Next Article in Journal
Paper Spray Tandem Mass Spectrometry for Assessing Oleic, Linoleic and Linolenic Acid Content in Edible Vegetable Oils
Previous Article in Journal
Lithium Extraction from Salt Lake Brine with High Mass Ratio of Mg/Li Using TBP-DIBK Extraction System
Previous Article in Special Issue
Development of a Quantitative Chromatographic Fingerprint Analysis Method for Sugar Components of Xiaochaihu Capsules Based on Quality by Design Concept
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Separations
Volume 10
Issue 1
10.3390/separations10010025
separations-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Article

Optimization of Steam Distillation Process for Volatile Oils from Forsythia suspensa and Lonicera japonica according to the Concept of Quality by Design

by
Xinying Chen
1,2,
Dongyun Guo
1,
Xingchu Gong
2,3,*,
Na Wan
1,* and
Zhenfeng Wu
1,4
1
State Key Laboratory of Innovation Medicine and High Efficiency and Energy Saving Pharmaceutical Equipment, Jiangxi University of Chinese Medicine, Nanchang 330004, China
2
Pharmaceutical Informatics Institute, College of Pharmaceutical Science, Zhejiang University, Hangzhou 310058, China
3
Jinhua Institute of Zhejiang University, Jinhua 321016, China
4
Key Laboratory of Modern Preparation of TCM, Ministry of Education, Jiangxi University of Chinese Medicine, Nanchang 330004, China
*
Authors to whom correspondence should be addressed.
Separations 2023, 10(1), 25; https://doi.org/10.3390/separations10010025
Submission received: 25 September 2022 / Revised: 7 November 2022 / Accepted: 9 November 2022 / Published: 1 January 2023
(This article belongs to the Special Issue Separation, Extraction and Purification of Natural Products from Plants)
Browse Figures
Versions Notes

Abstract

:
In this study, the process of steam distillation to collect volatile oils from Forsythia suspensa (F. suspensa) and Lonicera japonica (L. japonica) was optimized according to the concept of quality by design. First, the liquid/material ratio, distillation time, and collection temperature were identified as critical process parameters by a review of the literature and single-factor experiments. Then, a Box–Behnken design was used to study the quantitative relationship between the three process parameters, two raw material properties, and the yield of volatile oil. A mathematical model was established with an R2 value exceeding 0.90. Furthermore, the design space of the volatile oil yield was calculated by a probability-based method. The results of a verification experiment showed that the model was accurate and the design space was reliable. A total of 16 chemical constituents were identified in the volatile oil from mixtures of F. suspensa and L. japonica. The content of β-pinene was the highest (54.75%), and the composition was similar to that of the volatile oil of F. suspensa. The results showed that when F. suspensa and L. japonica were distilled together, the main contribution to the volatile oil was from F. suspensa. The volatile oil yield from the combination of F. suspensa and L. japonica was not higher than that from L. japonica.

Graphical Abstract

1. Introduction

Forsythia suspensa is the dry fruit of Forsythia suspensa (Thunb.) Vahl, and Lonicera japonica consists of the dry buds or flowers of Lonicera japonica Thunb. that bloom early in the spring [1]. Both have the medicinal functions of reducing fevers, detoxification, and dispersing wind-heat and are often used together as a pair in Chinese medicine [2,3,4]. The 2020 edition of the Chinese Pharmacopoeia lists 45 Chinese patent medicines that use F. suspensa and L. japonica in combination [1]. The volatile oils of F. suspensa and L. japonica are collected and used in the manufacture of four Chinese patent medicines, including Xiao’er Resuqing Koufuye, Xiao’er Resuqing Keli, Xiao’er Resuqing Tangjiang, and Jinchan Zhiyang Jiaonang [1]. At present, several studies have shown that the volatile oil of F. suspensa has antibacterial, antioxidant, antiviral, antipyretic, anti-inflammatory, antitumor, and other pharmacological effects [3,5,6]. The volatile oil of L. japonica also has pharmacological effects, such as heat clearing, detoxification, and antibacterial activity [2,4,7].
Steam distillation is a commonly used method to collect volatile oils [8,9,10,11,12,13], and it has the advantages of simple equipment, easy operation, low cost, and the use of safe solvents [14,15,16]. However, it is also a time-consuming process with a low volatile oil yield. The steam distillation process is used in the production of the abovementioned four Chinese patent medicines from the volatile oils collected from F. suspensa and L. japonica [1].
References from the literature concerning the distillation of the volatile oils of F. suspensa or L. japonica by steam distillation are listed in Table 1. Liu Yan et al. [17] and Wang Yan et al. [18] studied the three parameters of soaking time, distillation time, and material/liquid ratio and found that the influence of each parameter on the volatile oil yield was: material/liquid ratio > distillation time > soaking time. The volatile oil yields from F. suspensa and L. japonica were approximately 0.93 mL/100 g and 0.34 mL/100 g, respectively. Gu Ke et al. [19] and Li Jianjun et al. [20] studied the collection of volatile oil from L. japonica by steam distillation, and the volatile oil yields were about 0.15 g/100 g and 0.17 g/100 g. However, Tong Qiaozhen et al. [21] failed to distillate volatile oil from L. japonica by steam distillation. In these published works, the authors suggested that the volatile oil of L. japonica has a relatively high solubility in water, which may lead to the loss of L. japonica volatile oil in the steam distillation process. When co-distilled with F. suspensa, the volatile oil of F. suspensa may extract some L. japonica volatile oil from the aqueous phase, resulting in the collection of more L. japonica volatile oil. However, at present, there are no references in the literature addressing the steam distillation of volatile oil from mixtures of F. suspensa and L. japonica. Therefore, the authors tried to obtain the volatile oil by the co-distillation of F. suspensa and L. japonica.
In recent years, the concept of quality by design [22,23,24,25] has been used in the optimization of many processes related to Chinese medicines, such as distillation [26], precipitation [27], and column chromatography [28]. In this study, based on the concept of quality by design, the steam distillation process was optimized to distill the volatile oils of F. suspensa and L. japonica. One of the aims of this work was to find the optimized parameters of steam distillation for collecting a relatively stable amount of volatile oil, which would improve the batch-to-batch consistency of Chinese medicine quality. The critical process parameters were determined through a search of the literature and single-factor experiments. The critical raw material properties of F. suspensa were also determined. The quantitative relationship between the process parameters, raw material properties, and volatile oil yield was studied by a Box–Behnken design [29], and a mathematical model was established. The design space of the distillation process of volatile oil from F. suspensa and L. japonica was calculated by a probability-based method. The operation points inside and outside the design space were selected for verification. Finally, the chemical composition of the volatile oil of F. suspensa and the volatile oil of mixtures of F. suspensa and L. japonica were analyzed and compared.

