility temperature range are more susceptible to experimental noise, leading to slightly lower r² values. This is a well-recognised limitation of linear regression, which benefits from broader data coverage to enhance fit robustness. For example, in the CoSO₄/water and NaNO₃/NaCl–H₂O systems, ΔT_max showed minimal change across the studied solubility concentrations. Moreover, in these systems, ΔT_max does not increase consistently with solubility temperature, which disrupts the expected linear trend and leads to greater deviation when the data are transformed and fitted using eqn (7). This inconsistency contributes to higher residuals and reduces the overall r² value. Theoretically, nucleation depends on multiple interconnected factors, including the degree of supercooling, nucleation temperature (T_nuc), reference solubility temperature , solubility concentration at (i.e., ), supersaturation at the T_nuc (i.e., Δc_max), and cooling rate. The proposed model performs particularly well in systems where ΔT_max increases with solubility temperature, regardless of the applied cooling rate supporting its general applicability across a wide range of crystallisation scenarios.

Fig. 2 Plot of ln(ΔC_max/ΔT_max) + ln(R′) versus 1/T_nuc for (a) 6 different combinations of API and solvents involving 4 APIs, (b) 11 different combinations of API and solvents involving 6 APIs, (c) combination of inorganics/solvents involving 8 different compounds and (d) API intermediate, amino acid and a large molecule. Note: these values are valid only at the cooling rates studied given in Table 1. Fig. 2a: : paracetamol/water (R′: 0.5 K s⁻¹); : dextrose/water (R′: 0.0278 K s⁻¹); : L-asparagine monohydrate/water (R′: 0.005 K s⁻¹); : L-asparagine monohydrate/water (R′: 0.0033 K s⁻¹). Fig. 2b: : ibuprofen/ethanol (R′: 0.0167 K s⁻¹); : paracetamol/ethanol (R′: 0.0167 K s⁻¹); : pyrazinamide/acetone (R′: 0.0167 K s⁻¹); : fenofibrate/ethyl acetate (R′: 0.05 K s⁻¹); : gestodene/ethanol (R′: 0.0083 K s⁻¹); : gestodene/ethanol (R′: 0.005 K s⁻¹); : carbamazepine_saccharine/ethanol (R′: 0.0167 K s⁻¹); : pyrazinamide/acetone (R′: 0.0033 K s⁻¹); : gestodene/ethanol (R′: 0.00167 K s⁻¹). Fig. 2c: : NaNO₃/NaCl + NaNO₃ + H₂O solution (R′: 0.000833 K s⁻¹); : NaNO₃/NaCl + NaNO₃ + H₂O solution (R′: 0.001667 K s⁻¹); : CoSO₄/water (R′: 0.000833 K s⁻¹); : CoSO₄/water (R′: 0.001667 K s⁻¹); : CoSO₄/water (R′: 0.0025 K s⁻¹); : (NH₄)₂B₄O₇·4H₂O/water (R′: 0.00833 K s⁻¹); : (NH₄)₂B₄O₇·4H₂O/water (R′: 0.0025 K s⁻¹); : Na₃VO₄/NaOH solution (R′: 0.005 K s⁻¹); : Sr(OH)₂·8H₂O/water (R′: 0.001388 K s⁻¹); : Sr(OH)₂·8H₂O/water (R′: 0.00277 K s⁻¹); : ZnL₂/water (R′: 0.00138 K s⁻¹); : ZnL₂/water (R′: 0.00275 K s⁻¹); : borax/water (R′: 0.003472 K s⁻¹); : borax/water (R′: 0.01066 K s⁻¹); : ammonium oxalate/water (R′: 0.000833 K s⁻¹ – plotted in secondary axis). Fig. 2d: : L-arabinose/water (R′: 0.0083 K s⁻¹); : glycine/water (R′: 0.001667 K s⁻¹); : glycine/water (R′: 0.005 K s⁻¹); : lysozyme/NaCl solution (R′: 0.002778 K s⁻¹ – we assumed this cooling rate – shown in secondary axis).

Table 1 Nucleation parameters as a function of cooling rate obtained using the proposed model as in eqn (7) for 11 different combinations of APIs/solvents that involve 10 APIs, 8 inorganic compounds in their solution, an API intermediate, amino acid and lysozyme (a large molecule)

