CN101123888A - 寡糖混合物 - Google Patents
寡糖混合物 Download PDFInfo
- Publication number
- CN101123888A CN101123888A CNA2006800054679A CN200680005467A CN101123888A CN 101123888 A CN101123888 A CN 101123888A CN A2006800054679 A CNA2006800054679 A CN A2006800054679A CN 200680005467 A CN200680005467 A CN 200680005467A CN 101123888 A CN101123888 A CN 101123888A
- Authority
- CN
- China
- Prior art keywords
- lactose
- oligosaccharides
- oligosaccharide
- mixture
- newborn
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Granted
Links
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Classifications
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- A—HUMAN NECESSITIES
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- A23C9/14—Milk preparations; Milk powder or milk powder preparations in which the chemical composition of the milk is modified by non-chemical treatment
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- A—HUMAN NECESSITIES
- A23—FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
- A23C—DAIRY PRODUCTS, e.g. MILK, BUTTER OR CHEESE; MILK OR CHEESE SUBSTITUTES; MAKING THEREOF
- A23C9/00—Milk preparations; Milk powder or milk powder preparations
- A23C9/12—Fermented milk preparations; Treatment using microorganisms or enzymes
- A23C9/1203—Addition of, or treatment with, enzymes or microorganisms other than lactobacteriaceae
- A23C9/1206—Lactose hydrolysing enzymes, e.g. lactase, beta-galactosidase
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- A—HUMAN NECESSITIES
- A23—FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
- A23L—FOODS, FOODSTUFFS, OR NON-ALCOHOLIC BEVERAGES, NOT COVERED BY SUBCLASSES A21D OR A23B-A23J; THEIR PREPARATION OR TREATMENT, e.g. COOKING, MODIFICATION OF NUTRITIVE QUALITIES, PHYSICAL TREATMENT; PRESERVATION OF FOODS OR FOODSTUFFS, IN GENERAL