2. Materials and Methods

2.1. Materials and Reagents

Methanol (chromatographically pure) was obtained from Merck, Germany. Acetonitrile (chromatographically pure) was also obtained from Merck, Germany. Ultrapure water was prepared by an ultrapure water preparation system (Milli-Q, Millipore, Germany). β-Pinene (batch number: C12071236, purity ≥ 98%) was purchased from Shanghai McLean Biochemical Technology Co., Ltd. The medicinal material numbers, origins, and suppliers of F. suspensa and L. japonica are shown in Table 2.

2.2. Steam Distillation

The volatile oil in F. suspensa and L. japonica was collected by steam distillation. The experimental setup is shown in Figure 1. A low-temperature thermostated bath (THYD-1030 W, Ningbo Tianheng Instrument Factory) was used to lower the temperature of the collection part of the volatile oil extractor [30]. An electronic balance (CN-LQC60002, Kunshan Youkeweiter Electronic Technology Co., Ltd.) was used to weigh 50 g of F. suspensa and 50 g of L. japonica (Medicinal Material Number: JYH-2). The samples were placed in a 2000 mL flask. A certain amount of water was added, and the flask was shaken to fully wet the medicinal materials. The volatile oil extractor and the condenser pipe were connected. The condensed glycerol and condensed water were fed into the water-cooling jacket and the condenser pipe of the volatile oil extractor, respectively. The volatile oil extractor was filled with water from the top of the condenser until it overflowed into the flask. The electric heater (DZTW 2000 mL, Shaoxing Yuecheng Kechen Instrument and Equipment Co., Ltd.) was turned on, and it started slowly heating the water to boiling. After boiling began, the power of the electric heater was adjusted to 50 W. Starting with the first drop of condensed water dripping into the volatile oil extractor, heating was stopped after heating and refluxing for a certain period of time. After the volatile oil stood for 10 min, its volume was recorded. The volatile oil yield was calculated as shown in Formula (1).
Volatile oil yield (mL/100 g) = volatile oil volume (mL)/medicinal material (100 g)

2.3. Determination of the Volatile Oil Content in F. suspensa

The thermostat was used to lower the temperature of the collection part of the volatile oil extractor [30]. An electronic balance was used to weigh 100 g of F. suspensa, which was then placed in a 2000 mL flask. A certain amount of water was added, and the flask was shaken to fully wet the medicinal materials. The volatile oil extractor and the condenser pipe were connected. The condensed glycerol and condensed water were fed into the water-cooling jacket and the condenser pipe of the volatile oil extractor, respectively. The volatile oil extractor was filled with water from the top of the condenser until it overflowed into the flask. The electric heater was turned on, and it slowly heated the water to boiling. After boiling, the power of the electric heater was adjusted to 50 W. Starting with the first drop of condensed water dripping into the volatile oil extractor, heating was stopped after heating and refluxing for a certain period of time. After the volatile oil stood for 10 min, its volume was recorded. The volatile oil content (mL/100 g) in different batches of F. suspensa was calculated as shown in Formula (1).

2.4. Determination of β-Pinene Content in F. suspensa

2.4.1. Preparation of Reference Solution and Test Solution

Because the reference substance of β-pinene was a liquid, we precisely measured 83.40 mg of the β-pinene reference substance with a pipette. After that, it was diluted to 10 mL with methanol to obtain the storage reference solution with a concentration of 8340 μg/mL. Then, the storage reference solution was diluted 50, 100, 200, 400, 500, and 800 times with methanol, respectively, to prepare reference solutions with concentrations of 166.8, 83.40, 41.70, 20.85, 16.68, and 10.42 μg/mL.
One hundred microliters of the distilled F. suspensa volatile oil was precisely measured, placed in a 10 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the concentrated stock solution of the test product. A total of 100 μL of the concentrated stock solution of the test product was precisely measured, placed in a 5 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the test solution.

2.4.2. Chromatographic Conditions

The β-Pinene content in the volatile oil was determined using liquid chromatography (Agilent 1100-DAD, Agilent, USA). The HPLC conditions were modified from the method described in the literature [31]. The details were as follows: Column—Agilent ZORBAX SB-C18, 4.6×250 mm (5-Micron). Mobile phase—0.4% phosphoric acid solution (A)/acetonitrile (B), gradient elution (0 min, 65% B; 0~5 min, 65~70% B; 5~25 min, 70% B; 25~30 min, 70~80% B). Post-run—15 min.; injection volume—10 μL; flow rate—1 mL/min.; column temperature—25 °C; detection wavelength—202 nm. The chromatograms of the reference solution and test solution are shown in Figure 2.

2.4.3. Methodological Validation

Linear relationship investigation: The β-pinene reference substance was used to investigate the linear relationship. Reference solutions with concentrations of 166.8, 83.40, 41.70, 20.85, 16.68, and 10.42 μg/mL were prepared according to the method described in Section 2.4.1. A 0.22 μm microporous filter membrane was used for filtration, injection, and analysis according to the chromatographic conditions described in Section 2.4.2. Taking the concentration of the reference solution as the abscissa (X, μg/mL) and the peak area as the ordinate (Y, mAU), the linear regression equation and correlation coefficient were obtained.
Precision test: The volatile oil of F. suspensa was used to prepare the concentrated stock solution of the test product according to the method outlined in Section 2.4.1. One milliliter of the concentrated stock solution of the test product was accurately absorbed, placed in a 10 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the test solution. The test solution was filtered with a 0.22 μm microporous membrane. The samples were injected into the column 6 times continuously according to the chromatographic conditions provided in Section 2.4.2, and the RSD value of the peak area was calculated.
Repeatability test: Six replicates of the same batch of F. suspensa volatile oil were obtained. The concentrated stock solution of the test product was prepared according to the method in Section 2.4.1. One milliliter of the concentrated stock solution of the test product was accurately absorbed, placed in a 10 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the test solution. The test solution was filtered with a 0.22 μm microporous membrane. The samples were injected and analyzed according to the chromatographic conditions outlined in Section 2.4.2, and the RSD value of the concentration was calculated.
Stability test: The volatile oil of F. suspensa was used to prepare a concentrated stock solution of the test product according to the method described in Section 2.4.1. One milliliter of the concentrated stock solution of the test product was accurately measured, placed in a 10 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the test solution. The test solution was filtered with a 0.22 μm microporous membrane. The samples were injected and analyzed at 0, 3, 6, 9, 12, and 24 h according to the chromatographic conditions described in Section 2.4.2, and the relative standard deviation (RSD) value of the peak area was calculated.
Sample addition and recovery test: We took 9 aliquots of F. suspensa volatile oil from the same batch with a known content of β-pinene and prepared a concentrated stock solution of the test sample according to the method described in Section 2.4.1. One milliliter of the concentrated stock solution of the test sample was accurately absorbed, placed in a 20 mL volumetric flask, diluted to volume with methanol, and shaken well to obtain the test solution (33.2 μg/mL). The reference solution (41.7 μg/mL) was prepared according to the method outlined in Section 2.4.1. The test solution was divided into three groups: low, medium, and high. We precisely measured 1.25 mL of each group and placed it in a 5 mL volumetric flask. The ratios of the added amount of the reference substance to the content of β-pinene in the test solution were controlled at approximately 0.5:1.0, 1.0:1.0, and 1.5:1.0, and 0.5, 1.0, and 1.5 mL of the reference substance was added to the low, medium, and high groups, respectively. Each mixture was diluted to volume with methanol, shaken well, and filtered with a 0.22 μm microporous membrane. The samples were injected and analyzed according to the chromatographic conditions provided in Section 2.4.2, and the β-pinene content and sample recovery rate of each group were calculated.