API/solvent	R′, K s^−1	k n, m^−3 s^−1	T nuc, K		Δcmax, molecules per m^3	ΔTmax, K	ΔG, kJ mol^−1	J, m^−3 s^−1	γ , mJ m^−2	r c, m	V ^1/3cell, m	λ = 2rc/V^1/3cell	N m/V	t ind, s	r ^2	Ref.
Note: the unit cell volumes of all compounds studied were obtained from the crystallographic information files (CIFs) retrieved from the International Centre for Diffraction Data (ICDD) powder diffraction file (PDF-5+, 2025), using the database tools provided by the ICDD.
Psilocybin/water	0.0167	6.4 × 10^32	326.02	3.86	6.6 × 10^25	14.87	62.1	7.12 × 10^22	28.35	9.32 × 10^−10	1.38 × 10^−9	1.35	6.35 × 10^25	892	0.9789	23
			330.35	3.13	7.2 × 10^25	12.38		9.63 × 10^22	25.55	9.82 × 10^−10		1.42	7.15 × 10^25	743
			332.70	2.83	7.63 × 10^25	11.38		1.13 × 10^23	24.13	1.01 × 10^−9		1.46	7.71 × 10^25	683
			334.91	2.61	8.17 × 10^25	11.01		1.3 × 10^23	22.98	1.04 × 10^−9		1.50	8.65 × 10^25	661
			338.30	2.21	8.31 × 10^25	9.01		1.64 × 10^23	20.39	1.10 × 10^−9		1.59	8.85 × 10^25	541
			341.90	1.87	8.2 × 10^25	6.09		2.06 × 10^23	17.52	1.19 × 10^−9		1.72	7.55 × 10^25	366
Paracetamol/ethanol	0.0167	2.3 × 10^26	285.21	1.59	5.14 × 10^26	22.99	15.22	3.75 × 10^23	7.97	8.70 × 10^−10	1.14 × 10^−9	1.51	5.17 × 10^26	1379	0.9823	23
			288.86	1.54	5.13 × 10^26	21.05		4.06 × 10^23	7.63	8.90 × 10^−10		1.54	5.14 × 10^26	1263
			296.63	1.38	4.72 × 10^26	15.61		4.80 × 10^23	6.42	9.70 × 10^−10		1.68	4.50 × 10^26	937
			299.74	1.41	5.2 × 10^26	16.85		5.11 × 10^23	6.75	9.46 × 10^−10		1.64	5.18 × 10^26	1011
			303.93	1.41	5.72 × 10^26	16.70		5.56 × 10^23	6.81	9.41 × 10^−10		1.63	5.58 × 10^26	1002
			304.63	1.49	6.56 × 10^26	19.73		5.64 × 10^23	7.55	8.94 × 10^−10		1.55	6.68 × 10^26	1184
			310.22	1.54	7.76 × 10^26	21.05		6.29 × 10^23	8.00	8.69 × 10^−10		1.50	7.95 × 10^26	1263
Pyrazinamide/acetone	0.0016	1.7 × 10^25	294.45	1.10	3.5 × 10^24	3.68	22.63	1.64 × 10^21	3.31	1.65 × 10^−9	8.30 × 10^−10	3.97	3.62 × 10^24	2210	0.9007	30
			299.72	1.11	4.4 × 10^24	3.60		1.92 × 10^21	3.42	1.62 × 10^−9		3.9	4.17 × 10^24	2162
			305.51	1.07	3.85 × 10^24	2.89		2.29 × 10^21	2.75	1.81 × 10^−9		4.36	3.97 × 10^24	1734
			311.14	1.05	2.97 × 10^24	2.26		2.69 × 10^21	2.05	2.09 × 10^−9		5.05	3.65 × 10^24	1354
Pyrazinamide/acetone	0.0033	2.4 × 10^25	292.70	1.18	5.67 × 10^24	5.43	21.42	3.62 × 10^21	4.56	1.37 × 10^−9	8.30 × 10^−10	3.29	5.90 × 10^24	1628	0.9602	30
			298.10	1.18	6.93 × 10^24	5.23		4.25 × 10^21	4.59	1.36 × 10^−9		3.28	6.67 × 10^24	1568
			303.73	1.15	7.24 × 10^24	4.67		4.99 × 10^21	4.19	1.43 × 10^−9		3.43	7.00 × 10^24	1402
			309.84	1.10	6.08 × 10^24	3.56		5.89 × 10^21	3.28	1.61 × 10^−9		3.88	6.31 × 10^24	1069
L-Asparagine monohydrate/water	0.0016	1.3 × 10^28	290.65	1.27	2.16 × 10^25	4.40	34.69	7.81 × 10^21	6.79	1.42 × 10^−9	8.67 × 10^−10	3.28	2.06 × 10^25	2639	0.9723	24
			297.87	1.26	2.92 × 10^25	5.11		1.11 × 10^22	6.75	1.43 × 10^−9		3.29	3.39 × 10^25	3068
			303.94	1.22	3.22 × 10^25	4.05		1.46 × 10^22	6.13	1.50 × 10^−9		3.46	3.56 × 10^25	2433
			308.46	1.20	3.68 × 10^25	3.50		1.78 × 10^22	5.90	1.53 × 10^−9		3.52	3.76 × 10^25	2098
			315.24	1.17	4.24 × 10^25	2.76		2.39 × 10^22	5.38	1.60 × 10^−9		3.69	3.96 × 10^25	1654
L-Asparagine monohydrate/water	0.0033	2.5 × 10^28	288.69	1.39	2.88 × 10^25	6.36	34.55	1.42 × 10^22	8.38	1.28 × 10^−9	8.67 × 10^−10	2.95	2.71 × 10^25	1907	0.9887	24
			294.24	1.49	4.67 × 10^25	8.74		1.86 × 10^22	9.66	1.19 × 10^−9		2.75	4.88 × 10^25	2622
			301.39	1.37	4.90 × 10^25	6.60		2.6 × 10^22	8.36	1.28 × 10^−9		2.95	5.15 × 10^25	1980
			305.81	1.36	5.83 × 10^25	6.15		3.17 × 10^22	8.28	1.29 × 10^−9		2.97	5.86 × 10^25	1844
			313.68	1.26	6.02 × 10^25	4.32		4.46 × 10^22	6.92	1.41 × 10^−9		3.25	5.79 × 10^25	1295
L-Asparagine monohydrate/water	0.005	1.6 × 10^28	284.41	1.70	4.19 × 10^25	10.64	32.35	1.87 × 10^22	11.13	1.07 × 10^−9	8.67 × 10^−10	2.48	3.99 × 10^25	2127	0.9891	24
			292.21	1.64	5.53 × 10^25	10.77		2.69 × 10^22	10.84	1.09 × 10^−9		2.51	5.82 × 10^25	2154
			299.61	1.49	5.95 × 10^25	8.38		3.75 × 10^22	9.52	1.16 × 10^−9		2.68	6.28 × 10^25	1676
			302.44	1.59	8.21 × 10^25	9.52		4.23 × 10^22	10.61	1.10 × 10^−9		2.54	8.06 × 10^25	1904
			312.16	1.35	7.63 × 10^25	5.84		6.32 × 10^22	8.09	1.26 × 10^−9		2.91	7.38 × 10^25	1168
Dextrose/water	0.0027	1.9 × 10^24	286.42	1.25	3.28 × 10^26	17.01	8.55	5.41 × 10^22	3.99	9.22 × 10^−10	7.57 × 10^−10	2.44	3.31 × 10^25	6124	0.9824	29
			290.45	1.26	3.64 × 10^26	17.03		5.68 × 10^22	4.16	9.03 × 10^−10		2.39	3.49 × 10^26	6131
			294.52	1.25	3.70 × 10^26	17.07		5.97 × 10^22	4.12	9.07 × 10^−10		2.40	3.67 × 10^26	6144
			298.60	1.24	3.76 × 10^26	16.55		6.26 × 10^22	4.08	9.12 × 10^−10		2.41	3.73 × 10^26	5958