- A23L29/00—Foods or foodstuffs containing additives; Preparation or treatment thereof
- A23L29/30—Foods or foodstuffs containing additives; Preparation or treatment thereof containing carbohydrate syrups; containing sugars; containing sugar alcohols, e.g. xylitol; containing starch hydrolysates, e.g. dextrin
-
- A—HUMAN NECESSITIES
- A23—FOODS OR FOODSTUFFS; TREATMENT THEREOF, NOT COVERED BY OTHER CLASSES
- A23L—FOODS, FOODSTUFFS, OR NON-ALCOHOLIC BEVERAGES, NOT COVERED BY SUBCLASSES A21D OR A23B-A23J; THEIR PREPARATION OR TREATMENT, e.g. COOKING, MODIFICATION OF NUTRITIVE QUALITIES, PHYSICAL TREATMENT; PRESERVATION OF FOODS OR FOODSTUFFS, IN GENERAL
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Abstract
本发明涉及来源于动物乳的寡糖混合物、包含所述寡糖混合物的食品和用于生产所述寡糖混合物的方法。
Description
发明领域
本发明涉及来源于动物乳的寡糖混合物、包含所述寡糖混合物的食品和用于生产所述寡糖混合物的方法。
发明背景
人类的大肠被多种细菌所建群,所述细菌对消化道生理具有正面和负面的双重作用,也具有其它系统性的影响。结肠中所发现的细菌的优势类群包括类菌体、双歧杆菌、真细菌、梭菌和乳杆菌。所存在的细菌响应结肠中的底物可用性、氧化还原电位、pH、O2压和分布,具有波动的活性。通常,肠内的细菌可分为对宿主发挥潜在危害或有益作用的种类。致病作用(例如,其可能由梭菌或类菌体引起)包括腹泻、感染、肝脏损害、致癌作用和肠腐烂。健康促进作用可以由有害细菌的生长抑制、免疫功能的刺激、增强必需营养成分的消化和吸收及维生素的合成所引起。具有健康促进作用的细菌类群(例如双歧杆菌和乳杆菌)在数量和活性上的增加是值得期望的。
特别就婴儿来说,直至出生前,婴儿的胃肠道被认为是无菌的。在出生的过程中,其遭遇了来自母亲消化道和皮肤的细菌并开始变得被建群。对应于婴儿的喂养,消化道小型生物群的组成存在大的不同。母乳喂养的婴儿的粪便菌群包括双歧杆菌和一些乳杆菌种类的可观群体,而配方喂养的婴儿具有更复杂的小型生物群,双歧杆菌、类菌体、梭菌和链球菌通常都存在。断乳后,类似成人模式的消化道小型生物群模式得以建立。
对于所有婴儿均建议使用母乳。然而,在一些情况下,母乳喂养是不充分的,或者由于医学原因是不成功的,或者母亲并不选择母乳喂养。针对这些情况,已开发了婴儿配方。
向食品中添加益生元是促进结肠中有益细菌的数量和/或活性增长的一种方法。益生元是不易消化的食品成分,其通过选择性地刺激结肠中一种或有限数量的细菌的生长和/或活性来有益地影响宿主,从而增进宿主健康。此类成分是不易消化的,因为其在胃或小肠中不能被分解和吸收,从而完整地通过并到达结肠,在此处由有益细菌选择性地进行发酵。益生元的例子包括某些寡糖,例如果寡糖(FOS)和半乳寡糖(GOS)。