2.4.4. Determination of Content

An appropriate amount of volatile oil was taken from different batches of F. suspensa. The test solutions were prepared according to the method outlined in Section 2.4.1. Then, the test solutions were injected and analyzed according to the chromatographic conditions described in Section 2.4.2. The peak areas were recorded, and the β-pinene contents in different batches of F. suspensa were calculated.

2.5. Optimization of Distillation Process Parameters

Based on the literature search and single-factor experiments, it was believed that the critical process parameters affecting the volatile oil yield from F. suspensa and L. japonica by steam distillation were the amount of water, distillation time, and collection temperature, and the critical properties of the raw materials were the volatile oil content and the β-pinene content of F. suspensa.
A Box–Behnken design was adopted, and the water addition (X1), distillation time (X2), collection temperature (X3), volatile oil content (Z1), and β-pinene content (Z2) were used as the investigation factors. The volatile oil yield (Y) was used as the evaluation index to optimize the distillation process of volatile oil from F. suspensa and L. japonica. The factors and levels of the Box–Behnken design are shown in Table 3, and the results are shown in Table 4.

2.6. Analysis of Chemical Constituents of Volatile Oil

A combined total of 20 μL of volatile oil from F. suspensa and volatile oil from F. suspensa and L. japonica was accurately measured; then, the samples were supplemented with 1 mL of diethyl ether for dilution, filtered with a 0.22 μm microporous membrane, and placed into sample bottles. The chemical constituents in the volatile oil of F. suspensa and the volatile oil of F. suspensa and L. japonica were analyzed.
The chemical constituents of the volatile oils were analyzed with a gas chromatography–mass spectrometer [32,33] (GC–MS; Agilent 7890B-7000C, Agilent, USA). The GC–MS conditions were modified from the methods describe in the literature [34,35]. The conditions were as follows: chromatographic column—Agilent HP-5MS, 30 m × 0.25 mm × 0.25 μm; inlet temperature—250 °C; flow—1 mL/min constant flow (He); split ratio—10:1; heating program—40 °C for 4 min, 2 °C/min to 100 °C, hold for 10 min, 10 °C/min to 200 °C, and hold for 5 min; MS detector—detector temperature 250 °C and scan range m/z 30–550.

2.7. Data Processing

2.7.1. Mathematical Model

The results of the Box–Behnken design were analyzed using Design-Expert 12.0.3 software (American Stat-Ease Company). Taking the volatile oil yield (Y) as the evaluation index, quadratic polynomial fitting was performed on the five factors of water addition (X1), distillation time (X2), collection temperature (X3), volatile oil content (Z1) and β-pinene content (Z2). The mathematical model is shown as Formula (2).
Y = a 0 + i = 1 n b i X i + i = 1 n b i i X i 2 + i = 1 n 1 j = i + 1 n b i j X i X j + k = 1 m d k Z k
where X is a process parameter; Z is a raw material property; Y is the evaluation index; superscripts n and m are the number of process parameters and raw material properties, respectively; a0 is the intercept; and b and d are the partial regression coefficients. The model was simplified using a stepwise regression method with p values of 0.1 for both inclusion and removal from the model.

2.7.2. Design Space

The construction design space was calculated by the probability-based method using MATLAB R2018b (American Math Works Company). Under the conditions of fixed batches of medicinal materials, the effects of the changes in the three process parameters on the volatile oil yield were randomly simulated. The parameter combination with a lower limit of volatile oil yield of 0.60 mL and a probability of reaching the standard of no less than 0.80 was used as the design space. In the calculation, the steps of water addition, distillation time, and collection temperature were set to 0.04, 0.03, and 0.10, respectively. The number of simulations was 1000.

3. Results

3.1. Single-Factor Experiments

The results of the single-factor experiments are shown in Table 5. The results indicated that the effects of crushed particle size and soaking time on the volatile oil yield were not significant. The volatile oil yield decreased with increasing water addition, which may have been due to the increase in water improving the amount of volatile oil dissolved in water, which resulted in a decrease in the volatile oil yield.
Table 6 shows the results of separately distilling volatile oils from F. suspensa and L. japonica. The results showed that no volatile oil was distilled from the two different batches of L. japonica, which may have been because the L. japonica used in this study contained little volatile oil. F. suspensa could be distilled to obtain volatile oil. Therefore, in a follow-up study, we will investigate whether the distillation of volatile oil from L. japonica can be promoted by the combined steam distillation of F. suspensa and L. japonica.
The results of the co-distillation of volatile oil from F. suspensa and L. japonica are shown in Table 7. The effects of water addition and collection temperature on the volatile oil yield were investigated. The results showed that both had a certain influence on the volatile oil yield.

3.2. Methodological Validation

Taking the concentration of the β-pinene reference solution as the abscissa (X, μg/mL) and the corresponding peak area as the ordinate (Y, mAU), linear regression was performed to obtain the linear regression equation: Y = 210.56X + 282.59. The linear range of β-pinene was 10.425–166.8 μg/mL, and the coefficient of determination R2 in this range was 0.9997, which confirmed a good linear relationship. The results of the precision test showed that the RSD of the peak area of β-pinene was 0.68%, indicating that the precision of the instrument was good. The results of the repeatability test showed that the RSD of the β-pinene concentration was 0.84%, which proved that the method had good repeatability. The results of the stability test showed that the peak-area RSD of β-pinene was 1.84%, indicating that the test solution had good stability within 24 h. The results of the sample addition recovery test are shown in Table S1. The measured recovery rates were between 95 and 102%, the average recovery rate was 98.71%, and the RSD of the three levels was 1.89%, which met the measurement requirements, indicating that the method has good accuracy.