			302.46	1.23	3.80 × 10^26	16.36		6.54 × 10^22	4.03	9.18 × 10^−10		2.42	3.86 × 10^26	5889
Paracetamol/water	0.5	7.2 × 10^27	292.08	1.66	3.16 × 10^25	14.85	21.34	1.09 × 10^24	9.58	9.40 × 10^−10	1.14 × 10^−9	1.64	3.24 × 10^26	30	0.9951	29
			296.03	1.78	4.30 × 10^25	16.99		1.22 × 10^24	10.57	8.95 × 10^−10		1.56	4.16 × 10^26	34
			304.37	1.49	3.56 × 10^25	11.65		1.55 × 10^24	8.40	1.00 × 10^−9		1.75	3.62 × 10^25	23
			303.19	1.61	4.29 × 10^25	14.21		1.50 × 10^24	9.47	9.46 × 10^−10		1.65	4.28 × 10^25	28
			313.66	1.32	3.22 × 10^25	8.12		1.99 × 10^24	6.77	1.12 × 10^−9		1.95	3.24 × 10^25	16
			318.36	1.28	3.32 × 10^25	7.37		2.25 × 10^24	6.34	1.16 × 10^−9		2.02	3.32 × 10^25	15
			321.35	1.22	2.80 × 10^25	4.77		2.42 × 10^24	5.48	1.24 × 10^−9		2.17	2.32 × 10^25	10
Gestodene form1/ethanol	0.0017	1.6 × 10^25	301.58	1.41	2.67 × 10^25	11.43	20.90	3.81 × 10^21	7.49	1.05 × 10^−9	1.20 × 10^−9	1.75	2.62 × 10^25	6857	0.9814	25
			308.32	1.33	2.62 × 10^25	9.71		4.57 × 10^21	6.70	1.11 × 10^−9		1.85	2.67 × 10^25	5829
			315.44	1.25	2.43 × 10^25	7.62		5.51 × 10^21	5.75	1.20 × 10^−9		2	2.52 × 10^25	4571
			321.62	1.22	2.59 × 10^25	6.54		6.42 × 10^21	5.43	1.24 × 10^−9		2.06	2.52 × 10^25	3924
Gestodene form1/ethanol	0.0050	3.4 × 10^25	298.15	1.56	3.31 × 10^25	14.86	19.95	1.09 × 10^22	8.70	9.54 × 10^−10	1.20 × 10^−9	1.59	3.25 × 10^25	2971	0.99	25
			305.02	1.46	3.36 × 10^25	13.02		1.31 × 10^22	7.98	9.96 × 10^−10		1.66	3.41 × 10^25	2603
			312.40	1.36	3.28 × 10^25	10.67		1.57 × 10^22	7.07	1.06 × 10^−9		1.76	3.37 × 10^25	2133
			319.46	1.30	3.33 × 10^25	8.70		1.87 × 10^22	6.41	1.11 × 10^−9		1.85	3.26 × 10^25	1740
Gestodene form1/ethanol	0.0083	2.5 × 10^25	296.18	1.65	3.64 × 10^25	16.83	19.15	1.06 × 10^22	9.27	9.05 × 10^−10	1.20 × 10^−9	1.51	2.15 × 10^25	2019	0.9896	25
			303.62	1.52	3.65 × 10^25	14.41		1.28 × 10^22	8.40	9.51 × 10^−10		1.59	2.23 × 10^25	1730
			311.76	1.39	3.45 × 10^25	11.30		1.56 × 10^22	7.25	1.02 × 10^−9		1.71	2.13 × 10^25	1356
			318.83	1.32	3.53 × 10^25	9.33		1.84 × 10^22	6.61	1.07 × 10^−9		1.79	2.07 × 10^25	1120
Fenofibrate/ethyl acetate	0.0050	3.1 × 10^27	279.80	2.59	1.07 × 10^27	27.37	22.51	1.94 × 10^23	14.43	7.87 × 10^−10	9.92 × 10^−10	1.586	1.07 × 10^27	5474	0.999	31
			284.53	2.54	1.23 × 10^27	27.00		2.28 × 10^23	14.43	7.87 × 10^−10		1.586	1.24 × 10^27	5400
			287.48	2.52	1.33 × 10^27	26.63		2.52 × 10^23	14.42	7.87 × 10^−10		1.587	1.34 × 10^27	5327
			290.16	2.49	1.44 × 10^27	26.53		2.75 × 10^23	14.40	7.88 × 10^−10		1.588	1.46 × 10^27	5306
			292.79	2.47	1.55 × 10^27	26.11		2.99 × 10^23	14.38	7.88 × 10^−10		1.588	1.56 × 10^27	5222
			295.26	2.45	1.67 × 10^27	25.79		3.24 × 10^23	14.38	7.88 × 10^−10		1.589	1.67 × 10^27	5159
			296.89	2.43	1.75 × 10^27	25.64		3.40 × 10^23	14.37	7.88 × 10^−10		1.589	1.74 × 10^27	5127
Vismodegib/MIBK	0.0167	1.5 × 10^30	345.96	2.71	2.74 × 10^25	19.04	51.54	2.48 × 10^22	22.62	9.51 × 10^−10	1.28 × 10^−9	1.49	2.84 × 10^25	1142	0.9975	28
			349.89	2.32	3.92 × 10^25	21.12		3.07 × 10^22	20.35	1.00 × 10^−9		1.57	3.85 × 10^25	1267
			354.00	2.13	5.08 × 10^25	22.10		3.73 × 10^22	19.10	1.03 × 10^−9		1.62	4.95 × 10^25	1326
			372.98	3.86	3.24 × 10^25	6.02		9.09 × 10^22	29.14	8.38 × 10^−10		1.31	3.28 × 10^25	361
			379.98	5.82	2.30 × 10^25	7.98		1.23 × 10^23	35.20	7.62 × 10^−10		1.19	5.92 × 10^25	479
Carbamazepine–saccharin cocrystal/water	0.0167	9.1 × 10^25	297.27	1.84	7.27 × 10^24	19.17	23.70	6.24 × 10^21	11.39	9.08 × 10^−10	1.57 × 10^−9	1.16	8.34 × 10^26	415	0.9865	32
			298.89	1.80	7.32 × 10^24	18.66		6.57 × 10^21	11.15	9.18 × 10^−10		1.17	9.74 × 10^26	419
			300.00	1.78	7.42 × 10^24	18.33		6.81 × 10^21	11.03	9.23 × 10^−10		1.18	1.08 × 10^27	411
			301.23	1.77	7.69 × 10^24	18.27		7.08 × 10^21	11.01	9.24 × 10^−10		1.18	1.15 × 10^27	384
			302.46	1.76	7.93 × 10^24	18.07		7.36 × 10^21	10.97	9.26 × 10^−10		1.18	1.31 × 10^27	380
			303.37	1.77	8.26 × 10^24	18.10		7.57 × 10^21	11.03	9.23 × 10^−10		1.18	1.53 × 10^27	376
			303.85	1.77	8.41 × 10^24	18.10		7.68 × 10^21	11.05	9.22 × 10^−10		1.18	1.73 × 10^27	372
Ibuprofen/ethanol	0.0167	1.7 × 10^30	287.99	1.58	8.37 × 10^26	6.91	32.75	2.09 × 10^24	10.27	1.12 × 10^−9	1.36 × 10^−9	1.65	7.18 × 10^24	1150	0.9994	26
			291.09	1.59	9.66 × 10^26	6.98		2.32 × 10^24	10.40	1.12 × 10^−9		1.64	7.36 × 10^24	1120
			293.67	1.58	1.07 × 10^27	6.85		2.62 × 10^24	10.39	1.12 × 10^−9		1.64	7.49 × 10^24	1100
			296.64	1.56	1.16 × 10^27	6.40		2.99 × 10^24	10.24	1.13 × 10^−9		1.66	7.77 × 10^24	1096
			299.74	1.55	1.30 × 10^27	6.33		3.43 × 10^24	10.21	1.13 × 10^−9		1.66	7.98 × 10^24	1084
			303.68	1.54	1.53 × 10^27	6.27		4.07 × 10^24	10.25	1.13 × 10^−9		1.66	8.22 × 10^24	1086