已知人乳比大多数其它动物乳含有更大量的不能消化的寡糖。事实上,不能消化的寡糖代表着母乳中第三大固体成分(在乳糖和脂类之后),初乳中以12-15g/l的浓度存在,成熟乳汁中以5-8g/l存在。人乳寡糖对于酶水解是非常有抵抗力的,表明这些寡糖可显示出与其热值并不直接相关的基本功能。
由于人乳的组成已有更好的了解,也已建议将益生元添加至婴儿配方中。补充了益生元的多种婴儿配方例如果寡糖和半乳寡糖混合物的多种婴儿配方可通过商业途径获得。然而,此类混合物只是粗略地近似人乳中寡糖的混合物。人乳中已检测到超过100种不同的寡糖成分,其中一些至今根本未在动物乳例如牛奶中检测到,或者仅检测到少量。仅以非常小的量在牛奶和初乳中存在或根本不存在的人乳寡糖种类的例子有唾液酸化和岩藻糖基化的寡糖。
美国专利申请号2003/0129278描述了以产生于一种或几种动物乳的寡糖为基础的寡糖混合物,其特征在于其包含至少两种寡糖级分,每一级分均由至少两种不同的寡糖组成,游离的乳糖不属于所述寡糖。存在于寡糖混合物中的寡糖全谱不同于在动物乳或从中提取寡糖级分的动物乳中所存在的那些寡糖。此外a)如果所述仅寡糖提取于一种动物乳,中性寡糖与酸性(唾液酸化)寡糖的比率为96-60∶10-40重量%,或b)如果所述寡糖提取于至少两种动物乳,从两种不同动物乳中所提取的寡糖每种占寡糖混合物中所存在的寡糖总量的10重量%。
美国专利号5,270,462描述了从干酪乳清或粗制凝乳酶乳清以高浓度回收唾液酸结合的寡糖、唾液酸结合的肽和唾液酸结合的脂类的方法,其包括如下步骤:调整干酪乳清或粗制凝乳酶乳清至pH2-5;将乳清与阳离子交换剂相接触以产生通过交换剂的溶液;并将所述通过交换剂的溶液浓缩和/或脱盐。所得的具有高含量唾液酸的组合物可用作食品材料或医学材料。
EP0458358涉及生产含有按重量计10-15%的半乳寡糖的脱脂奶粉的方法,其包括:
(i)浓缩脱脂乳以获得具有按重量计20-50%的固体含量的浓缩乳,
(ii)向浓缩乳中加入β-半乳糖苷酶,以产生酶促反应,
(iii)加热所获得的反应混合物30秒钟至15分钟,至70-85℃的温度,以便终止酶促反应,并
(iv)喷雾干燥反应终止的混合物。
本发明的目标是提供寡糖混合物,其作为益生元是有效的,特别是在人类消化道中是有效的,并且其具有比那些果寡糖和半乳寡糖混合物所提供的寡糖谱更加接近于人乳寡糖谱的寡糖谱。
发明概述
在一方面,本发明涉及来自动物乳的寡糖混合物,其中混合物具有小于250的乳糖∶寡糖比例,且含有与其所来源的乳相同的寡糖谱。此成分是新的保护性和免疫调节成分,例如,与可获得的益生元成分例如果寡糖和半乳寡糖相比,其结构上更接近于人母乳寡糖,例如因为具有更高比例的唾液酸化的寡糖。低乳糖∶寡糖比例具有下述优势,即可将寡糖混合物加入婴儿配方和其它食品中,也不会导致非自然的高含量乳糖。例如,可将0.5至50g寡糖混合物加入每升配方奶粉中。优选地,混合物具有125至1.25的乳糖∶寡糖比例。
优选地,寡糖混合物来自一种或多种奶牛奶、山羊奶或水牛奶,尽管来自其它动物例如绵羊、骆驼、马和大象的奶也可使用。
任选地寡糖混合物进一步包含β-半乳-寡糖(β-GOS)。人乳比其它动物乳例如奶牛奶含有显著更多的中性寡糖,因此,提高本发明寡糖混合物中的GOS含量从而生产具有更加接近于人乳寡糖谱的混合物是所希望的。本发明混合物中的寡糖∶β-半乳-寡糖比例可在0.01至99的范围内。优选地,OS∶GOS比例在1∶2至1∶20之间,特别优选的比例在1∶2至1∶6之间。
在本发明的另一方面涉及包含如上所述的寡糖混合物的食品。任选地食品为婴儿食品或配方,但该产品可为任何由小孩、婴儿或成人使用的食物或饮料。含有寡糖混合物作为益生元的食品的消耗将选择性地促进结肠中一种或有限数量的细菌的生长和/或活性,从而增进宿主健康。
在本发明更进一步的方面中提供了用于生产寡糖混合物的方法,所述寡糖混合物来自动物乳并具有与其所来源的乳相同的寡糖谱,该方法包括下述步骤(a)将去蛋白质的乳材料浓缩至50-75%总固体量,(b)将浓缩的乳材料进行乳糖去除步骤以产生具有小于250的乳糖∶寡糖比例的液体,且(c)将乳材料脱矿质,脱矿质步骤在浓缩步骤之前或者乳糖去除步骤之后进行。