3.3. Characterization of Raw Material Properties of Different Batches of F. suspensa

The process parameters of the steam distillation method were fixed as follows: 100 g raw material, 1000 mL water addition, 5 °C collection temperature, and 6 h distillation time. The contents of volatile oil and β-pinene in different batches of F. suspensa were measured as shown in Table 8. The results showed that the raw material properties of different batches of F. suspensa were quite different. For example, the volatile oil content of LQ-4 was 1.394 mL/100 g, while the volatile oil content of LQ-5 was 1.969 mL/100 g. The β-pinene content of LQ-6 was 0.746 mg/100 g, while the β-pinene content of LQ-5 reached 1.139 mg/100 g.

3.4. Optimization of Distillation Parameters of Volatile Oil

3.4.1. Data Processing and Model Fitting

The polynomial regression model obtained by modeling the data acquired from the experimental distillation of volatile oil from F. suspensa and L. japonica is shown in Formula (3).
Y = 0.2294 + 0.04977 × 2 − 0.5199Z1 + 1.325Z2 − 0.000318 × 1X3
The coefficient of determination of the model R2 was 0.9022, indicating that the model fit well and could explain the changes in the experimental data. The variance analysis of each item in the model is shown in Table 9. The p value of the model was less than 0.0001, indicating that the model was extremely significant. In the model, X2 (p = 0.0067), Z1 (p = 0.0014), and Z2 (p = 0.0001) were all extremely significant items, indicating the influence of distillation time and raw material properties (volatile oil content, β-pinene content) on the volatile oil yield. X1X3 (p = 0.0139) was also a significant item, which indicated that the interaction of the two factors of water addition and collection temperature was significant for volatile oil yield.

3.4.2. Contour Diagram

The contour maps of the volatile oil yield from F. suspensa and L. japonica are shown in Figure 3, Figure 4 and Figure 5. The figures reflect the effect of water addition, distillation time, and collection temperature on the volatile oil yield under the conditions of fixed raw material properties. Under the conditions of a constant collection temperature with increasing distillation time, the volatile oil yield increased gradually. Under the conditions of a constant distillation time with increasing water addition and a decreasing collection temperature, or decreasing water addition and an increasing collection temperature, the volatile oil yield increased. Under the conditions of unchanging water addition with increasing distillation time, the volatile oil yield increased gradually.

3.4.3. Design Space Calculation and Verification

The properties of the raw materials were fixed as LQ-6, and the design space calculated by the probability-based method is shown in Figure 6 and Figure 7. The design space diagram shows that the distillation time had the greatest influence on the volatile oil yield.
A point inside the design space and a point outside the design space were selected for verification. The selection conditions of the verification points in the design space were as follows: the water addition was 10 mL/g, the distillation time was 6 h, and the collection temperature was 10 °C. The probability of reaching the standard was 0.976. Under these conditions, the volatile oil yield predicted by the model was 0.71 mL. According to the above conditions, three parallel experiments were carried out. The obtained volatile oil yields were 0.76 mL, 0.71 mL, and 0.74 mL, respectively. The average volatile oil yield was 0.74 mL, and the relative standard deviation was 2.52%.
The selection conditions of the verification point outside the design space were as follows: the water addition was 10 mL/g, the distillation time was 3 h, and the collection temperature was 10 °C. The probability of reaching the standard was 0.333. Under these conditions, the volatile oil yield predicted by the model was 0.56 mL, and the experimental results were 0.60 mL, 0.60 mL, and 0.58 mL, respectively. The average volatile oil yield was 0.59 mL, and the relative standard deviation was 1.15%. The measured values of the two verification points were relatively close to the model-predicted values, indicating that the mathematical model established according to the Box–Behnken design was accurate. The volatile oil yield at the verification point in the design space was higher than the preset standard, and the volatile oil yield at the verification point outside the design space was lower than the preset standard, indicating that the design space was reliable.

3.5. Qualitative Analysis of Chemical Constituents of Volatile Oil

The distilled volatile oil of F. suspensa and the volatile oil of mixtures of F. suspensa and L. japonica were analyzed by GC–MS. The total ion chromatogram is shown in Figure 8, and the mass spectrometry results are shown in Table 10 and Table 11. Interactions between multiple components can also have an impact on pharmacological activity [36,37]. A total of 16 chemical components were identified in the volatile oil of F. suspensa, among which the relative content of β-pinene was the largest (53.71%). Some other components with relatively large contents were α-pinene (21.12%), terpinene-4-ol (5.97%), (+)-limonene (4.36%), and α-thujene (4.25%). A total of 16 chemical components were identified in the volatile oil of F. suspensa and L. japonica, among which the relative content of β-pinene was also the largest (54.75%). Some other components with relatively large contents were α-pinene (21.38%), terpinene-4-ol (4.98%), (+)-limonene (4.48%), and α-thujene (4.41%).
Table 10 and Table 11 show that the chemical composition of the volatile oil of F. suspensa was basically the same as that of the mixtures of F. suspensa and L. japonica. This meant that when F. suspensa and L. japonica were distilled together, the main contribution of the volatile oil chemical components came from F. suspensa, while L. japonica basically did not contribute. The combination of the two medicinal materials did not increase the amount of volatile oil distilled from L. japonica.
The authors attempted to distill the volatile oil from L. japonica but failed to collect any volatile oil. Li Jianjun et al. [20] studied the collection of volatile oil from L. japonica by steam distillation, and a total of 79 chemical components were identified in the volatile oil, among which the contents of palmitic acid (46.42%) and linoleic acid (14.32%) were the highest.