			306.79	1.53	1.72 × 10^27	6.20		4.65 × 10^24	10.21	1.13 × 10^−9		1.66	8.34 × 10^24	1086
NaNO3/NaCl–NaNO3–H2O solution	0.00083	1.7 × 10^24	282.1	1.06	2.24 × 10^26	5.99	9.23	3.29 × 10^22	1.69	1.47 × 10^−9	7.6 × 10^−10	3.89	2.37 × 10^26	7188	0.9226	54
			287.7	1.06	2.39 × 10^26	5.65		3.55 × 10^22	1.71	1.46 × 10^−9		3.87	2.41 × 10^26	6780
			298.8	1.04	1.96 × 10^26	4.73		4.10 × 10^22	1.40	1.61 × 10^−9		4.27	2.33 × 10^26	5676
			303.0	1.03	1.55 × 10^26	3.86		4.32 × 10^22	1.17	1.77 × 10^−9		4.67	2.00 × 10^26	4632
			305.7	1.03	1.32 × 10^26	3.6		4.45 × 10^22	1.04	1.87 × 10^−9		4.96	1.92 × 10^26	4320
			309.2	1.02	1.24 × 10^26	2.66		4.64 × 10^22	0.97	1.94 × 10^−9		5.13	1.48 × 10^26	3192
NaNO3/NaCl–NaNO3–H2O solution	0.001667	2.2 × 10^23	281.06	1.08	2.74 × 10^26	7.06	4.45	3.30 × 10^22	1.52	1.08 × 10^−9	7.6 × 10^−10	2.8	1.40 × 10^26	4236	0.8911	54
			286.9	1.07	2.76 × 10^26	6.39		3.44 × 10^22	1.48	1.09 × 10^−9		2.9	1.32 × 10^26	3834
			298	1.05	2.42 × 10^26	5.52		3.68 × 10^22	1.27	1.18 × 10^−9		3.1	1.22 × 10^26	3312
			302.3	1.04	1.96 × 10^26	4.52		3.78 × 10^22	1.08	1.28 × 10^−9		3.4	1.03 × 10^26	2712
			308.9	1.03	1.45 × 10^26	2.99		3.92 × 10^22	0.85	1.44 × 10^−9		3.8	7.04 × 10^25	1794
Ammonium oxalate monohydrate/water	0.00083	1.0 × 10^29	299.36	1.40	7.34 × 10^25	1.16	30.07	5.64 × 10^23	8.28	1.20 × 10^−9	6.8 × 10^−10	3.53	7.88 × 10^25	139.7	0.9335	55
			300.45	1.40	7.62 × 10^25	1.00		5.89 × 10^23	8.33	1.20 × 10^−9		3.52	7.09 × 10^25	120.4
			302.41	1.41	8.23 × 10^25	1.08		6.37 × 10^23	8.47	1.19 × 10^−9		3.49	8.29 × 10^25	130.1
			306.15	1.40	8.98 × 10^25	0.96		7.37 × 10^23	8.46	1.19 × 10^−9		3.49	8.52 × 10^25	115.6
			308.75	1.39	9.40 × 10^25	1.00		8.15 × 10^23	8.38	1.19 × 10^−9		3.51	9.82 × 10^25	120.5
L-Arabinose/water	0.0022	8.7 × 10^25	306.84	1.60	2.15 × 10^27	26.04	15.84	1.76 × 10^23	8.53	8.58 × 10^−10	8.5 × 10^−10	2.01	2.06 × 10^27	11 718	0.9615	56
			311.19	1.61	2.38 × 10^27	28.12		1.92 × 10^23	8.72	8.48 × 10^−10		1.99	2.42 × 10^27	12 654
			315.54	1.63	2.62 × 10^27	28.68		2.08 × 10^23	8.89	8.40 × 10^−10		1.97	2.69 × 10^27	12 906
			320.08	1.64	2.89 × 10^27	29.06		2.27 × 10^23	9.06	8.32 × 10^−10		1.96	2.97 × 10^27	13 077
			325	1.64	3.19 × 10^27	28.68		2.49 × 10^23	9.20	8.26 × 10^−10		1.94	3.21 × 10^27	12 906
			329.73	1.66	3.55 × 10^27	28.12		2.70 × 10^23	9.41	8.17 × 10^−10		1.92	3.42 × 10^27	12 654
Cobalt sulfate/water	0.00083	2.3 × 10^24	284.13	1.09	1.32 × 10^26	9.14	12.28	1.30 × 10^22	2.39	1.43 × 10^−9	6.5 × 10^−10	4.39	1.43 × 10^26	10 965	0.9407	15
			290.27	1.10	1.50 × 10^26	7.99		1.45 × 10^22	2.54	1.38 × 10^−9		4.26	1.39 × 10^26	9583
			296.80	1.08	1.28 × 10^26	6.30		1.63 × 10^22	2.25	1.47 × 10^−9		4.53	1.23 × 10^26	7556
			310.01	1.04	7.46 × 10^25	3.22		2.01 × 10^22	1.51	1.80 × 10^−9		5.53	7.78 × 10^25	3870
Cobalt sulfate/water	0.00167	1.5 × 10^24	282.75	1.10	1.50 × 10^26	10.52	9.59	2.56 × 10^22	2.40	1.26 × 10^−9	6.5 × 10^−10	3.87	1.61 × 10^26	6313	0.9399	15
			288.12	1.12	1.80 × 10^26	10.14		2.76 × 10^22	2.64	1.20 × 10^−9		3.69	1.67 × 10^26	6083
			293.27	1.11	1.80 × 10^26	9.83		2.96 × 10^22	2.60	1.21 × 10^−9		3.73	1.74 × 10^26	5897
			308.40	1.06	1.01 × 10^26	4.84		3.59 × 10^22	1.70	1.49 × 10^−9		4.60	1.04 × 10^26	2902
Cobalt sulfate/water	0.0025	9.8 × 10^23	279.83	1.13	1.88 × 10^26	13.44	7.63	3.70 × 10^22	2.58	1.08 × 10^−9	6.5 × 10^−10	3.33	1.99 × 10^26	5375	0.9453	57
			285.05	1.15	2.22 × 10^26	13.21		3.93 × 10^22	2.82	1.04 × 10^−9		3.19	2.08 × 10^26	5283
			289.20	1.15	2.37 × 10^26	13.90		4.12 × 10^22	2.90	1.02 × 10^−9		3.14	2.29 × 10^26	5559
			296.72	1.12	1.97 × 10^26	11.52		4.46 × 10^22	2.52	1.10 × 10^−9		3.37	2.06 × 10^26	4607
			306.78	1.07	1.27 × 10^26	6.45		4.94 × 10^22	1.84	1.28 × 10^−9		3.94	1.27 × 10^26	2580
Glycine/water	0.00167	2.4 × 10^25	293.86	1.19	3.82 × 10^26	8.94	14.29	7.00 × 10^22	4.11	1.17 × 10^−9	6.9 × 10^−10	3.40	3.76 × 10^26	5365	0.9905	57
			303.32	1.16	3.96 × 10^26	8.06		8.40 × 10^22	3.85	1.21 × 10^−9		3.51	4.06 × 10^26	4833
			311.52	1.14	4.02 × 10^26	6.87		9.76 × 10^22	3.60	1.25 × 10^−9		3.63	4.02 × 10^26	4123
			318.61	1.13	4.06 × 10^26	6.06		1.10 × 10^23	3.39	1.29 × 10^−9		3.74	4.01 × 10^26	3636
Glycine/water	0.005	1.8 × 10^25	290.75	1.26	4.95 × 10^26	12.05	13.54	6.76 × 10^22	4.86	1.05 × 10^−9	6.9 × 10^−10	3.04	1.63 × 10^26	2409	0.9927	57
			300.95	1.22	4.99 × 10^26	10.42		8.17 × 10^22	4.46	1.10 × 10^−9		3.18	1.70 × 10^26	2084
			309.75	1.18	4.92 × 10^26	8.65		9.53 × 10^22	4.08	1.15 × 10^−9		3.32	1.65 × 10^26	1729
			316.62	1.17	5.22 × 10^26	8.06		1.07 × 10^23	3.97	1.16 × 10^−9		3.37	1.72 × 10^26	1611
Na3VO4/NaOH solution	0.005	4.6 × 10^30	306.55	1.16	1.23 × 10^25	6.39	49.94	1.44 × 10^22	5.76	1.85 × 10^−9	7.6 × 10^−10	4.88	1.84 × 10^25	1279	0.98	58