优选地,方法的步骤(b)包括在浓缩步骤之后的乳糖结晶步骤,以除去乳糖晶体并产生具有小于250的乳糖∶寡糖比例的液体。
备选地,乳糖去除步骤可包括将步骤a)中产生的浓缩材料进行喷雾干燥,然后加水溶解寡糖,而使乳糖处于结晶形式。
任选地,可重复(在其中一些乳糖已通过结晶去除的情况中)或增加(在其中使用了差别溶解度的情况中)乳糖结晶和去除步骤,以便进一步浓缩液体和除去乳糖。
优选地,脱矿质步骤在乳糖去除步骤之后进行。
优选地,去蛋白质的乳材料是乳或乳清的超滤渗透物。然而,任何去蛋白质的乳材料例如酸乳清或甜乳清(均为干酪制造的副产品)在乳清蛋白质去除之后均可用于每种情况中。
任选地,方法进一步包括用β-半乳糖苷酶处理以生产β-半乳-寡糖。所使用的β-半乳糖苷酶可为任何微生物、植物或动物来源,条件是它显示出重要的转半乳糖苷活性。优选地,所使用的β-半乳糖苷酶来源于米曲霉(Aspergillus oryzae)。该酶处理可在去蛋白质的乳材料浓缩之前或乳糖去除步骤完成之后,或者如希望在去蛋白质的乳材料浓缩之前和乳糖去除步骤完成之后发生,但是优选地发生在乳糖去除步骤完成之后。
在乳糖去除步骤之后,液体产品可用单独的蛋白酶和/或其组合进行处理,以将任何残留的乳蛋白质和肽降解为分子量减小的实体。这是特别优选的,如果将寡糖混合物掺入低变应原性婴儿配方中,该配方是为具有发生牛奶过敏反应危险的婴儿设计的,且因此仅含有部分水解的蛋白质。
所获得的液体产品可以液体形式使用,但优选地将其喷雾干燥以产生粉末。
发明详述
本发明提供了来自动物乳的寡糖混合物及其生产方法,其中混合物具有小于250的乳糖∶寡糖比例,并含有与其所来源的乳相同的寡糖谱。该混合物可掺入婴儿或成人食品中并赋予益生、免疫调节和保护的效果。
此处将寡糖定义为那些在动物乳中天然发现的并具有3至20(包括3和20)范围之内的聚合度(DP)的寡糖。
本发明的寡糖混合物也含有乳糖(DP=2),且具有小于250,优选地在125至1.25之间的乳糖∶寡糖比例。与最初的动物乳相比,这相当于在寡糖混合物中降低了2至200倍的乳糖含量,其等于寡糖与乳糖之间的比例增加2至200倍。
本发明的寡糖混合物来自于一种或多种动物乳。该乳可从任何一种动物获得,特别是从奶牛、山羊、水牛、马、大象、骆驼或绵羊中获得。
用于生产寡糖混合物的方法中的原料是去蛋白质的乳材料,例如已除去蛋白质的乳、或者已从中去除乳清蛋白质的乳清或任何制备的或改良的乳清材料。此类材料包括酸乳清和甜乳清。优选的原料是乳超滤渗透物和乳清超滤渗透物。备选地,原料可为重构的粉末,例如粉末状超滤渗透物。
原料应为去蛋白质的产品,因为浓缩过程中蛋白质的存在可导致不希望的美拉反应和褐变。可通过任何已知的方式对原料进行去蛋白质,例如酸沉淀、加热方法、离子交换。然而,优选地,通过超滤来实现蛋白质的去除,这还从原料中去除了脂类。
也可通过任何已知的方式,例如反渗透、纳膜过滤或离子交换对原料脱矿质。备选地,脱矿质步骤可在乳糖去除步骤之后再次利用任何已知的方式来进行。
原料的pH可在3至7.5之间,尽管优选5至6范围内的pH以阻止寡糖水解例如唾液酸乳糖的脱唾液酸化,并帮助减少褐变反应。
将去蛋白质的乳材料通过任何已知的方式浓缩至50-75%总固体(TS),优选地55-60%TS,条件是温度不升高至将寡糖水解或脱唾液酸的水平。优选地在50-90℃、更优选地50-75℃的温度下进行浓缩。蒸发是一种优选的技术,其在80-200mbar的压力下进行。在此方法中,温度不升至60℃以上,以保证寡糖不受影响。备选地,如果原料是粉末,可通过粉末的适当重构来实现浓缩至所期望的水平。
此方法任选地包括进一步用β-半乳糖苷酶处理去蛋白质的乳材料的步骤,以便生产包含β-半乳-寡糖(GOS)的乳材料。因此,在乳材料浓缩(步骤(a))之前和/或乳糖去除步骤(步骤(b))之后可用β-半乳糖苷酶对乳材料进行处理,但是优选地发生在乳糖去除步骤完成之后。β-半乳糖苷酶催化乳糖分解为单糖半乳糖和葡萄糖,且随后形成半乳-寡糖。优选地,所用的β-半乳糖苷酶来源于米曲霉。此种酶是作为Lactase F可通过商业途径从Amano,日本获得的。根据FCCIV方法所测定的酶活性可为1000至30000U/kg乳糖之间。原料的酶处理可在3-8的pH范围内,4-70℃的温度下,乳糖浓度为5-70g/100g TS之间,酶浓度为1.5-10g每kg寡糖混合物。优选地,大约酶kg寡糖混合物使用约5g酶,在40-70℃下孵育1至24小时。酶可在使用后通过加热来灭活。