4. Conclusions

In this study, the steam distillation process of volatile oil from F. suspensa and L. japonica was optimized according to the concept of quality by design. First, the liquid/material ratio, distillation time, and collection temperature were identified as critical process parameters by a search of the literature and single-factor experiments. In addition, this study further investigated the effect of different batches of F. suspensa on the distillation of volatile oil and determined that the critical raw material properties were the volatile oil content and β-pinene content. HPLC was used to evaluate the different batches. The content of β-pinene in F. suspensa was measured, and related methodological verification work was performed. Then, a Box–Behnken design was used to study the quantitative relationship between three process parameters, two raw material properties, and the volatile oil yield. A mathematical model was established with R2 exceeding 0.90. Furthermore, the design space of the volatile yield was calculated by a probability-based method, and verification experiments were carried out. The measured values of two verification points were relatively close to the model-predicted values, indicating that the mathematical model established according to the Box–Behnken design was accurate. The volatile oil yield at the verification point in the design space was greater than the preset standard, and the volatile oil yield at the verification point outside the design space was lower than the preset standard, indicating that the design space was reliable. In this study, the chemical constituents of the volatile oil of F. suspensa and the volatile oil of F. suspensa and L. japonica were analyzed by GC–MS. A total of 16 chemical constituents were identified in the volatile oil of F. suspensa, among which the content of β-pinene was the largest (53.71%). A total of 16 chemical constituents were identified in the volatile oil of F. suspensa and L. japonica, among which the content of β-pinene was also the largest (54.75%), and the composition was similar to that of the volatile oil of F. suspensa. The results showed that when F. suspensa and L. japonica were distilled together, the main contributor to the volatile oil was F. suspensa. The contribution of L. japonica was small. The combination of F. suspensa and L. japonica did not increase the volatile oil yield from L. japonica.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/separations10010025/s1, Table S1: Sample Recovery Test Results.

Author Contributions

Conceptualization, X.G., N.W., and Z.W.; investigation, X.C. and D.G.; data curation, X.C. and X.G.; writing—original draft preparation, X.C., X.G., and N.W.; writing—review and editing, X.G., Z.W., and N.W.; supervision, N.W. and X.G.; funding acquisition, X.G., N.W., and Z.W. All authors have read and agreed to the published version of the manuscript.

Funding

This work was supported by the National Natural Science Foundation of China (82060720); the Open Project of the State Key Laboratory of Innovative Medicine and High-Efficiency and Energy-Saving Pharmaceutical Equipment at Jiangxi University of Chinese Medicine (grant number: GZSYS202001); the Provincial College Students’ Innovation and Entrepreneurship Program (S202210412062); the Innovation Team and Talent Cultivation Program of the National Administration of Traditional Chinese Medicine (ZYYCXTD-D-202002); and the Jiangxi Traditional Chinese Medicine Research Program (2018A318).