			314.08	1.63	6.84 × 10^25	8.98		2.30 × 10^22	13.06	1.23 × 10^−9		3.24	4.13 × 10^25	1795
			330.52	1.70	1.58 × 10^26	12.42		5.95 × 10^22	14.31	1.18 × 10^−9		3.10	1.48 × 10^26	2484
			340.55	1.63	2.19 × 10^26	12.79		1.02 × 10^23	13.73	1.20 × 10^−9		3.16	2.60 × 10^26	2557
Ammonium biborate tetrahydrate/water	0.00083	4.2 × 10^25	283.53	1.21	3.03 × 10^25	9.50	22.72	2.76 × 10^21	5.01	1.34 × 10^−9	3.6 × 10^−10	7.27	3.14 × 10^25	11 396	0.9981	59
			287.85	1.24	4.03 × 10^25	10.14		3.19 × 10^21	5.49	1.28 × 10^−9		6.95	3.88 × 10^25	12 173
			293.03	1.23	4.56 × 10^25	9.93		3.77 × 10^21	5.36	1.30 × 10^−9		7.03	4.49 × 10^25	11 914
			306.07	1.15	4.64 × 10^25	6.98		5.61 × 10^2	4.21	1.46 × 10^−9		7.93	4.70 × 10^25	8375
Ammonium biborate tetrahydrate/water	0.0025	3.4 × 10^26	281.37	1.31	4.08 × 10^25	11.66	24.71	8.86 × 10^21	6.40	1.24 × 10^−9	3.6 × 10^−10	6.71	4.13 × 10^25	4662	0.9988	59
			285.90	1.33	5.14 × 10^25	12.09		1.05 × 10^22	6.75	1.21 × 10^−9		6.53	5.06 × 10^25	4834
			290.80	1.33	6.08 × 10^25	12.16		1.25 × 10^22	6.81	1.20 × 10^−9		6.50	6.07 × 10^25	4863
			303.69	1.25	7.18 × 10^25	9.35		1.93 × 10^22	5.92	1.29 × 10^−9		6.98	7.20 × 10^25	3741
Lysozyme/NaCl solution	0.00028	1.1 × 10^34	300.86	1.82	2.80 × 10^23	9.52	87.15	8.15 × 10^18	17.5	1.41 × 10^−9	7.1 × 10^−9	0.39	2.79 × 10^23	26	0.9952	60
			303.92	2.80	4.12 × 10^23	10.45		1.16 × 10^19	19.4	1.34 × 10^−9		0.37	4.35 × 10^23	29
			306.43	2.54	7.47 × 10^23	14.15		1.54 × 10^19	23.8	1.21 × 10^−9		0.34	7.82 × 10^23	35
			307.74	3.13	1.12 × 10^24	17.66		1.78 × 10^19	27.3	1.13 × 10^−9		0.32	1.13 × 10^24	39
			308.96	3.62	1.15 × 10^24	20.43		2.03 × 10^19	29.6	1.08 × 10^−9		0.30	1.49 × 10^24	42
Sr(OH)2·8H2O/water	0.00139	1.4 × 10^24	279.65	1.31	2.57 × 10^24	7.37	18.62	4.76 × 10^20	5.81	1.13 × 10^−9	9.8 × 10^−10	2.30	2.52 × 10^24	5306	0.9981	61
			292.96	1.15	2.13 × 10^24	4.39		6.85 × 10^20	3.96	1.37 × 10^−9		2.79	2.16 × 10^24	3161
			305.02	1.08	1.79 × 10^24	2.76		9.26 × 10^20	2.75	1.64 × 10^−9		3.35	1.84 × 10^24	1987
			316.88	1.02	7.03 × 10^23	1.06		1.22 × 10^21	1.14	2.54 × 10^−9		5.18	9.30 × 10^23	763
			327.63	1.01	6.52 × 10^23	0.58		1.54 × 10^21	0.85	2.94 × 10^−9		6.00	6.42 × 10^23	418
Sr(OH)2·8H2O/water	0.00278	3.5 × 10^22	279.11	1.34	2.81 × 10^24	8.09	8.51	9.90 × 10^22	4.77	8.42 × 10^−10	9.8 × 10^−10	1.72	2.88 × 10^26	2912	0.9802	61
			291.81	1.21	2.77 × 10^24	5.64		1.16 × 10^23	3.67	9.59 × 10^−10		1.96	2.36 × 10^26	2030
			303.57	1.14	2.87 × 10^24	4.13		1.33 × 10^23	2.94	1.07 × 10^−9		2.19	1.98 × 10^26	1487
			316.08	1.05	1.71 × 10^24	1.87		1.52 × 10^23	1.61	1.45 × 10^−9		2.96	1.02 × 10^26	673
			327.28	1.02	1.13 × 10^24	0.84		1.70 × 10^23	0.95	1.88 × 10^−9		3.84	5.14 × 10^25	302
Zinc lactate/water	0.002775	8.9 × 10^24	300.78	1.30	1.14 × 10^25	11.32	20.16	2.80 × 10^21	6.25	2.27 × 10^−9	1.1 × 10^−9	2.06	1.14 × 10^25	4080.4	0.99832	62
			319.68	1.34	1.97 × 10^25	12.32		4.52 × 10^21	6.88	2.15 × 10^−9		1.96	2.01 × 10^25	4438.7
			308.81	1.37	1.67 × 10^25	13.29		3.46 × 10^21	7.08	2.12 × 10^−9		1.93	1.66 × 10^25	4789.9
			329.97	1.40	2.97 × 10^25	14.23		5.72 × 10^21	7.74	2.03 × 10^−9		1.85	2.93 × 10^25	5127.7
Zinc lactate/water	0.003472	1.1 × 10^25	299.18	1.35	1.29 × 10^25	12.92	19.99	3.46 × 10^21	6.78	2.16 × 10^−9	1.1 × 10^−9	1.97	1.29 × 10^25	3722.2	0.9984	62
			318.00	1.39	2.20 × 10^25	14.00		5.56 × 10^21	7.45	2.06 × 10^−9		1.88	2.24 × 10^25	4032.9
			307.11	1.42	1.84 × 10^25	14.99		4.25 × 10^21	7.62	2.04 × 10^−9		1.85	1.84 × 10^25	4317.2
			328.25	1.45	3.26 × 10^25	15.95		7.04 × 10^21	8.30	1.95 × 10^−9		1.78	3.23 × 10^25	4594.0
Borax/water	0.0033	1.4 × 10^27	278.32	1.65	2.28 × 10^25	10.78	28.07	7.69 × 10^21	9.97	1.06 × 10^−9	1.2 × 10^−9	1.83	2.50 × 10^25	3235	0.9982	63
			282.02	1.62	2.66 × 10^25	10.66		9.03 × 10^21	9.99	1.06 × 10^−9		1.83	2.89 × 10^25	3198
			288.28	1.48	2.62 × 10^25	8.35		1.17 × 10^22	8.61	1.14 × 10^−9		1.97	2.93 × 10^25	2504
			292.35	1.43	2.85 × 10^25	7.68		1.38 × 10^22	8.22	1.16 × 10^−9		2.01	3.17 × 10^25	2303
			295.62	1.41	3.13 × 10^25	7.31		1.56 × 10^22	8.01	1.18 × 10^−9		2.04	3.43 × 10^25	2193
Borax/water	0.01067	2.3 × 10^27	273.93	2.01	2.93 × 10^25	15.17	26.28	2.22 × 10^22	12.12	9.27 × 10^−10	1.2 × 10^−9	1.60	3.16 × 10^24	1422	0.9967	63
			279.98	1.86	3.21 × 10^25	13.71		2.74 × 10^22	11.47	9.53 × 10^−10		1.65	3.52 × 10^25	1285
			285.23	1.69	3.35 × 10^25	11.39		3.51 × 10^22	10.29	1.01 × 10^−9		1.74	3.75 × 10^25	1068
			288.94	1.67	3.83 × 10^25	11.09		4.04 × 10^22	10.19	1.01 × 10^−9		1.75	4.20 × 10^25	1039
			292.76	1.60	4.10 × 10^25	10.17		4.67 × 10^22	9.71	1.04 × 10^−9		1.79	4.45 × 10^25	954