优选地,乳糖去除步骤可通过乳糖结晶来实现。在浓缩的原料中通过例如在加入或不加入晶种时冷却浓缩的材料可实现乳糖结晶。然后将乳糖晶体通过任一已知的方法,例如通过离心、过滤、倾析除去。
从寡糖中分离乳糖的备选方法使用差别溶解度。将原料喷雾干燥,然后加水溶解寡糖,同时使寡糖处于结晶形式。
所获得的液体高度富含寡糖,寡糖∶乳糖的比例与该液体所来源的乳中所发现的比例相比高2至200倍。
可如上所述对液体进行再浓缩,并可进行进一步的乳糖去除步骤。此方法可根据需要进行重复。
当除去所期望量的乳糖时,可用单独的蛋白酶和/或其组合来处理液体,以将任何残留的乳蛋白质和肽降解为分子量减小的实体。如果有意将该混合物掺入低变应原性婴儿配方中,此步骤是所希望的。
优选地,该液体也如上所述用β-半乳糖苷酶处理以形成β-半乳-寡糖。这样获得了第二种用于食品的建议成分,所述食品包含如上所述的乳寡糖和具有3-10的DP的GOS。
当用1-6mg β-半乳糖苷酶每g TS处理具有50%的总固体浓度和大约35%乳糖的液体时,所获得的溶液可含有大约2-4%寡糖、大约2-15%GOS、大约15-30%乳糖、大约5-10%半乳糖和大约2-14%葡萄糖。寡糖∶β-GOS的比例可在0.01至99的范围内,但在1.2至1∶20,优选地1∶2至1∶6的范围内。
所获得的液体可以液体形式使用或者可进行干燥(例如通过喷雾干燥)以形成粉末。所获得的粉末含有大约50%乳糖,剩余物是寡糖(大约1-20%,包括唾液酸化寡糖)、单糖例如葡萄糖和半乳糖、大约10%非蛋白质的含氮化合物、2%剩余蛋白和一些剩余盐的混合物。
在本发明优选的方面,将如上所述的寡糖混合物掺入食品中。在本发明的上下文中,术语“食品”意为包含任何可消费的物质。因此,其可为有意供给人类消费的产品,特别是婴儿配方、脱水奶粉,包括成长奶粉或谷类混合物。
婴儿配方可通过任何合适的方式来制备。例如,可通过将蛋白质源、除乳糖之外的任何糖类和脂肪源以合适的比例混和在一起来制备婴儿配方。如果需要的话可加入乳化剂。此时可加入维生素和矿物质,但通常随后再加入以避免热降解。任何亲脂维生素、乳化剂等可在混和之前溶解于脂肪源中。水,优选地已进行反向透析的水,可随后混和进去以形成液体混合物。
然后可将液体混合物加热处理以减少细菌负载量。例如,可将液体混合物快速加热至大约80℃至大约110℃范围的温度大约5秒钟至大约5分钟。这可通过蒸汽注射或通过热交换器例如板式热交换器来完成。
然后将液体混合物冷却至大约60℃至大约85℃,例如通过瞬时冷却。然后将液体混合物搅匀,例如以两个步骤进行,在第一步中在大约7MPa至大约40MPa下,第二步中在大约2MPa至大约14MPa下。然后进一步冷却搅匀的混合物,以便加入热敏感成分例如维生素和矿物质。此时方便地对搅匀的混合物的pH和固体含量进行标准化。
将搅匀的混合物转移至合适的干燥设备中,例如喷雾干燥器或冷冻干燥器中,并将其转变为粉末。该粉末应当具有以重量计少于约5%的含湿量。
可在制造过程中的合适阶段通过湿混和或者通过干混和将本发明的寡糖混合物加入婴儿配方或其它食品中,但优选地在喷雾干燥前立即通过湿混和加入,例如在标准罐中。然而,对于本领域的技术人员,这一点是明显的,即婴儿配方中糖类的量需要进行调整以便考虑寡糖混合物将要提供的另外的糖类。小孩或婴儿食品或配方中寡糖混合物的终浓度优选地在2至50g/l之间,例如作为消费的配方中的32.5g/l。然而,这些量不应视为限制性的,且应根据目标人群进行调整,例如基于小孩或婴儿的体重和年龄或健康进行调整。优选地,每次喂养时给小孩喂养含有本发明寡糖混合物的配方。