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

All data generated or analyzed during this study are included in the published article.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Chinese Pharmacopoeia Commission. Pharmacopoeia of the People’s Republic of China; China Medical Science and Technology Publishing House: Beijing, China, 2020. [Google Scholar]
  2. Liu, X.; Li, C.; Xue, J. Research progress on main active components and pharmacological effects of honeysuckle. J. Xinxiang Med. Univ. 2021, 38, 992–995. [Google Scholar]
  3. Tian, D.; Shi, M.; Wang, Y. Volatile Oil from Forsythia suspense: Chemical Constituents and Pharmacological Effects. Nat. Prod. Res. Dev. 2018, 30, 1834–1842. [Google Scholar]
  4. Xia, W.; Yu, Y.; Yang, H.; Tan, Z.; Xu, L.; Dong, W.; Lu, H.; Luo, F.; Liang, H. Research Advances on Chemical Constituent and Pharmacology Effects of Honeysuckle. J. Anhui Agric. Sci. 2017, 45, 126–127+165. [Google Scholar]
  5. Wang, Z.; Xia, Q.; Liu, X.; Liu, W.; Huang, W.; Mei, X.; Luo, J.; Shan, M.; Lin, R.; Zou, D.; et al. Phytochemistry, pharmacology, quality control and future research of Forsythia suspensa (Thunb.) Vahl: A review. J. Ethnopharmacol. 2018, 210, 318–339. [Google Scholar] [CrossRef] [PubMed]
  6. Shao, S.; Zhang, F.; Yang, Y.; Feng, Z.; Jiang, J.; Zhang, P. Neuroprotective and anti-inflammatory phenylethanoidglycosides from the fruits of Forsythia suspensa. Bioorg. Chem. 2021, 113, 105025. [Google Scholar] [CrossRef]
  7. Tang, X.; Liu, X.; Zhong, J.; Fang, R. Potential Application of Lonicera japonica Extracts in Animal Production: From the Perspective of Intestinal Health. Front. Microbiol. 2021, 12, 719877. [Google Scholar] [CrossRef]
  8. Kaya, D.A.; Ghica, M.V.; Dănilă, E.; Öztürk, Ş.; Türkmen, M.; Kaya, M.G.A.; Dinu-Pîrvu, C.-E. Selection of Optimal Operating Conditions for Extraction of Myrtus Communis L. Essential Oil by the Steam Distillation Method. Molecules 2020, 25, 2399. [Google Scholar] [CrossRef] [PubMed]
  9. Zhang, H.; Huang, T.; Liao, X.; Zhou, Y.; Chen, S.; Chen, J.; Xiong, W. Extraction of Camphor Tree Essential Oil by Steam Distillation and Supercritical CO2 Extraction. Molecules 2022, 27, 5385. [Google Scholar] [CrossRef]
  10. Geraci, A.; Stefano, V.D.; Martino, E.D.; Schillaci, D.; Schicchi, R. Essential oil components of orange peels and antimicrobial activity. Nat. Prod. Res. 2017, 31, 653–659. [Google Scholar] [CrossRef]
  11. Haro-González, J.N.; Castillo-Herrera, G.A.; Martínez-Velázquez, M.; Espinosa-Andrews, H. Clove Essential Oil ( Syzygium aromaticum L. Myrtaceae): Extraction, Chemical Composition, Food Applications, and Essential Bioactivity for Human Health. Molecules 2021, 26, 6387. [Google Scholar] [CrossRef]
  12. Jeliazkova, E.; Zheljazkov, V.D.; Kačániova, M.; Astatkie, T.; Tekwani, B.L. Sequential Elution of Essential Oil Constituents during Steam Distillation of Hops (Humulus lupulus L.) and Influence on Oil Yield and Antimicrobial Activity. J. Oleo. Sci. 2018, 67, 871–883. [Google Scholar] [CrossRef] [Green Version]
  13. Romanik, G.; Gilgenast, E.; Przyjazny, A.; Kamiński, M. Techniques of preparing plant material for chromatographic separation and analysis. J. Biochem. Biophys. Methods 2007, 70, 253–261. [Google Scholar] [CrossRef] [PubMed]
  14. Zou, J.; Zhang, X.; Shi, Y.; Guo, D.; Cheng, J.; Cui, C.; Tai, J.; Liang, Y.; Wang, Y.; Wang, M. Kinetic study of extraction of volatile components from turmeric by steam distillation. China J. Tradit. Chin. Med. Pharm. 2020, 35, 1175–1180. [Google Scholar]
  15. Božović, M.; Navarra, A.; Garzoli, S.; Pepi, F.; Ragno, R. Esential oils extraction: A 24-hour steam distillation systematic methodology. Nat. Prod. Res. 2017, 31, 2387–2396. [Google Scholar] [CrossRef] [PubMed]
  16. Aziz, Z.A.A.; Ahmad, A.; Setapar, S.H.M.; Karakucuk, A.; Azim, M.M.; Lokhat, D.; Rafatullah, M.; Ganash, M.; Kamal, M.A.; Ashraf, G.M. Essential Oils: Extraction Techniques, Pharmaceutical And Therapeutic Potential - A Review. Curr. Drug Metab. 2018, 19, 1100–1110. [Google Scholar] [CrossRef] [PubMed]
  17. Liu, Y.; Tian, J.; FU, X.; Fu, C. Technological research on extraction of volatile oil from Lianqiao and inclusion of compunds with β-cyclodextrin. J. Luzhou Med. Coll. 2010, 33, 382–384. [Google Scholar]
  18. Wang, Y.; Gao, J.; Cui, J.; Wang, F.; Zhang, S.; Yang, Y. Optimization of extraction process of volatile oil from Shanxi Hypericum Perforatum L. and GC-MS analysis of its chemical compositions. Chem. Bioeng. 2016, 33, 28–32. [Google Scholar]
  19. Gu, K.; Wang, X.; Hu, P.; Li, H.; Wang, H.; Wang, X. Study on the technologies of steam distillation and salting out method for honeysuckle volatile oil extraction. Asia Pac. Tradit. Med. 2020, 16, 55–58. [Google Scholar]
  20. Li, J.; Ren, M.; Shang, X.; Lian, X.; Wang, H. Extraction of volatile oil from Honeysuckle by distillation and its component analysis. J. Henan Agric. Sci. 2017, 46, 144–148. [Google Scholar]
  21. Tong, Q.; Zhou, R.; Du, F.; Pei, G.; Peng, F. Study on the extraction technology of volatile oil from honeysuckle. J. Hunan Univ. Chin. Med. 2002, 22, 24–25. [Google Scholar]
  22. Yu, L.X.; Amidon, G.; Khan, M.A.; Hoag, S.W.; Polli, J.; Raju, G.K.; Woodcock, J. Understanding pharmaceutical quality by design. AAPS J. 2014, 16, 771–783. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  23. Swain, S.; Parhi, R.; Jena, B.R.; Babu, S.M. Quality by Design: Concept to Applications. Curr. Drug Discov. Technol. 2019, 16, 240–250. [Google Scholar] [CrossRef]
  24. Kasemiire, A.; Avohou, H.T.; Bleye, C.D.; Sacre, P.-Y.; Dumont, E.; Hubert, P.; Ziemons, E. Design of experiments and design space approaches in the pharmaceutical bioprocess optimization. Eur. J. Pharm. Biopharm. 2021, 166, 144–154. [Google Scholar] [CrossRef] [PubMed]
  25. Debevec, V.; Srčič, S.; Horvat, M. Scientific, statistical, practical, and regulatory considerations in design space development. Drug Dev. Ind. Pharm. 2018, 44, 349–364. [Google Scholar] [CrossRef] [PubMed]
  26. Gong, X.; Chen, H.; Pan, J.; Qu, H. Optimization of Panax notoginseng extraction process using a design space approach. Sep. Purif. Technol. 2015, 141, 197–206. [Google Scholar] [CrossRef]