---

The ΔG values typically range from 8 to 62 kJ mol⁻¹ for the APIs, 13.5 for amino acid, 15.84 kJ mol⁻¹ for the API intermediate. The ΔG values for the inorganic compounds range from 4.45 to ∼50 kJ mol⁻¹. Most of these values agree with the ΔG values reported for several organic/inorganic compounds.^7,33–51 Furthermore, we also noticed that there doesn't exist a perfect correlation between the molecular weight and the Gibbs free energy of nucleation (see Table 1). However, the ΔG values are higher for compounds with higher molecular weight. Noticeably for the case of the largest molecule studied (lysozyme), eqn (7) predicted a ΔG value of 87 kJ mol⁻¹. This agrees with the classical nucleation theory which states that the higher the molecular volume is tougher in the nucleation. The surface energy, calculated using our model in conjunction with classical nucleation theory, ranges from 0.8517 mJ m⁻² to 35.2 mJ m⁻² across all systems studied. The radius of the critical nucleus of all the studied APIs, API intermediate, amino acid and lysozyme was found to be in the range of ∼10⁻¹⁰ m to ∼10⁻⁹ m. Similar magnitudes were also observed for the inorganic compounds, indicating that the critical nucleus size remains within the nanometre scale across both organic and inorganic solutes. Using the size of the critical radius, we mathematically estimated the number of unit cells constituting the critical nucleus. This was done by calculating the normalized critical nucleus size (λ), defined as the ratio of the diameter of the stable nucleus (2r_c) to the cube root of the unit cell volume, V_cell. The unit cell volumes for the API crystals were obtained from their respective crystallographic information files (CIF file) (see Table 1). Finally, using this normalized size, the approximate number of unit cells in the critical nucleus was calculated as equal to λ.³ This estimation provides a simple theoretical approximation of the structural size of the critical nucleus in terms of unit cells. Note that, this approach assumes that the spherical critical nucleus has a diameter approximately equal to that of a cube-shaped nucleus composed of unit cells arranged in a simple cubic packing, i.e., the linear dimension of the nucleus is equivalent in both cases. This simplification allows for a geometric approximation of the number of unit cells. While this is a simplification and does not account for molecular packing or anisotropic crystal structures, it provides a first-order estimate of the number of unit cells that compose the critical radius. As shown in Table 1, the estimated diameter of the critical nucleus corresponds to approximately 1–5 times the average linear dimension of a unit cell for all the API–solvent systems studied. For the API–solvent combinations considered, the nucleus is estimated to consist of approximately 1 to 125 unit cells, calculated as λ.³ For inorganic compounds, where λ was found to range from 2 to 8, the critical nucleus is estimated to consist of approximately 8 to 512 unit cells, which is notably larger than the corresponding values estimated for the organic compounds. In the case of small organic molecules such as L-arabinose and glycine (excluding the large biomolecule lysozyme), the critical nucleus was estimated to contain approximately 8 to 64 unit cells, again based on the cube of the corresponding λ values reported in Table 1. In the case of lysozyme, the estimated value of λ suggests that the critical nucleus diameter is approximately equal to the linear dimension of a single unit cell, indicating that the nucleus may be composed of only one unit cell. As previously noted, these estimates are approximate and derived from theoretical calculations, as no direct experimental evidence is currently available to validate these values for the systems studied. Nevertheless, the results show good alignment with prior literature in which similar nucleus sizes (that falls within the range of λ³ values calculated here) have been reported using both computational simulations and advanced experimental techniques such as in situ transmission electron microscopy. For example, Prado et al., used molecular dynamics simulations to estimate the size of the critical nucleus for a model inorganic compound, BaS, and reported similar values.⁵² In specific their studies shows that the critical nucleus size typically ranges from 5.9 × 10⁻¹⁰ to 6.5 to 10⁻¹⁰ m depending on the degree of supercooling. These values fairly agree with the ones that we obtained for most of the inorganic and organic compounds. Additionally, Nakamura et al., employed in situ transmission electron microscopy (TEM) to experimentally observe nucleation from amorphous phases and identified clusters composed of several unit cells forming during early nucleation stages.⁵³ In specific the TEM results showed experimental evidence of the growth of unit cells containing 24 to 86 unit cells. While their work focused on amorphous-to-crystalline transitions, it provides conceptual support for the cluster sizes estimated in solution-phase crystallisation. In the specific case of lysozyme, which has the largest molecular volume among the systems studied, the calculated ΔG indicates a critical nucleus composed of approximately one unit cell. This observation is consistent with classical nucleation theory, which predicts that systems with large molecular volumes and high interfacial energy require larger energy barriers for nucleation but may only form stable nuclei at very small sizes due to packing constraints and limited supersaturation.