备选地,可通过干混和将寡糖混合物加入婴儿或成人食品中。该混合物可以约5至40克寡糖每100g干配方的浓度加入小孩或婴儿配方中,不会向配方中引入非天然的高含量乳糖。然而,这些量不应视为限制性的,并应根据目标人群进行适当调整,例如基于小孩或婴儿的体重和年龄、或者特定人群的健康进行调整。
尽管补充特别针对婴儿或小孩营养的食品是优选的,但补充非特别针对的或者针对成人人群的食品可以是有益的。例如,可将本发明的寡糖混合物掺入健康护理营养品和老年人营养品中。此类食品可包括奶、酸乳酪、凝乳、干酪、发酵奶、基于奶的发酵产品、冰淇淋、基于发酵谷类的产品或基于奶的产品等等。
现在将通过参考下列实施例对本发明进行进一步描述。
实施例1
下面描述了一种制备根据本发明的寡糖混合物的方法。
将200,000升乳清超滤渗透物预浓缩至22%(w/w)总固体(TS),在大约75℃巴氏消毒30秒,然后通过在60℃蒸发浓缩以达到59%(w/w)的TS。在结晶器中以每小时2℃的速度将液体冷却24小时至结晶出乳糖。洗涤结晶的乳糖,然后通过绞拧机将其除去。剩余的液体通过倾析器进行澄清。将从澄清器获得的17.7%TS的77000升通过60℃蒸发进行再浓缩以达到55%(w/w)的TS,并将其进行与前面相同条件下的第二次乳糖结晶步骤。将因此所获得的20.5%TS的29000升液体通过电渗析和离子交换的组合以本身已知的方式进行脱矿质,获得28500升90%脱矿质的17.3%TS的液体。此液体含有每100g TS大约2克动物乳寡糖和每100g TS 70克乳糖,可通过向湿相中添加而直接加入食品例如婴儿配方中,也可干燥,例如通过喷雾干燥并通过干混和加入食品例如婴儿配方中。
实施例2
将根据实施例1所生产的100kg 50%TS的寡糖混合物在标准罐中加热至60℃,并将pH调整至6至6.5。测定混合物中乳糖、葡萄糖、半乳糖、半乳寡糖和其它寡糖的浓度。每克TS中加入4.5mg Lactase F(Amano,日本)并将混合物在60℃下保持3小时。然后通过直接蒸汽注射将温度升至110℃11秒,使酶失活。再次测定混合物中乳糖、葡萄糖、半乳糖、半乳寡糖和其它寡糖的浓度并将结果显示如下。
| (%干物质) | 乳糖 | 葡萄糖 | 半乳糖 | OS | GOS |
| 时间0 | 70 | 3 | 5 | 2 | 0.7 |
| 3小时后 | 29 | 12 | 11 | 2 | 10 |
实施例3
如下给出了含有根据本发明的寡糖混合物的婴儿配方组合物的实施例。
| 营养物 | 每100kcal | 每升 |
| 能量(kcal) | 100 | 670 |
| 蛋白质(g) | 1.83 | 12.3 |
| 脂肪(g) | 5.3 | 35.7 |
| 亚油酸(g) | 0.79 | 5.3 |
| α-亚麻酸(mg) | 101 | 675 |
| 乳糖(g) | 11.2 | 74.7 |
| OS混合物(来自实施例1)(g) | 1.49 | 1.0 |
| GOS(来自实施例2)(g) | 0.746 | 5.0 |
| 矿物质(g) | 0.37 | 2.5 |
| Na(mg) | 23 | 150 |
| K(mg) | 89 | 590 |
| Cl(mg) | 64 | 430 |
| Ca(mg) | 62 | 410 |
| P(mg) | 31 | 210 |
| Mg(mg) | 7 | 50 |
| Mn(μg) | 8 | 50 |
| Se(μg) | 2 | 13 |
| 维生素A(μgRE) | 105 | 700 |
| 维生素D(μg) | 1.5 | 10 |
| 维生素E(mg TE) | 0.8 | 5.4 |
| 维生素K1(μg) | 8 | 54 |
| 维生素C(mg) | 10 | 67 |
| 维生素B1(mg) | 0.07 | 0.47 |
| 维生素B2(mg) | 0.15 | 1.0 |
| 烟酸(mg) | 1 | 6.7 |
| 维生素B6(mg) | 0.075 | 0.50 |
| 叶酸(μg) | 9 | 60 |
| 泛酸(mg) | 0.45 | 3 |
| 维生素B12(μg) | 0.3 | 2 |