  27. Tai, Y.; Qu, H.; Gong, X. Design Space Calculation and Continuous Improvement Considering a Noise Parameter: A Case Study of Ethanol Precipitation Process Optimization for Carthami Flos Extract. Separations 2021, 8, 74. [Google Scholar] [CrossRef]
  28. Chen, T.; Gong, X.; Zhang, Y.; Chen, H.; Qu, H. Optimization of a chromatographic process for the purification of saponins in Panax notoginseng extract using a design space approach. Sep. Purif. Technol. 2015, 154, 309–319. [Google Scholar] [CrossRef]
  29. Kusuma, H.S.; Mahfud, M. Box-Behnken design for investigation of microwave-assisted extraction of patchouli oil. Conf. Proc. 2015, 1699, 050014. [Google Scholar]
  30. Wan, N.; Lan, J.; Wu, Z.; Chen, X.; Zheng, Q.; Gong, X. Optimization of Steam Distillation Process and Chemical Constituents of Volatile Oil from Angelicae Sinensis Radix. Separations 2022, 9, 137. [Google Scholar] [CrossRef]
  31. Chen, Q.; Cao, C.; Wang, L.; He, J. Simultaneous Determination of Seven Components in Blumea balsamifera Oil by HPLC. J. Chin. Med. Mater. 2020, 43, 2189–2193. [Google Scholar]
  32. Zhao, X.; Zeng, Y.; Zhou, Y.; Li, R.; Yang, M. Gas Chromatography–Mass Spectrometry for Quantitative and Qualitative Analysis of Essential Oil from Curcuma wenyujin Rhizomes. World J. Tradit. Chin. Med. 2021, 7, 138–145. [Google Scholar] [CrossRef]
  33. Sadgrove, N.J.; Padilla-González, G.F.; Phumthum, M. Fundamental Chemistry of Essential Oils and Volatile Organic Compounds, Methods of Analysis and Authentication. Plants 2022, 11, 789. [Google Scholar] [CrossRef] [PubMed]
  34. Gong, L.; Jiang, H.; Zhang, H.; Cui, Q.; Rong, R. Analysis of volatile constituents in Forsythia Suspensa by gas chromatography-mass spectrometry. J. Shandong Univ. Tradit. Chin. Med. 2015, 39, 256–257+276. [Google Scholar]
  35. Dong, M.; Li, Y.; Wang, R.; Ni, Y. Study on volatile oil GC-MS characteristic spectrumin Shanxi Fructus forsythiae. Chin. J. Hosp. Pharm. 2011, 31, 355–357. [Google Scholar]
  36. Jiang, S.; Wang, M.; Yuan, H.; Xie, Q.; Liu, Y.; Li, B.; Jian, Y.; Liu, C.; Lou, H.; Rahman, A.U.; et al. Medicinal Plant of Bletilla striata: A Review of its Chemical Constituents, Pharmacological Activities, and Quality Control. World J. Tradit. Chin. Med. 2020, 6, 393–407. [Google Scholar]
  37. Jiang, H.; Wang, X.; Yang, L.; Zhang, J.; Hou, A.; Man, W.; Wang, S.; Yang, B.; Chan, K.; Wang, Q.; et al. The Fruits of Xanthium sibiricum Patr: A Review on Phytochemistry, Pharmacological Activities, and Toxicity. World J. Tradit. Chin. Med. 2020, 6, 408–422. [Google Scholar]
Separations 10 00025 g001 550
Figure 1. Experimental device for steam distillation.
Figure 1. Experimental device for steam distillation.
Separations 10 00025 g001
Separations 10 00025 g002 550
Figure 2. HPLC chromatograms of β-pinene.
Figure 2. HPLC chromatograms of β-pinene.
Separations 10 00025 g002
Separations 10 00025 g003 550
Figure 3. Volatile oil yield at a fixed collection temperature of 10 °C.
Figure 3. Volatile oil yield at a fixed collection temperature of 10 °C.
Separations 10 00025 g003
Separations 10 00025 g004 550
Figure 4. Volatile oil yield when the fixed distillation time was 4.5 h.
Figure 4. Volatile oil yield when the fixed distillation time was 4.5 h.
Separations 10 00025 g004
Separations 10 00025 g005 550
Figure 5. Volatile oil yield when the fixed water addition was 10 mL/g.
Figure 5. Volatile oil yield when the fixed water addition was 10 mL/g.
Separations 10 00025 g005
Separations 10 00025 g006 550
Figure 6. Three-dimensional design space diagram.
Figure 6. Three-dimensional design space diagram.
Separations 10 00025 g006
Separations 10 00025 g007 550
Figure 7. Two-dimensional design space diagram (water addition was fixed at 10 mL/g; “❌” is the verification point outside the design space; “🔴” is the verification point inside the design space; and the color bar on the right is the probability of meeting the standard.).
Figure 7. Two-dimensional design space diagram (water addition was fixed at 10 mL/g; “❌” is the verification point outside the design space; “🔴” is the verification point inside the design space; and the color bar on the right is the probability of meeting the standard.).
Separations 10 00025 g007
Separations 10 00025 g008 550
Figure 8. Total ion chromatogram of the GC–MS analysis of volatile oils.
Figure 8. Total ion chromatogram of the GC–MS analysis of volatile oils.
Separations 10 00025 g008
Table
Table 1. Literature on steam distillation.
Table 1. Literature on steam distillation.
Medicinal MaterialDesign of ExperimentMaterial/Liquid Ratio (g:mL)Soaking Time (h)Distillation Time (h)Optimum ConditionsVolatile Oil YieldReference
F. suspensaTaguchi design1:8~1:121~42~6Material/liquid ratio 1:8, soaking time 2 h, distillation time 6 h.0.926 mL/100 g[17]
F. suspensaBox–Behnken design1:4~1:108~248~20Material/liquid ratio 1:5, soaking time 21 h, distillation time 11 h.0.342 mL/100 g[18]
L. japonicaSingle-factor design, Box–Behnken design1:15~1:250~57~11Material/liquid ratio 1:20, soaking time 1 h, distillation time 7 h.0.14998 g/100 g[19]
L. japonicaSingle-factor design, Taguchi design1:9~1:1120~2838~42Material/liquid ratio 1:10, soaking time 28 h, distillation time 42 h0.171 g/100 g[20]
Table
Table 2. Origin and batch information of medicinal materials.
Table 2. Origin and batch information of medicinal materials.
Medicinal MaterialsNumberOriginCompanies
L. japonicaJYH-1ShandongZhejiang Huqing Yutang Materia Medica Co., Ltd.
JYH-2HebeiHebei Linyitang Pharmaceutical Co., Ltd.
F. suspensaLQ-1ShanxiHaozhou Feimao Pharmaceutical Co., Ltd.
LQ-2ShaanxiHaozhou Chujian Huakai E-Commerce Co., Ltd.
LQ-3ShanxiNanjing Shangyuantang Pharmaceutical Co., Ltd.
LQ-4ShaanxiAnguo Pharmaceutical Source Trading Co., Ltd.
LQ-5ShanxiHebei Linyitang Pharmaceutical Co., Ltd.
LQ-6GansuSichuan Xunbai Herbal Industry Co., Ltd.
Table
Table 3. The factors and levels of the Box–Behnken design.
Table 3. The factors and levels of the Box–Behnken design.
FactorLevel
Low (−1)Medium (0)High (1)
X1: water addition (mL/g)81012
X2: distillation time (h)3.04.56.0
X3: collection temperature (°C)51525
Table
Table 4. The results of the Box–Behnken design.
Table 4. The results of the Box–Behnken design.