The higher number of unit cells estimated within the critical nucleus of inorganic compounds, compared to organic systems, can be explained by several key factors. First, inorganic crystals typically possess smaller and more symmetrical unit cells, owing to their simpler atomic or ionic structures. In contrast, organic compounds, particularly active pharmaceutical ingredients (APIs), often feature larger and more complex unit cells due to their flexible molecular frameworks and lower packing densities. As a result, for a given critical radius, more inorganic unit cells can be accommodated simply because each unit cell occupies less volume. Second, inorganic compounds tend to exhibit higher interfacial energies (γ), due to the stronger ionic or covalent bonding at the interface between the crystal and the surrounding phase. According to classical nucleation theory, a higher interfacial energy leads to an increased Gibbs free energy barrier and, consequently, a larger critical nucleus radius. When this larger critical radius is compared to the smaller unit cell dimension of an inorganic crystal, the number of unit cells required to form a stable nucleus is further amplified. Finally, the high packing efficiency and structural rigidity of inorganic lattices—featuring uniform, tightly arranged ions or atoms—contrasts with the relative disorder in organic systems, where flexible side chains, hydrogen bonding, and solvent inclusions are more common. This inherent structural order in inorganic systems may favour the formation of larger, more compact nuclei, again increasing the number of unit cells involved in the initial nucleation event.

Finally, we used our model as in eqn (7) to theoretically estimate two more parameters that are important to homogeneous nucleation, this includes in the number density or the number of molecules formed per unit volume, N_m/V when the time is equal to the induction time t_ind. According to Kubota, MSZW is assumed to be a point where the accumulated crystals that are grown up to detectable size had reached a fixed value, (N_m/V) when the time t = t_ind that can be related to the nucleation rate J by the relation:

Eqn (2) and eqn (10) can be combined to form:Eqn (10) and (11) can be combined to theoretically calculate the t_ind as follows:where, N_m/V can be obtained from eqn (10) as follows:Eqn (11) to (13) allows us to theoretically calculate, t_ind, and N_m/V for each of the cooling rate provided we have the experimentally obtained information on the MSZW (i.e., ΔT_max) and theoretically obtained nucleation rate J (which can be obtained eqn (2) and (7)). From eqn (12) and (13), it can be understood that the induction time is defined as the ratio of the metastable zone width to the cooling rate. In this context, the induction time represents the duration required to observe nucleation at starting from . The calculated t_ind and N_m/V calculated using eqn (12) and (13) are given in Table 1. Clearly for all the APIs studied, at the MSZW, the N_m/V was found to be equal to 10²⁴ to 10²⁷ molecules per m³.

For demonstration purposes, in Fig. 3, we plotted the nucleation rate obtained using the classical nucleation theory as a function of temperature based on the ΔG values calculated using the model proposed as in eqn (7) for all the combinations of solute and solutions involved. It is worth mentioning here that, in this work we considered up to 10 different APIs whose molecular weight ranges from 73.09 to 421.3 g mol⁻¹. For these APIs, according to the model proposed in this work and the nucleation temperature studied, the nucleation rate ranges from 10²¹ to 10²⁴ m⁻³ s⁻¹. In Table 1, we showed the theoretically obtained t_ind and ΔT_max for all the 11 different combinations of API/solvent systems. The N_m/V typically ranges from 10²⁴ to 10²⁷ molecules per m³ when time, t = t_ind. In the case of inorganic compounds, Fig. 3c shows that the nucleation rate (J) ranges from 10²⁰ to 10²³ m⁻³ s⁻¹, with corresponding number densities (N_m/V) between 10²³ and 10²⁶ molecules per m³. Comparable values were observed for the API intermediate and glycine, where the predicted nucleation rates ranged from 10²² to 10²³ m⁻³ s⁻¹, and the corresponding N_m/V values were between 10²⁶ and 10²⁷ molecules per m³. Among all the systems studied, lysozyme, which has the largest molecular volume, exhibited the lowest nucleation rate, on the order of 10¹⁸ to 10¹⁹ m⁻³ s⁻¹, with a corresponding number density of 10²³ to 10²⁴ molecules per m³. According to classical nucleation theory, such low nucleation rates are expected for large molecules, as the Gibbs free energy barrier (ΔG) for nucleation increases significantly with both molecular volume and interfacial energy. For lysozyme, the calculated ΔG was approximately 87 kJ mol⁻¹, which is substantially higher than the ΔG values estimated for smaller organic molecules in this study. This outcome is consistent with the theoretical prediction that systems with larger molecular volumes or lower supersaturation ratios exhibit higher nucleation barriers and therefore lower nucleation rates.

Fig. 3 Plot of nucleation rate versus the temperature for (a) 9 combinations of solvents/APIs involving 5 APIs, (b) 6 combinations of solvents/APIs involving 5 APIs, (c) combination of inorganics/solvents involving 8 different compounds and (d) API intermediate, amino acid and a large molecule. Fig. 3a: : dextrose/water (R′: 0.00278 K s⁻¹); : L-asparagine monohydrate/water (R′: 0.005 K s⁻¹); : L-asparagine monohydrate/water (R′: 0.0033 K s⁻¹); : gestodene form I/ethanol (R′: 0.0083 K s⁻¹); : gestodene form I/ethanol (R′: 0.005 K s⁻¹); : carbamazepine_saccharine/ethanol (R′: 0.0167 K s⁻¹); : Gestodene form I/ethanol (R′: 0.00167 K s⁻¹); : pyrazinamide/acetone (R′: 0.00167 K s⁻¹); : pyrazinamide/acetone (R′: 0.0033 K s⁻¹). Fig. 3b: : ibuprofen/water (R′: 0.0167 K s⁻¹); : paracetamol/water (R′: 0.5 K s⁻¹); : paracetamol/ethanol (R′: 0.5 K s⁻¹); : fenofibrate/ethyl acetate (R′: 0.005 K s⁻¹); : psilocybin/water (R′: 0.0167 K s⁻¹); : vismodegib/MIBK (R′: 0.0167 K s⁻¹). Fig. 3c: : NaNO₃/NaCl + NaNO₃ + H₂O solution (R′: 0.000833 K s⁻¹); : NaNO₃/NaCl + NaNO₃ + H₂O solution (R′: 0.001667 K s⁻¹); : CoSO₄/water (R′: 0.000833 K s⁻¹); : CoSO₄/water (R′: 0.001667 K s⁻¹); : CoSO₄/water (R′: 0.0025 K s⁻¹); : (NH₄)₂B₄O₇·4H₂O/water (R′: 0.00833 K s⁻¹); : (NH₄)₂B₄O₇·4H₂O/water (R′: 0.0025 K s⁻¹); : Na₃VO₄/NaOH solution (R′: 0.005 K s⁻¹); : Sr(OH)₂·8H₂O/water (R′: 0.001388 K s⁻¹); : Sr(OH)₂·8H₂O/water (R′: 0.00277 K s⁻¹); : ZnL₂/water (R′: 0.00138 K s⁻¹); : ZnL₂/water (R′: 0.00275 K s⁻¹); : borax/water (R′: 0.003472 K s⁻¹); : borax/water (R′: 0.01066 K s⁻¹); : ammonium oxalate/water (R′: 0.000833 K s⁻¹ – plotted in secondary axis). Fig. 3d: : L-arabinose/water (R′: 0.0083 K s⁻¹); : glycine/water (R′: 0.001667 K s⁻¹); : glycine/water (R′: 0.005 K s⁻¹); : lysozyme/NaCl solution (R′: 0.002778 K s⁻¹ – we assumed this cooling rate – shown in secondary axis).

The theoretical model developed in this work offers a practical and physically grounded framework for extracting key nucleation parameters from metastable zone width (MSZW) data obtained under different cooling rates. Using only three experimentally measurable quantities, MSZW, nucleation temperature, and cooling rate, the model enables the prediction of critical nucleation characteristics, including the nucleation rate kinetic constant, Gibbs free energy of nucleation, induction time, and the number density of nuclei at the onset of crystallisation. A key strength of the model lies in its ability to capture the dependence of nucleation rate on cooling rate, in contrast to existing models (e.g., those by Nývlt, Kubota, and Sangwal), which assume a single, cooling-rate-independent nucleation rate derived from MSZW data. By directly incorporating classical nucleation theory, the proposed model provides a more realistic and adaptable tool for interpreting experimental results under varying process conditions. In addition to kinetic parameters, the model facilitates the estimation of important thermodynamic quantities such as surface free energy, critical nucleus radius, and the approximate number of unit cells constituting the stable nucleus. These estimates are derived by comparing the critical nucleus size to the cube root of unit cell volume, offering valuable molecular-level insight into nucleation behaviour. The model was validated using MSZW data from a diverse range of 22 solute–solvent systems, including 11 API–solvent combinations, 8 inorganic compounds, one API intermediate (L-arabinose), one amino acid (glycine), and one biomolecule (lysozyme). In most cases, the model fit the experimental data with coefficients of determination (r²) exceeding 0.97, confirming its robustness, generality, and predictive accuracy across a wide spectrum of chemical systems.

In terms of theoretical limitations, the model, by design, does not predict the order of nucleation, which is commonly estimated using alternative models such as those developed by Nývlt, Kubota, and Sangwal. As the proposed approach is based on classical nucleation theory, it does not assign a fixed reaction order but rather an Arrhenius-like temperature dependence. While classical nucleation theory predicts a first-order dependence on supersaturation under low-supersaturation conditions, at higher supersaturation, the theory implies a nonlinear and more complex relationship. If needed, an empirical nucleation order can still be inferred using a phenomenological expression such as J = k′(Δc_max)ⁿ; where k′ is a kinetic constant. In this case, based on the J obtained using eqn (7), the order of nucleation and the kinetic constant, k′ according to the power law type expression can be obtained from the linear expression: ln J = ln(k′) + n ln(Δc_max). It is worth to mention here that, the primary aim of this work was to develop a model capable of predicting the nucleation rate from MSZW data obtained at different cooling rates. Nucleation fundamentally depends on both supersaturation and induction time, both of which are directly influenced by the cooling rate. This is important because cooling rate is a key process variable that governs the properties of the final crystals. At higher cooling rates, the solution cools rapidly into the labile zone, leading to faster attainment of the critical supersaturation required for nucleation. In such cases, by the time nucleation occurs—after the induction period involving the formation of prenucleation clusters and their structural rearrangement into a stable nucleus—the solution achieves a higher supersaturation. This promotes a higher nucleation rate and results in a larger number of smaller crystals. Conversely, at lower cooling rates, the solution cools more slowly, reaching the induction point at a lower temperature and thus at a lower supersaturation. Here, the longer time allows molecular clusters to form and reorganise at lower driving forces, typically leading to fewer nuclei and larger crystals. This relationship between cooling rate, supersaturation, and nucleation rate is well established, and industries often exploit this by adjusting cooling rates to tailor crystal size and size distribution. In this context, the proposed model is particularly valuable as it can predict nucleation rates as a function of cooling rate. If experimental correlations between MSZW, cooling rate, and solubility are available, the nucleation rate predictions can be linked to the resulting crystal population characteristics. This makes the model useful for designing batch crystallisation processes to achieve targeted product attributes. In continuous crystallisation, knowledge of nucleation rate at different cooling rates is even more critical. The nucleation rate directly determines the production rate (JV) and thus the required residence time to reach a target suspension density or productivity. Higher J values at a given cooling rate reduce the necessary residence time, improving process efficiency. Furthermore, understanding how J varies with cooling rate is essential for designing washout-safe operations, as insufficient nucleation rates relative to dilution rates can lead to washout of nuclei from the crystalliser. Overall, the proposed model is a simple yet useful for analysing nucleation phenomena using MSZW data observed at different cooling rates. Its broad applicability and minimal data requirements make it particularly valuable for both research and industrial crystallisation processes, where understanding and controlling nucleation is essential.

Notation

c*	Solubility concentration (molecules per m^3) (see eqn (3))
	Solubility concentration at nucleation temperature (molecules per m^3)
	Solubility concentration at reference temperature (molecules per m^3)
Δcmax	Supersaturation at metastable zone width (molecules per m^3) (see eqn (5))
ΔG	Critical Gibbs free energy of nucleation (kJ mol^−1) (see eqn (1))
J	Nucleation rate (molecules per m^3) (see eqn (2))
k n	Nucleation rate constant (molecules per m^3 s) (see eqn (1))
	Number density (molecules per m^3) (see eqn (10))
r c	Critical radius (m) (see eqn (9))
R	Gas constant, (J mol^−1 K^−1) (see eqn (1))
R′	Cooling rate (K s^−1) (see eqn (3))
S	Supersaturation (dimensionless) (see eqn (8))
t	time (s)
t ind	Induction time (s) (see eqn (12))
T	Solubility temperature (K) (see eqn (3))
T nuc	Nucleation temperature (K) (see eqn (6))
	Reference temperature (K)
ΔTmax	Metastable zone width (K) (see eqn (5))
V cell	Unit cell volume (m^3)
γ	Interfacial surface energy (mJ m^−2) (see eqn (8))
ϑ	Molecular volume (m^3) (see eqn (8))

Data availability

The ESI† file includes the experimental data, calculation procedures, model equations, and graphical outputs for four representative systems: pyrazinamide, glycine, borax, and lysozyme. Data and calculations for the remaining systems discussed in the manuscript, along with the corresponding theoretical parameters, are available from the authors upon reasonable request.

Conflicts of interest

There are no conflicts to declare.

Acknowledgements

We acknowledge the financial support of the Science Foundation Ireland (Grant 12/RC/2275, 12/RI/2345/SOF and 18/SIRG/5479). M. V. would like to acknowledge the Bernal Institute, Boston Scientific, Department of Chemical Sciences, and the University of Limerick Foundation for the funding support through the mULtiply program.

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Footnote

† Electronic supplementary information (ESI) available. See DOI: https://doi.org/10.1039/d5ce00467e

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