| 生物素(μg) | 2.2 | 15 |
| 胆碱(mg) | 10 | 67 |
| Fe(mg) | 1.2 | 8 |
| I(μg) | 15 | 100 |
| Cu(mg) | 0.06 | 0.4 |
| Zn(mg) | 0.75 | 5 |
Claims (18)
1.来源于动物乳的寡糖混合物,其中混合物具有小于250的乳糖∶寡糖比例,且含有与其所来源的乳相同的寡糖谱。
2.如权利要求1所述的寡糖混合物,其中混合物具有125至1.25的乳糖∶寡糖比例。
3.如前述权利要求中任意一项的寡糖混合物,其来源于奶牛奶、山羊奶或水牛奶的一种或多种。
4.如前述权利要求中任意一项的寡糖混合物,其还包含β-半乳-寡糖。
5.如权利要求4中所述的寡糖,其中寡糖∶β-半乳-寡糖比例为0.01至99。
6.如权利要求4或5所述的寡糖混合物,其中寡糖∶β-半乳-寡糖比例为1∶2至1∶20之间。
7.食品,其包含如前述权利要求中任意一项所述的寡糖混合物。
8.如权利要求7所述的食品,其为婴儿食品或配方。
9.生产寡糖混合物的方法,所述寡糖混合物来源于动物乳并具有与其所来源的乳相同的寡糖谱,该方法包括下述步骤:
(a)将去蛋白质的乳材料浓缩至50-75%总固体;
(b)将浓缩的乳材料进行乳糖去除步骤,以产生具有小于250的乳糖∶寡糖比例的液体;以及
(c)将乳材料脱矿质,脱矿质步骤在浓缩步骤之前或在乳糖去除步骤之后进行。
10.如权利要求9中所述的方法,其中步骤(b)包括乳糖结晶步骤,及浓缩步骤以去除乳糖晶体,并产生具有小于250的乳糖∶寡糖比例的液体。
11.如权利要求9中所述的方法,其中步骤(b)包括将去蛋白质的乳材料喷雾干燥,且然后加水溶解寡糖,而使乳糖处于结晶形式。
12.如权利要求9至11中任意一项所述的方法,其中去蛋白质的乳材料是乳超滤渗透物或乳清超滤渗透物。
13.如权利要求9至12中任意一项所述的方法,其中将乳糖去除步骤重复一次或多次,以进一步浓缩液体和去除乳糖。
14.如权利要求9至13中任意一项所述的方法,其还包括用单独的蛋白酶和/或其组合处理液体产物,以便将任何残留的乳蛋白质和肽降解为具有减小的分子量的实体。
15.如权利要求9至14中任意一项所述的方法,其还包括用β-半乳糖苷酶处理乳材料以产生包含β-半乳糖-寡糖的乳清材料。
16.如权利要求9至14中任意一项所述的方法,其还包括用β-半乳糖苷酶处理液体产物以产生包含β-半乳糖-寡糖的液体。
17.如权利要求15或16所述的方法,其中所使用的β-半乳糖苷酶来源于米曲霉。
18.如权利要求9至17任意一项所述的方法,其还包括将液体产物喷雾干燥得到粉末。
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-
2006
- 2006-02-21 RU RU2007135017/10A patent/RU2442438C2/ru active
- 2006-02-21 CA CA2601917A patent/CA2601917C/en not_active Expired - Fee Related
- 2006-02-21 CN CN200680005467.9A patent/CN101123888B/zh active Active
- 2006-02-21 MX MX2007010094A patent/MX2007010094A/es active IP Right Grant
- 2006-02-21 ES ES06708410T patent/ES2781328T3/es active Active
- 2006-02-21 WO PCT/EP2006/060130 patent/WO2006087391A1/en active Application Filing
- 2006-02-21 EP EP06708410.3A patent/EP1926394B1/en active Active
- 2006-02-21 BR BRPI0607633-5A patent/BRPI0607633A2/pt not_active Application Discontinuation
- 2006-02-21 AU AU2006215603A patent/AU2006215603A1/en not_active Abandoned
- 2006-02-21 PT PT67084103T patent/PT1926394T/pt unknown
- 2006-02-21 US US11/816,516 patent/US8591981B2/en active Active
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2007
- 2007-09-20 ZA ZA200708100A patent/ZA200708100B/xx unknown
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- 2012-06-19 AU AU2012203568A patent/AU2012203568C1/en active Active
Cited By (4)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN103797021A (zh) * | 2010-11-23 | 2014-05-14 | 雀巢产品技术援助有限公司 | 寡糖混合物以及包含该混合物的食品,特别是婴儿配方产品 |
| CN103797021B (zh) * | 2010-11-23 | 2016-08-10 | 雀巢产品技术援助有限公司 | 寡糖混合物以及包含该混合物的食品,特别是婴儿配方产品 |
| US9409690B2 (en) | 2010-12-21 | 2016-08-09 | Nestec S.A. | Container and pouch |
| CN103547173A (zh) * | 2011-05-24 | 2014-01-29 | 雀巢产品技术援助有限公司 | 包含牛乳中存在的可溶性寡糖级分并具有低单糖水平的用于婴儿配方产品的牛乳寡糖-低聚半乳糖组合物以及生产该组合物的方法 |
Also Published As
| Publication number | Publication date |
|---|---|
| MX2007010094A (es) | 2007-09-25 |
| EP1926394A1 (en) | 2008-06-04 |
| EP1926394B1 (en) | 2020-02-19 |
| CN101123888B (zh) | 2016-03-23 |
| ES2781328T3 (es) | 2020-09-01 |
| WO2006087391A1 (en) | 2006-08-24 |
| CA2601917C (en) | 2013-12-10 |
| RU2442438C2 (ru) | 2012-02-20 |
| PT1926394T (pt) | 2020-05-22 |
| AU2012203568C1 (en) | 2017-11-02 |
| ZA200708100B (en) | 2009-09-30 |
| BRPI0607633A2 (pt) | 2009-09-22 |
| AU2006215603A1 (en) | 2006-08-24 |
| AU2012203568B2 (en) | 2015-02-19 |
| US8591981B2 (en) | 2013-11-26 |
| US20090035813A1 (en) | 2009-02-05 |
| CA2601917A1 (en) | 2006-08-24 |
| AU2012203568A1 (en) | 2012-07-12 |
| RU2007135017A (ru) | 2009-03-27 |
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