NoX1: Water Addition (mL/g)X2: Distillation Time (h)X3: Collection Temperature (°C)Z1: Volatile Oil Content (mL/100 g)Z2: β-Pinene Content (mg/g)Y: Volatile Oil Yield (mL/100 g)
183.0151.6010.8570.63
2123.0151.5990.8670.54
386.0151.7921.0390.92
4126.0151.3490.8120.83
584.551.9691.1390.90
6124.551.6010.8570.80
784.5251.5990.8670.80
8124.5251.7921.0390.83
9103.051.3490.8120.74
10106.051.9691.1390.98
11103.0251.6010.8570.61
12106.0251.5990.8670.71
13104.5151.7921.0390.82
14104.5151.3490.8120.80
15104.5151.9691.1390.89
16104.5151.9691.1390.94
17104.5151.9691.1390.90
Table
Table 5. Single-factor experiments.
Table 5. Single-factor experiments.
FactorMedicine NumberParticle SizeSoaking Time (h)Water Addition (mL/g)Distillation (h)Volatile Oil Yield (mL/100 g)
Particle sizeLQ-5Not crushed01051.900
Coarsest flour1.820
Coarse flour1.827
Soaking timeLQ-5Not crushed01051.900
21.922
41.952
Water additionLQ-1Not crushed0851.485
101.479
121.350
Table
Table 6. Separate distillation of volatile oils from F. suspensa or L. japonica.
Table 6. Separate distillation of volatile oils from F. suspensa or L. japonica.
Medicine NumberWater Addition
(mL/g)		Distillation Time
(h)		Collection Time
(°C)		Volatile Oil Yield (mL/100 g)
LQ-510551.864
JYH-110550
JYH-210550
Table
Table 7. Co-distillation of volatile oils from F. suspensa and L. japonica.
Table 7. Co-distillation of volatile oils from F. suspensa and L. japonica.
Medicine NumberWater Addition
(mL/g)		Distillation Time
(h)		Collection Temperature
(°C)		Volatile Oil Yield (mL/100 g)
LQ-5JYH-2105Indoor temperature0.930
125Indoor temperature0.851
LQ-1JYH-210550.880
12550.930
Table
Table 8. Characterization of raw material properties of different batches of F. suspensa.
Table 8. Characterization of raw material properties of different batches of F. suspensa.
Medicine NumberVolatile Oil Content (mL/100 g)β-Pinene Content (mg/100 g)
LQ-11.6010.857
LQ-21.5990.867
LQ-31.7921.039
LQ-41.3940.812
LQ-51.9691.139
LQ-61.5000.746
Table
Table 9. Regression coefficient and variance analysis of the model.
Table 9. Regression coefficient and variance analysis of the model.
FactorY
Coefficientp Value
Constant0.2294
X20.049770.0067 **
Z1−0.51990.0014 **
Z21.3250.0001 **
X1X3−0.0003180.0139 *
Model p value<0.0001
R20.9022
R2adj0.8695
* p < 0.05, ** p < 0.01.
Table
Table 10. The volatile oil of F. suspensa.
Table 10. The volatile oil of F. suspensa.
NoRetention Time (Min)IUPAC NameCommon NameChemical FormulaBase Peak
(m/z)		Relative Content (%)
110.14Bicyclo [3.1.0]hex-2-ene, 2-methyl-5-(1-methylethyl)-α-ThujeneC10H1693.204.25
210.51Bicyclo [3.1.1]hept-2-ene, 2,6,6-trimethyl-α-PineneC10H1693.2921.12
311.15Bicyclo [2.2.1]heptane, 2,2-dimethyl-3-methylene-CampheneC10H1693.201.62
413.09Bicyclo [3.1.1]heptane, 6,6-dimethyl-2-methylene-β-PineneC10H1693.2953.71
514.131,6-Octadiene, 7-methyl-3-methylene-β-MyrceneC10H1693.201.66
615.491,3-Cyclohexadiene, 1-methyl-4-(1-methylethyl)-α-TerpineneC10H16121.200.82
716.04Benzene, 1-methyl-3-(1-methylethyl)-m-cymeneC10H14119.202.38
816.28Cyclohexene, 1-methyl-4-(1-methylethenyl)-, (4R)-(+)-LimoneneC10H1693.204.36
918.351,4-Cyclohexadiene, 1-methyl-4-(1-methylethyl)-γ-TerpineneC10H1693.201.96
1020.32Cyclohexene, 1-methyl-4-(1-methylethylidene)-TerpinoleneC10H1693.200.38
1123.53Bicyclo [3.1.1]heptan-3-ol, 6,6-dimethyl-2-methylene-, (1S,3R,5S)-(-)-trans-PinocarveolC10H16O92.200.32
1225.16Bicyclo [3.1.1]heptan-3-one, 6,6-dimethyl-2-methylene-PinocarvoneC10H14O81.200.18
1326.393-Cyclohexen-1-ol, 4-methyl-1-(1-methylethyl)-Terpinen-4-olC10H18O71.205.97
1427.363-Cyclohexene-1-methanol, α,α,4-trimethyl-α-TerpineolC10H18O59.200.40
1527.47Bicyclo [3.1.1]hept-2-ene-2-carboxaldehyde, 6,6-dimethyl-MyrtenalC10H14O79.200.50
1627.69Bicyclo [3.1.1]hept-2-ene-2-methanol, 6,6-dimethyl-MyrtenolC10H16O79.200.39
Table
Table 11. The volatile oil of mixtures of F. suspensa and L. japonica.
Table 11. The volatile oil of mixtures of F. suspensa and L. japonica.
NoRetention Time (Min)IUPAC NameCommon NameChemical FormulaBase Peak
(m/z)		Relative Content (%)
110.13Bicyclo [3.1.0]hex-2-ene, 2-methyl-5-(1-methylethyl)-α-ThujeneC10H1693.204.48
210.50Bicyclo [3.1.1]hept-2-ene, 2,6,6-trimethyl-α-PineneC10H1693.2921.38
311.15Bicyclo [2.2.1]heptane, 2,2-dimethyl-3-methylene-CampheneC10H1693.201.63
413.13Bicyclo [3.1.1]heptane, 6,6-dimethyl-2-methylene-β-PineneC10H1693.2954.75
514.131,6-Octadiene, 7-methyl-3-methylene-β-MyrceneC10H1693.201.56
615.491,3-Cyclohexadiene, 1-methyl-4-(1-methylethyl)-α-TerpineneC10H16121.201.23
716.03Benzene, 1-methyl-3-(1-methylethyl)-m-cymeneC10H14119.201.66
816.27Cyclohexene, 1-methyl-4-(1-methylethenyl)-, (4R)-(+)-LimoneneC10H1693.204.41
918.351,4-Cyclohexadiene, 1-methyl-4-(1-methylethyl)-γ-TerpineneC10H1693.202.29
1020.32Cyclohexene, 1-methyl-4-(1-methylethylidene)-TerpinoleneC10H1693.200.37
1123.53Bicyclo [3.1.1]heptan-3-ol, 6,6-dimethyl-2-methylene-, (1S,3R,5S)-(-)-trans-PinocarveolC10H16O92.200.28
1225.17Bicyclo [3.1.1]heptan-3-one, 6,6-dimethyl-2-methylene-PinocarvoneC10H14O81.200.14
1326.373-Cyclohexen-1-ol, 4-methyl-1-(1-methylethyl)-Terpinen-4-olC10H18O71.204.98
1427.423-Cyclohexene-1-methanol, α,α,4-trimethyl-α-TerpineolC10H18O59.200.28
1527.47Bicyclo [3.1.1]hept-2-ene-2-carboxaldehyde, 6,6-dimethyl-MyrtenalC10H14O79.200.43
1627.70Bicyclo [3.1.1]hept-2-ene-2-methanol, 6,6-dimethyl-MyrtenolC10H16O79.200.13
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Chen, X.; Guo, D.; Gong, X.; Wan, N.; Wu, Z. Optimization of Steam Distillation Process for Volatile Oils from Forsythia suspensa and Lonicera japonica according to the Concept of Quality by Design. Separations 2023, 10, 25. https://doi.org/10.3390/separations10010025

AMA Style

Chen X, Guo D, Gong X, Wan N, Wu Z. Optimization of Steam Distillation Process for Volatile Oils from Forsythia suspensa and Lonicera japonica according to the Concept of Quality by Design. Separations. 2023; 10(1):25. https://doi.org/10.3390/separations10010025

Chicago/Turabian Style

Chen, Xinying, Dongyun Guo, Xingchu Gong, Na Wan, and Zhenfeng Wu. 2023. "Optimization of Steam Distillation Process for Volatile Oils from Forsythia suspensa and Lonicera japonica according to the Concept of Quality by Design" Separations 10, no. 1: 25. https://doi.org/10.3390/separations10010025

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop